Prostate Cancer
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A diagnosis like cancer often causes panic, primarily due to the lack of knowledge and fear of the unknown. However, great strides have been made in the treatment of prostate cancer. As never before, you have options, and members of our prostate cancer community who " have been there, done that " will universally recommend that you move beyond the panic stage and start to gain knowledge. Knowledge is power. We recommend that you take your time, do your research and arrive at the best treatment decision for you and your family based on the characteristics of your total health situation [1].
Be aware that some medical specialist may steer you in the direction of their specialty and often will understate the risk involved with their treatment of choice. Urologist tends to favor surgical option, radiation therapist favor radiation, and medical oncologist may focus on Androgen Deprivation Therapy (ADT) and/or Chemotherapy.
Sitting in the doctor's consultation room with your spouse or other supportive person(s), a patient will better understand treatment information that your physician is presenting only if the patient and his family have been empowered with knowledge.
Patient's Perspective on Prostate Cancer
Active treatment usually begins a few weeks to months after diagnosis, you should meet with various doctors, identify the stage and extend of the cancer, talk over treatment possibilities from your doctor and learn what survivors in our prostate cancer community have to say about their experiences.
StriveWell's Prostate Cancer Community tries to break down everything you need to know about Prostate Cancer and provide a patients perspective through testimonials.
"We are here to help you make an informed emotional decision"
Contents |
The prostate is part of a man's reproductive system. It is located in front of the rectum and under the bladder. It surrounds the urethra, the tube through which urine flows. A healthy prostate is about the size of a walnut. The prostate makes part of seminal fluid. During ejaculation, seminal fluid helps carry sperm out of the man's body as part of semen. Male hormones (androgens) make the prostate grow. The testicles are the main source of male hormones, including testosterone. The adrenal gland also makes testosterone, but in small amounts. If the prostate grows too large, it squeezes the urethra. This may slow or stop the flow of urine from the bladder to the penis [2].
Cancer begins in cells, the building blocks that make up tissues. Tissues make up the organs of the body. Normally, cells grow and divide to form new cells as the body needs them. When cells grow old, they die, and new cells take their place. Sometimes, this orderly process goes wrong. New cells form when the body does not need them, and old cells do not die when they should. These extra cells can form a mass of tissue called a growth or tumor [2].
Tumors can be benign or malignant:
Benign tumors are not cancer:
Malignant tumors are cancer:
Patient's Perspective on Understanding Prostate Cancer
When prostate cancer spreads, cancer is often found in nearby lymph nodes. If cancer has reached these nodes, it also may have spread to other lymph nodes, the bones, or other organs. When cancer spreads from its original place to another part of the body, the new tumor has the same kind of abnormal cells and the same name as the primary tumor. For example, if prostate cancer spreads to bones, the cancer cells in the bones are actually prostate cancer cells. The disease is metastatic prostate cancer, not bone cancer. For that reason, it is treated as prostate cancer, not bone cancer. Doctors call the new tumor "distant" or metastatic disease [2].
Patient's Perspective on Risk factor
In general about 17 of every 100 males in the United States will be diagnosed with prostate cancer during their lifetime. This is the absolute risk of prostate cancer for U.S. males [3].
What are the risk factors for Prostate Cancer?
| Age Range | Probability of Prostate Cancer Diagnosis |
|---|---|
| Under age 40 | 1 in 19,299 |
| Ages 40 through 59 | 1 in 45 |
| Ages 60-79 | 1 in 7 |
| BMI category | % increased risk of death compared to a person with BMI < 25 |
|---|---|
| Overweight (BMI 25-29.9) | 25% increased risk of death |
| Mildly obease men (BMI 30-34.9) | 46% increased risk of death |
| Severely obease men (BMI 35) | 100% increased risk of death |
Patient's Perspective on Prevention
Chemoprevention: Chemoprevention is the use of specific natural or man-made drugs, vitamins, or other agents to reverse, suppress, or prevent cancer growth. Several agents, including difluoromethylornithine (DFMO), isoflavonoids, selenium, vitamins D and E, and lycopene have shown potential benefit in studies. Further studies are needed to confirm this [8].
Diet and Lifestyle: The effect of diet on prostate cancer risk is under study. A diet high in fat, especially animal fat, may be associated with an increased risk of prostate cancer. More studies are needed to determine if a low-fat diet with more fruits and vegetables helps prevent prostate cancer .
Studies show that a diet high in dairy products and calcium may be linked to an increased risk of prostate cancer, although the increase may be small [8].
Hormonal Prevention: Studies are underway to discover the role of certain drugs, such as finasteride, that reduce the amount of male hormone as preventive agents for prostate cancer [8].
Prostate cancer tends to grow slower than most other cancers, hence symptoms may not show in many cases until the disease has metastasized to other parts of the body. This makes yearly screening for prostate cancer extremely important.
Signs of Prostate cancer:
What prostate changes should you be aware of?
Growing older raises your risk of prostate problems. The three most common prostate problems are:
These changes, or an infection, can cause problems passing urine. Sometimes men in their 30s and 40s may begin to have these urinary symptoms and need medical attention. For others, symptoms aren't noticed until much later in life.
Patient's Perspective on Signs and Symptoms
Be sure to tell your doctor if you have any urinary symptoms like:
One change does not lead to another. For example, having prostatitis or an enlarged prostate does not raise your chance of prostate cancer. It is also possible for you to have more than one condition at the same time [9].
Patient's Perspective on Screening
Major medical associations and societies have issued conflicting recommendations regarding screening, making it difficult for an individual to decide if screening is right.
American Cancer Society, American Urological Association, and American College of Physicians recommend that men:
Us TOO Prostate Cancer Education and Support Group recommends that men have annual prostate examinations, which should include both a PSA blood test AND a digital rectal examination (DRE), starting at the following ages:
Moreover,
A PSA of 2.0 and over at any age should be investigated to rule out prostate cancer [12].
Arguments for screening — Experts in favor of prostate cancer screening cite the following arguments:
Arguments against screening:
Patient's Perspective on Blood test for Prostate Specific Antigen (PSA)
PSA is a protein secreted by the epithelial cells of the prostate gland including cancer cells; an elevated level in the blood indicates an abnormal condition of the prostate gland, either benign or malignant; it is used to detect potential problems in the prostate gland and to follow the progress of PC therapy [14]. PSA velocity and PSA doubling time are important markers that can indicate the existence of prostate cancer.
PSA velocity (PSAV) the calculation of the rate of increase in PSA levels in succeeding PSA tests; before diagnosis, a PSAV of 0.75 ng/ml/year (or higher) may be an indication of the presence of PC;
and PSA doubling time (PSADT) the calculation of the time it takes for the PSA value to double based on at least three values separated by at least three months each; before diagnosis, a PSADT of less than 10 years may be an indication of the presence of PC [14].
A first step in investigation of a PSA elevated at 2.0 or above should be a free-PSA percentage test. PSA readings that bounce up and down are more indicative of a benign process than a malignant process. A PSA that shows a persistent rise over time, particularly three consecutive rises three months apart, is suspicious for prostate cancer regardless of the PSA level. Any amount of PSA in excess of the measured benign-related PSA should be considered to have been produced by a malignant process until proven otherwise [12].
Free PSA are PSA molecules in the blood stream that are not "bound" to other proteins. Free PSA percentage test reports the percentage of free PSA, which is expressed based on free PSA divided by total PSA x 100. One study showed that men with free PSA % > 25% had low risk of PC while those with < 10% free PSA % were more likely to have PC [15] [16].
Patient's Perspective on Free PSA
Patient's Perspective on Digital Rectal Exam (DRE)
Digital Rectal Exam is a procedure where the doctor inserts a lubricated, gloved finger into the rectum and feels the prostate through the rectal wall. The prostate is checked for size, hard or lumpy areas and any pain caused by touching or pressing the prostate. The DRE allows the doctor to feel only one side of the prostate. The test lasts about 10-15 seconds.
This exam checks for:
The DRE allows the doctor to feel only one side of the prostate. A PSA test is another way to help your doctor check your prostate.
[2][17].
Transrectal ultrasound can be done in an office, and no sedation or anesthesia is needed. A small probe, about the size of a finger, is inserted into the rectum, and uses sound waves that bounce off the prostate to create an echo. A computer translates these echoes into an image (called a sonogram) of the prostate. About 80 percent of cancers have an abnormal ultrasound image. Transrectal ultrasound can also help to guide a surgeon to biopsy any area that appears abnormal [13].
Patient's Perspective on Transrectal Ultrasound
Transrectal ultrasound (TRUS) may facilitate diagnosis by directing needle biopsy; however, ultrasound is operator dependent and does not assess lymph node size. Moreover, a prospective multi-institutional study of preoperative TRUS in men with clinically localized prostate cancer felt to be eligible for radical prostatectomy showed that TRUS was no better than digital rectal examination in predicting extracapsular tumor extension or seminal vesicle involvement[18][19].
Patient's Perspective on Color Doppler
A new development in ultrasound involves the use of color Doppler imaging with microbubble contrast so that physicians are better able to determine the presence and exact location of a mass within the prostate. Doppler imaging can sense differences in velocity (i.e. blood flow versus solid tissue) and transmits these differences through different color pixels to create a picture on a screen. Microbubbles are tiny bubbles of gas that can permeate through small blood vessels without creating any harm. The microbubbles further enhance imaging by increasing the intensity of backscatter signal. Since blood vessels and blood flow are more prevalent in cancerous tissues than regular tissues, microbubbles tend to concentrate in the cancer, which is revealed on the created picture. This allows physicians to more accurately locate where biopsies should be taken [20].
Researcher from France recently conducted a clinical study to determine the effectiveness of contrast-enhanced color Doppler ultrasound using microbubbles in determining biopsy sites in men suspected of having prostate cancer. This trial included 85 men who underwent conventional Doppler and microbubble-enhanced color Doppler during the biopsy procedure. The results between the two were directly compared based on biopsy results. Contrast-enhanced color Doppler had a 93% detection rate of prostate cancer, compared with only 54% for un-enhanced color Doppler. Biopsies from areas of the prostate that did not contain cancer occurred in 21% of biopsies under Doppler that was not enhanced, compared with only 11% of biopsies under contrast-enhanced Doppler[20].
The researchers concluded that microbubble-enhanced color Doppler used for endorectal ultrasound improves the detection of prostate cancer and reduces unnecessary biopsies, compared to color Doppler that is not enhanced. They also state that this procedure is simple and not time consuming[20][22].
In the early 1990s, at about the same time that PSA testing was starting to gain widespread adoption, a young molecular biologist from Holland began post-doctoral work at The Brady Urological Institute of Johns Hopkins University. There, in the laboratory of William B. Isaacs, Marion Bussemakers performed studies on human prostate tissue using the technique of differential display, a then newly described method to identify gene expression in different tissues. During this series of experiments, an mRNA was discovered that appeared to be highly specific for prostate cancer[23] .
Patient's Perspective on PCA3
Recently, an additional new screening tool has become available. Bostwick Laboratories now offers the uPM3 test, the first urine-based genetic test for prostate cancer. uPM3 is based on PCA3, a specific gene that is profusely expressed in prostate cancer tissue. On average, the amount of PCA3 is 34 times greater in malignant prostate tissue than it is in benign prostate tissue. No other human tissues have ever been shown to produce PCA3. The uPM3 test predicts cancer as confirmed by prostate biopsy with 81% accuracy, compared to 47% accuracy for PSA. Therefore, after an elevated PSA, further investigations might reasonably include uPM3 testing to enhance the accuracy of diagnosis. Systematic biopsy of the prostate under ultrasound guidance, however, remains the definitive diagnostic procedure when clinical and/or laboratory findings indicate the possibility of prostate cancer[23].
Patient's Perspective on Prostate Biopsy
Prostate Biopsies involve excising cores of tissue from the prostate through the rectum, they should not be performed unless there is a persuasive indication that cancer might be present. Making the decision to biopsy [12]:
The biopsy is usually performed in a physician's office. Prior to the procedure, most men are given a course of antibiotics to reduce the risk of infection from the procedure. It is not usually necessary to stop eating or drinking before the biopsy. The man is positioned in the fetal position, lying on the side with the knees held against the chest. A urologist (a doctor who specializes in treatment of urinary, bladder, and prostate issues) performs the procedure[13] .
Before the biopsy, the physician injects the patient with a local anesthetic to numb the skin where the biopsies will be taken (either inside the rectum or at the perineum, the area between the penis and anus). An ultrasound probe (a thin wand) is inserted into the rectum to locate the prostate and guide the biopsies. A spring-loaded device is used to rapidly remove a 1/16 inch (2.5 mm) by 1/2 inch (20 mm) long cylinder of tissue from the prostate; this is usually repeated 12 times to ensure that tissues from the entire prostate are sampled. The entire procedure usually takes about 15 minutes [13].
The biopsy samples are then examined with a microscope by a pathologist. The results are usually available within one week. After the procedure, most men feel soreness in the rectum or perineum. Blood may be seen in the urine or semen.
Up to one in five men with a negative result on an initial biopsy will have cancer diagnosed after subsequent biopsies [13]. Imaging guided biopsies like the TRUS-guided needle biopsy [24] or Endorectal MRI with Spectroscopic guided biopsies can reduce the possibilities of a false negative result.
Patient's Perspective on Your Feelings
Learning that you have cancer can come as a shock. How did you react? You may have felt numb, frightened, or angry. You may not have believed what the doctor was saying. You may have felt all alone, even if your friends and family were in the same room with you. These feelings are all normal.
For many people, the first few weeks after diagnosis are very difficult. After you hear the word "cancer," you may have trouble breathing or listening to what is being said. When you are at home, you may have trouble thinking, eating, or sleeping.
People with cancer and those close to them experience a wide range of feelings and emotions. These feelings can change often and without warning. You will have many feelings after you learn that you have cancer. These feelings can change from day to day, hour to hour, or even minute to minute [25].
Some of the feelings you may go through include: denial, anger, fear, stress and anxiety, depression and sadness, guilt, loneliness
All these feelings are normal. You may feel like your life is out of control. There are ways you can be in charge:
Feeling hopeful is also normal. No one is cheerful all the time, but while you are dealing with cancer, hope can be an important part of your life [25].
Patient's Perspective on Family Matters
Families come in many forms. Some are husband, wife, and children. Others are life partners. Still others are groups of people who love and support each other [26].
No matter what form your family takes, your cancer will not only change your life, but also the lives of those around you.
Cancer impacts families in different ways [26].
As you think about how cancer has changed your life and your family's life, think about reaching outside your family to get help [26] .
Most families find that being honest and open about the cancer, about the problems that arise, and about their feelings, helps them handle the changes that cancer causes [26].
Patient's Perspective on Support Groups
Cancer support groups are meetings for people with cancer and those touched by cancer. These groups allow you and your loved ones to talk with others facing the same problems. Support groups often have a lecture as well as time to talk. Almost all groups have a leader who runs the meeting. The leader can be someone with cancer or a trained counselor.
You may think that a support group is not right for you. Maybe you think that a group won't help or that you don't want to talk with others about your feelings. Or perhaps you are afraid that the meetings will make you sad or depressed.
It may be good to know that many people find support groups very helpful. People in the groups often:
Prostate Cancer Support Groups:
Patient's Perspective on Choosing a doctor
You will have many factors to consider when choosing a doctor. To make an informed decision, you may wish to speak with several doctors before choosing one. When you meet with each doctor, you might want to consider the following[27]:
If you are choosing a surgeon, you may wish to ask additional questions about the surgeon’s background and experience with specific procedures. These questions may include:
It is important for you to feel comfortable with the specialist that you choose because you will be working closely with that person to make decisions about your cancer treatment. Trust your own observations and feelings when deciding on a doctor for your medical care [27].
Getting a Second Opinion
Once you receive your doctor’s opinion about the diagnosis and treatment plan, you may want to get another doctor’s advice before you begin treatment. This is known as getting a second opinion. You can do this by asking another specialist to review all of the materials related to your case. A second opinion can confirm or suggest modifications to your doctor’s proposed treatment plan, provide reassurance that you have explored all of your options, and answer any questions you may have [27].
Getting a second opinion is done frequently, and most physicians welcome another doctor’s views. In fact, your doctor may be able to recommend a specialist for this consultation. However, some people find it uncomfortable to request a second opinion. When discussing this issue with your doctor, it may be helpful to express satisfaction with your doctor’s decision and care, and mention that you want your decision about treatment to be as thoroughly informed as possible. You may also wish to bring a family member along for support when asking for a second opinion. It is best to involve your doctor in the process of getting a second opinion, because your doctor will need to make your medical records (such as your test results and x-rays) available to the specialist [27].
Some health care plans require a second opinion, particularly if a doctor recommends surgery. Other health care plans will pay for a second opinion if the patient requests it. If your plan does not cover a second opinion, you can still obtain one if you are willing to cover the cost[27].
Patient's Perspective on Staging
What does proper staging mean? Staging is determining the extent of disease. In the prostate cancer patient, proper staging means to assess the patient’s risk of having organ-confined disease vs capsular penetration vs seminal vesicle involvement vs lymph node involvement vs bone involvement. It is important to know the stage in order to plan treatment.
The following stages are used for prostate cancer:
As prostate cancer progresses from Stage I to Stage IV, the cancer cells grow within the prostate, through the outer layer of the prostate into nearby tissue, and then to lymph nodes or other parts of the body.
Stage I
In stage I, cancer is found in the prostate only. It cannot be felt during a digital rectal exam and is not visible by imaging. It is usually found accidentally during surgery for other reasons, such as benign prostatic hyperplasia. The Gleason score is low. Stage I prostate cancer may also be called stage A1 prostate cancer.
Stage II
In stage II, cancer is more advanced than in stage I, but has not spread outside the prostate. The Gleason score can range from 2-10. Stage II prostate cancer may also be called stage A2, stage B1, or stage B2 prostate cancer.
Stage III
In stage III, cancer has spread beyond the outer layer of the prostate to nearby tissues. Cancer may be found in the seminal vesicles. The Gleason score can range from 2-10. Stage III prostate cancer may also be called stage C prostate cancer.
Stage IV
In stage IV, cancer has metastasized (spread) to lymph nodes near or far from the prostate or to other parts of the body, such as the bladder, rectum, bones, liver, or lungs. Metastatic prostate cancer often spreads to the bones. The Gleason score can range from 2-10. Stage IV prostate cancer may also be called stage D1 or stage D2 prostate cancer.
Patient's Perspective on Gleason Score
Gleason score is given to prostate cancer based on it's microscopic appearance. It is the most widespread method of prostate cancer tissue grading used today, is the single most important prognostic factor in PC. The Gleason score is important because higher Gleason scores are associated with cancer which is more aggressive. To assign a Gleason score, a piece of prostatic tissue must be obtained either by sampling the gland with a needle introduced through the rectum (Transrectal biopsy) or by removing the gland (prostatectomy).
The Gleason score ranges from two to ten. A Gleason score of two is associated with the best prognosis and a score of ten with the worst. The final score is a combination of two different scores which each range from one to five. Gleason scores are associated with the following features:
A pathologist examines the biopsy specimen and attempts to give a score to the two patterns. First called the primary grade, represents the majority of tumor (has to be greater than 50% of the total pattern seen). Second - a secondary grade - relates to the minority of the tumor (has to be less than 50%, but at least 5%, of the pattern of the total cancer observed). These scores are then added to obtain the final Gleason score. For example, a prostate biopsy specimen may exhibit two different patterns, one which is assigned a number two and the other a number three. The final Gleason score in this case would be five.
Together with other parameters, the Gleason score is incorporated into a strategy of prostate cancer staging which predicts prognosis and helps guide therapy; prognosis refers to the expected biologic aggressive potential of a patient’s PC to spread to other organs. Hence, once the diagnosis of prostate cancer is made on biopsy, tumor grading, especially the Gleason score, strongly influences decisions regarding options for therapy [13].
Patient's Perspective on Partin Table
The Partin Tables represent one of the many algorithms that can help to establish probabilities as to the extent of progression of prostate cancer. In 1993, Dr. Alan Partin, et al1 examined medical records of 703 patients with clinically localized disease who underwent a radical prostatectomy between 1982 and 1991. They compared pre-operative findings for:
with post-surgical findings of organ-confined disease (OCD), extraprostatic extension, seminal vesicle invasion and lymph node invasion. Using this data, they developed a model that could help predict the pathological stage in a newly diagnosed patient with clinically localized PC[28].
In 2001, the Partin Tables were updated based on a larger series of 5079 men treated with prostatectomy between 1994 and 2000 at Johns Hopkins Hospital. The 2001 Partin Table interactive calculator is available from John Hopkins James Buchanan Brady Urological Institute
The primary value of the updated Partin Tables is for “counseling patients regarding the probability of their tumor being a specific pathologic stage, rather than a strict decision-making tool”. The tables may help a patient determine whether it is advisable to undergo definitive local therapy in the hopes of curing his cancer. Results from the tables may also suggest the patient consider further laboratory, radiological or pathological testing to attempt to determine if the cancer has spread beyond the prostate gland[28].
Patient's Perspective on Radionuclide Bone Scan
A procedure to check if there are rapidly dividing cells, such as cancer cells, in the bone.
A very small amount of radioactive material is injected into a vein and travels through the bloodstream. The radioactive material collects in abnormal cells in the bones.
As the patient lies on a table that slides under the scanner, the radioactive material is detected and images are made on a computer screen or film [29]
A computed tomography scan (CT scan, also called a CAT scan) uses computer-controlled X-rays to create images of the body.
Patient's Perspective on CT/CAT Scan
A CT scan is three-dimensional. By imaging and looking at several three-dimensional slices of a body (like slices of bread) a doctor could not only tell if a tumor is present, but roughly how deep it is in the body. A CT scan can be three dimensional because the information about how much of the X-rays are passing through a body is collected not just on a flat piece of film, but on a computer. Conventional CT scans take pictures of slices of the body (like slices of bread).
These slices are a few millimeters apart. The newer spiral (also called helical) CT scan takes continuous pictures of the body in a rapid spiral motion, so that there are no gaps in the pictures collected. [31].
A dye may be injected into a vein or swallowed to help the organs or tissues show up more clearly. This procedure is also called computed tomography, computerized tomography, or computerized axial tomography [29][31].
Patient's Perspective on Endorectal MRI with Spectroscopic
Magnetic resonance imaging (MRI) is a technology where a large magnet is used to create images of various tissues in the body that a Radiologist can use to diagnose any abnormalities[32].
Prostate MRI is most powerful when obtained with an endorectal coil. The technique has demonstrated higher accuracy than other modalities in assessing seminal vesicle invasion and extra-capsular extension (ECE) of prostate cancer (96% and 81% respectively). Endorectal coil MRI is useful for determining the extent of spread and local invasion of cancers of the prostate, rectum, and anus.[33]
This coil is placed in the rectum at the start of the exam. Similar to ultrasound probe, the coil is placed rectally because it provides the greatest amount of signal when placed near the gland. This increased signal from the endorectal coil helps to provide excellent resolution (image quality)[32].
The endorectal coil, sometimes called a balloon coil, has a flexible shaft with a small balloon on one end. Once inserted, the balloon is filled with either air or a special liquid until it comes into contact with and conforms to the size and shape of the prostate. It is not painful, however, it may cause some initial discomfort[32].
The total exam time is about 40 minutes. You may be asked to restrict your diet for a short period prior to the exam[32].
Magnetic Resonance Spectroscopic Imaging (MRSI)
MRSI is the combination of endorectal MRI with spectroscopy, spectroscopy observes specific resonances (peaks) for citrate, choline and creatine from contiguous small volumes throughout the gland. The amount of choline and citrate is used as a differential test to confirm findings of MRI.
The use of endorectal MRI with spectroscopy has demonstrated high specificity in identifying cancer [35].
Video of patient experience courtesy of Us TOO Prostate Cancer Education & Support[36].
The positron emission tomography (PET) scan creates computerized images of chemical changes, such as sugar metabolism, that take place in tissue. Typically, the patient is given an injection of a substance that consists of a combination of a sugar and a small amount of radioactively labeled sugar. The radioactive sugar can help in locating a tumor, because cancer cells take up or absorb sugar more avidly than other tissues in the body [31].
After receiving the radioactive sugar, the patient lies still for about 60 minutes while the radioactively labeled sugar circulates throughout the body. If a tumor is present, the radioactive sugar will accumulate in the tumor. The patient then lies on a table, which gradually moves through the PET scanner 6 to 7 times during a 45-60-minute period. The PET scanner is used to detect the distribution of the sugar in the tumor and in the body. By the combined matching of a CT scan with PET images, there is an improved capacity to discriminate normal from abnormal tissues. A computer translates this information into the images that are interpreted by a radiologist [31].
PET scans may play a role in determining whether a mass is cancerous. However, PET scans are more accurate in detecting larger and more aggressive tumors than they are in locating tumors that are smaller than 8 mm and/or less aggressive. They may also detect cancer when other imaging techniques show normal results. PET scans may be helpful in evaluating and staging recurrent disease (cancer that has come back). PET scans are beginning to be used to check if a treatment is working - if a tumor cells are dying and thus using less sugar [31].
Patient's Perspective on Positron Emission Tomography (PET) Scan
Positron emission tomography (PET) using 18F-fluorodeoxyglucose (FDG) does not adequately detect local recurrence after radical prostatectomy, due to the low metabolic activity of prostate cancer and interference with normal urinary activity in the bladder.[38] PET only has a role in evaluating aggressive advanced prostate cancer. As a result, a more accurate and more sensitive non-invasive test, perhaps used in combination with existing tests, is needed [39].
Patient's Perspective on Single Photon Emission Computed Tomography (SPECT) scan
Similar to PET, single photon emission computed tomography (SPECT) uses radioactive tracers and a scanner to record data that a computer constructs into two- or three-dimensional images. A small amount of a radioactive drug is injected into a vein and a scanner is used to make detailed images of areas inside the body where the radioactive material is taken up by the cells. SPECT can give information about blood flow to tissues and chemical reactions (metabolism) in the body [31].
In this procedure, antibodies (proteins that recognize and stick to tumor cells) can be linked to a radioactive substance. If a tumor is present, the antibodies will stick to it. Then a SPECT scan can be done to detect the radioactive substance and reveal where the tumor is located [31].
Image of a SPECT scan on the right. It shows high levels of antibody in pelvis and axilla (red) and uptake in skin of the thigh and right shoulder (green) showing areas of cutaneous T-cell lymphoma [37]
Patient's Perspective on ProstaScint scan
ProstaScient is an imaging tool in which a radioactive isotope is attached to an antibody, called monoclonal antibody (mAb). The isotope-monoclonal antibody is injected into the bloodstream and seeks that specific cancer protein called prostate-specific membrane antigen (PSMA)associated with prostate cancer and attaches to it. Four days later, the patient is scanned with a SPECT camera that detects gamma radiation emitted by the isotope-mAb-protein sandwich, which serves to localize the cancer protein.
Why do you need ProstaScint?
Who needs ProstaScint?
It should be understood, however, that because ProstaScint imaging has been reported in some articles to have a false positive rate as high as 20%, patients with a low risk of nodal metastases are not appropriate candidates for this type of study. On the other hand, men who have an intermediate to high risk of nodal metastases are considered to be more appropriate candidates[39].
ProstaScint Fusion Imaging with CT or MRI
Fusion imaging combines ProstaScint imaging with CT or MRI imaging and co-registers the images to provide a uniquely detailed fusion image of high diagnostic quality. In order to optimize information obtained from ProstaScint imaging, it is now recommended that all studies be performed with either CT or MRI fusion [39].
Patient's Perspective on Prognosis
The prognosis (chance of recovery) and treatment options depend on the following:
Prognosis also depends on the Gleason score and the level of PSA.
Patient's Perspective on Prostatic Acid Phosphatase (PAP)
Prior to the PSA, the major biomarker of prostatic cancer was the prostatic acid phosphatase, or PAP, which is laboratory blood test like the PSA. Many physicians have discarded the PAP while many others still use it as a differential tool in their strategic analysis of the patient. In their experience, the PAP is an important baseline test since it has predictive value regarding the success or failure of RP or RT [43].
In a study by Moul et al [44], the PAP is useful for predicting the risk of PSA recurrence after a radical prostatactomy :
| Baseline PAP (bPAP)/(ng/ml) | PSA Recurrance at 4 years |
|---|---|
| < 3 | 21.2% |
| > 3 | 61.3% |
PAP maybe elevated due to trauma caused by prostate biopsies, DRE or sexual activity involving ejaculation. You should wait at least 5 weeks after a prostate biopsy and 48 hours after a DRE or sexual activity involving ejaculation before taking a PAP test [45] .
Patient's Perspective on DNA Ploidy
An analysis of the tumor cells DNA content, or ploidy, is a valuable prognostic tool. Normal DNA is comprosed of a pair of chromosome, and is thus termed "diploid." Diploid status is more commonly associated with tumors of a low to moderate Gleason score, whereas abnormal ploidy (aneuploid) status is more commonly associated with tumors of a higher Gleason score. However, this is not a hard and fast rule[46].
The importance of ploidy as an independent prognostic factor is clearly demonstrated by Lerner, et al[47]. In this paper, Lerner, et al examined the 5-year relapse rates in patients undergoing RP and having "apparent" organ confined disease. When the data were analyzed below with respect to PSA, GS and ploidy status, a significantly higher rate of disease relapse was seen in patients with non-diploid tumors[46].
| PSA | Gleason | Diploid | Anuploid | Tetraploid | Unknown |
|---|---|---|---|---|---|
| < 10ng/ml | 5 | 8% | 15% | - | 10% |
| 6 | 15% | 30% | - | 16% | |
| 7 | 30% | 42% | - | 34% | |
| 8-10 | 42% | 61% | - | 34% | |
| > 10ng/ml | 5 | 15% | 30% | - | 16% |
| 6 | 30% | 61% | 42% | 34% | |
| 7 | 42% | 61% | - | 34% | |
| 8-10 | 61% | 61% | - | 59% |
Patient's Perspective on Treatment
There are many available treatment options for prostate cancer. The type of treatment that you or your loved one receives will be based on the stage of prostate cancer. You should work together with your doctor to weigh the risks, advantages, and disadvantages of each option and its side effects and determine what treatment is right for you or your loved one[48].
If you have been diagnosed with:
Patient's Perspective on Watchful Waiting
Watchful waiting is often called "active surveillance" or "observation" and means that you decide to have no active treatment now. Your doctor will want to follow you closely to look for any signs that the disease may be changing. You will have tests like the ones you've already had such as digital rectal exams, PSA tests, and repeat biopsies. You can change your mind and decide to have treatment at any time. Watchful waiting is based on the fact that many early-stage prostate cancers grow so slowly that they may never cause problems or become life threatening. In some cases, it may be a way to avoid the harms of treatment without shortening life expectancy. Or it can be a decision based on your age and other serious health problems - older men in their 70s and 80s may not have the same views about undergoing surgery or radiation therapy as younger men [49].
Patient's Perspective on Surgery
Surgery is often a treatment choice for men who have early-stage prostate cancer and are in good health. Surgery to remove the prostate is called prostatectomy (PRAHS-ta- TEK-toe-mee). There are two approaches that are typically used by surgeons: Open(Retropubic) prostatectomy or Laproscopic Prostatectomy. The newest type of surgery to remove the prostate is called Robotic-Assisted Laparoscopic surgery (da Vinci)[49] [48].
Advantages of Prostatectomy
Disadvantages of Prostatectomy
Patient's Perspective on Radical Retropubic Prostatectomy
Your surgeon can remove the prostate through an incision just above the pubic bone in your lower abdomen[49].
Patient's Perspective on Radical Perineal Prostatectomy
This type of surgery, which is not used as often, reaches the prostate through an incision between your scrotum and anus.With this method, your surgeon is not able to check the lymph nodes for cancer. It is also more difficult to spare the nerves that control erections. This approach is used when the cancer is confined to the prostate [49].
Patient's Perspective on Laprascopic Prostatectomy
Laparoscopic surgery is a new type of surgery to remove the prostate. It is done with smaller incisions using a slender tube with a camera on the end (laparoscope) that provides 3D images of the interior of the body. The scope is inserted through the navel, and the surgeon can see a highly enlarged image of the prostate. Other long instruments are used to assist with the removal of the prostate through 4-5 small slit (1 inch) incisions. Compared with other types of prostatectomy, this technique may lead to shorter hospital stays, faster recovery, and less blood loss and pain [49][48].
Patient's Perspective on Robotic-Assisted Laprascopic Prostatectomy
Recent developments in the field of surgical robotics have ushered in a new era of minimally invasive surgery that now challenges conventional open surgery.
The robotic surgical team includes both console-side and patient-side surgeons. The operating surgeon sits at the console, and is not scrubbed. After the patient-side team is scrubbed, they place the ports, present the operative field to the operating surgeon, and use suction to keep the field clean[50].
Patient's Perspective on Cryosurgery (Cryo)
Cryosurgery freezes and thaws tissue to kill prostate cancer with the surgeon being guided by ultrasound. Also called cryotherapy, it is often used when the prostate has more advanced, yet still confined disease, and when surgery is not an option. The prostate is not removed with this approach[49].
Cryosurgery can result in injury to the rectum, incontinence, swelling of the scrotum, pain or numbness in the penis, or blocked urine flow. In 1 in 200 cases, a hole (called a fistula) appears between the rectum and prostate. Results depend highly on the doctor's skill and experience. Success rates may not be as high as with prostatectomy or with any form of external beam radiation therapy. Long-term results for this type of treatment are not yet known [49].
Advantages of Cryosurgery
Disadvantages of Cryosurgery
Patient's Perspective on Radiation Therapy
This type of treatment uses high-energy rays (eg, x-rays) or particles (eg, electrons or protons) to kill prostate cancer cells or prevent cancer cells from growing and spreading. Radiation therapy is an option when cancer is in your prostate but has not spread to other organs (Stage T1 and T2). It is also used when you cannot have surgery because of your age, health, or personal choice.
Radiation therapy is often used in combination with hormone therapy if cancer cells have spread beyond the prostate (Stage T3). Radiation therapy may be used for pain relief in prostate cancer that is no longer responding to hormone therapy and has spread to other tissues in the body, primarily bones (Stage M+)[48][49].
Radiation therapy techniques:[48]
External Beam Radiation Therapy (EBRT): radiation is generated and administered by a machine outside the body, usually in brief daily sessions for several weeks.
Internal Radiation Therapy:also called brachytherapy uses radiation that is placed very close to or inside the tumor. The radiation source is usually sealed in a small holder called an implant. Implants may be in the form of thin wires, plastic tubes called catheters, ribbons, capsules, or seeds. The implant is put directly into the body. Internal radiation therapy may require a hospital stay.
Advantages of Radiation Therapy
Disadvantages of Radiation Therapy
Patient's Perspective on 3-D Conformal Radiation Therapy
Traditionally, the planning of radiation treatments has been done in two dimensions (width and height)[52]. Radiation doses delivered to the prostate gland have been limited by the toxicity to the rectum and bladder in the conventional external beam radiation therapy (EBRT)[53].
Three-dimensional (3D) conformal radiation therapy uses computer technology to allow doctors to more precisely target a tumor with radiation beams (using width, height, and depth). Many radiation oncologists use this technique. A 3D image of a tumor can be obtained using computed tomography (CT), magnetic resonance imaging (MRI), positron emission tomography (PET), or single photon emission computed tomography (SPECT). Using information from the image, special computer programs design radiation beams that “conform” to the shape of the tumor. Because the healthy tissue surrounding the tumor is largely spared by this technique, higher doses of radiation can be used to treat the cancer[52].
A clinical study shows that 90% patients that were receiving higher doses of radiation achieved an optimal response, compared to 58-76% in patients that received a lower dose. The results of this clinical study suggest treatment with high-dose 3D-CRT for localized prostate cancer is safe and feasible, and may result in improved local control of disease[53].
Patient's Perspective on Intensity Modulated Radiation Therapy (IMRT)
IMRT has revolutionized the delivery of radiation therapy. IMRT is a new type of 3D conformal radiation therapy that uses radiation beams of varying intensities to deliver different doses of radiation to small areas of tissue at the same time. The technology allows for the delivery of higher doses of radiation within the tumor and lower doses to nearby healthy tissue. Some techniques deliver a higher dose of radiation to the patient each day, potentially shortening the overall treatment time and improving the success of the treatment. IMRT may also lead to fewer side effects during treatment[52].
IMRT is a combination of
There are literally thousands of beamlets or “pencil beams” coming from every conceivable direction to create radiation dose shapes never before possible. The process involves the physician outlining all the structures in the anatomical area on each 1 mm slice of the CT scan or MRI scan of the patient’s prostate. More recently, fusion of the two scans occurs with sophisticated software to create the most accurate representation of the patient’s anatomy (Figures 1-2). [54].
The radiation is delivered by a linear accelerator that is equipped with a multileaf collimator (a collimator helps to shape or sculpt the beams of radiation). The equipment can be rotated around the patient so that radiation beams can be sent from the best angles. The beams conform as closely as possible to the shape of the tumor. Because IMRT equipment is highly specialized, not every radiation oncology center uses IMRT[52].
| 3-D Conformal | IMRT |
|---|---|
| uses forward planning treatment which sets the fields of radiation and then adjusts the dose weighting and delivery, by trial and error, to refine the radiation plan. This method is thought to be accurate within 7 to 10 milimeters[54]. | uses inverse planning treatment which sets a dose for the tumor/target volume and restricts the dose amount to adjacent structures. It is considered to be accurate within 1-3 millimeters[54]. |
| In a report by Zelefsky et al, patients were treated to doses of 8100cGy: Grade 2 rectal toxicity of 13% and Grade 3 rectal toxicity of 2% [55] | In a report by Zelefsky et al, patients were treated to doses of 8100cGy: Grade 2 rectal toxicity of 0.5% and Grade 3 rectal toxicity of 0.5% [55]. |
Reported rates of long-term side effects from 3D-Conformal radiation are 2-3 times those reported with IMRT. IMRT represents the most refined and precise form of 3D-Conformal treatment. The long experience with 3D-Conformal provides an important foundation for implementing IMRT [54].
Patient's Perspective on Proton Beam Therapy (PBT)
Proton therapy is the most precise and advanced form of radiation treatment today. It primarily radiates the tumor site, leaving surrounding healthy tissue and organs intact. Conventional x-ray radiation often radiates healthy tissue in its path and surrounding the tumor site. Chemotherapy moves throughout the entire body, unlike radiation and surgery which are considered "site specific" treatments[56].
Proton Therapy was first proposed in 1954, but primarily had been available for very limited use. There was no hospital-based treatment centers in the world until the Proton Treatment Center opened in 1990 at Loma Linda University Medical Center. Most radiation oncologists know about proton therapy, but have not had experience working with the proton technology, making it difficult for them to advise patients on this form of treatment. But the benefits of proton treatment are expanding to other regions of the USA, including the southwest, midwest, southeast, and mid-atlantic[56].
A recent study at Loma Linda University concludes that when higher doses of conformal proton therapy are delivered at the target site, the results show a "low incidence of side effects" compared to conventional radiation[56].
Proton therapy has minimal to no side effects, compared to conventional forms of radiation. Hence it is much more easily tolerated than standard radiation therapy. Tumors like Prostate cancer that are localized and have not spread to distant areas of the body are the best candidate for Proton therapy[56].
Proton therapy can take anywhere from one day to seven weeks depending on the tumor site. The length of treatment time will also decrease over time as heavier doses begin to increase[56].
Nearly all insurance providers nationwide cover proton therapy as does the U.S. medicare program. Proton therapy costs more than conventional radiation, but generally less than surgery[56].
Nearly all insurance providers nationwide cover proton therapy as does the U.S. medicare program. Proton therapy costs more than conventional radiation, but generally less than surgery[56].
"Unlike conventional radiation," says Dr. Jerry Slater, Clinical Director of Loma Linda's Proton Therapy Center, " proton radiation has a well-defined high-dose area which can be manipulated to precisely surround an irregularly shaped target such as the prostate gland. This inherent characteristic of protons allows very little scatter to the bladder and rectal areas, higher doses to the prostate, and significantly less side effects[56]."
Video on new prostate cancer treatment Proton Therapy courtesy of The National Association for Proton Therapy [56]
Patient's Perspective on High Dose Radiation (HDR) Brachytherapy
HDR brachytherapy is a short-term internal beam therapy that uses higher dosage, non-permanent seeds. Because the seeds are implanted for a much shorter amount of time (approximately 1 hour), there is less likelihood of them migrating in the body[48].
There are four basic steps to HDR brachytherapy. They are
Advantages of HDR Brachytherapy:[57]
HDR is reliable in treating both early stage prostate cancer as well as early intermediate stage that extends beyond the prostate. HDR brachytherapy has a “scaffolding matrix” feature that provides both general stability and the ability to place catheters at or beyond the prostate capsule and into the seminal vesicles without the concern for source loss or migration to other organs[57].
Figure 3 shows the 100% therapeutic isodose line extending beyond the prostate capsule. High local tumor control rates in all risk groups confirm the efficacy of HDR to control disease both in and around the prostate[58][59].
As shown in Table 7, the results of HDR monotherapy for low-risk and early intermediate-risk groups in the literature are excellent[60][61][62]. A study of 294 patients from CET and William Beaumont Hospital showed the 5-year control rates to be 94%, the cause-specific survival to be 100%, and the fact that no patients had distant metastasis. The rectal complication rates were < 1% and there were < 5 % grade 3 urinary complications[57].
Patient's Perspective on Brachytherapy (Seeds)
Seed implantation is a type of internal radiation therapy. Radiation is delivered inside your body by implanting tiny seeds in your prostate. Usually 40 to 130 seeds are inserted into the prostate, depending on the size of your prostate. Each seed has a small amount of radioactive material that emits radiation within an inch of its surroundings. Low-dose seeds are left in the prostate permanently, although their radiation lasts for only 3 to 6 months. This procedure is usually done on an outpatient basis, without a hospital stay[49].
In recent years, seed implantation has become more popular as a treatment option. It has been estimated that up to 50% of patients with early stage prostate cancer are now receiving ultrasound-guided seed implantation[63][64].
This rise in popularity is most likely due to
Low energy of I-125 (Iodine 125) and Pd 103 (Palladium 103) isotopes dose falls off quickly with distance and, therefore, the seeds deliver low doses to the adjacent rectum and bladder[64].
The ultrasound-guided transperineal approach resulted in relatively even distribution of seeds throughout the prostate; this marked a major advance in prostate brachytherapy in that it minimized the need for external beam radiation and allowed more precise planning of the implant prior to the procedure. These advances also significantly increased the accuracy of seed placement and insured that the prostate would receive the proper number, strength, and positioning of radioactive sources. Derivatives of this technique are in wide use today.(see Figure 1)
Steps for Seed Implantation process:
1. Patient selection
2. Treatment planning
3. Seed implantation
4. Post-Operative evaluation
Patient's Perspective on High-Intensity Focused Ultrasound
HIFU: is a medical device piloted by a computer designed to treat localized prostate cancer using high intensity focused ultrasound (HIFU)[48].
What is HIFU?
What Do the Clinical Studies Show?
Is HIFU a Proven Therapy?
Advantages of HIFU
Disadvantages of HIFU
Patient's Perspective on Hormone Therapy/Androgen Deprivation Therapy (ADT)
Prostate Cancer is an Endocrine-Related Malignancy. Hormone Therapy or Androgen Deprevation Therapy (ADT) is essentially depriving the tumor cell of a necessary growth substance - androgen (Testosterone, 5α-dihydrotestosterone (DHT), dehydroepiandrosterone (DHEA), dehydroepiandrosterone sulfate (DHEA-S), and androstenedione). Most patients with PC will show some response to ADT. The degree of response is related to the tumor cell population being either androgen-dependent PC (ADPC) or androgen-independent PC (AIPC) and whether or not the testosterone level has been reduced to castration levels of below 20 ng/dl or below 0.69nM/L [71].
ADT is often recommended for patients who are planning treatment with EBRT, brachtherapy or cryosurgery. This is most common in settings where the prostate gland volume is too large to be effectively treated without the risk of excessive radiation scatter to the bladder and rectum. ADT can reduce gland volume, making local therapies more effective and reduce side effects[72].
EBRT of any kind, brachytherapy and cryosurgery are all cancer volume dependent therapies. If the volume of the cancer and/or gland is too large, these treatments will be less effective and in some cases completely ineffective. ADT, therefore is often used prior to and during these treatments[72].
Some patients initiate ADT to buy time to research their options for standard primary therapies of Radical Prostatectomy, Radiation therapy or cryosurgery[72].
Hormonal Pathways of Prostate Cancer
An understanding of the hormonal pathways involved in prostate cancer (PC) is important in the management of this disease. Knowledge of the biochemical steps that lead to testosterone and dihydrotestosterone (DHT) synthesis may allow for therapeutic maneuvers that can result in more complete androgen blockade[73].
What are the different types of Hormone Therapy ?
Single Hormone Blockade - Hormone Therapy typically employs a drug called LHRH agonist or LHRH-A (luteinizing hormone-releasing hormone agonist) which ultimately involves turning off a pituitary hormone called luteinizing hormone (LH) that normally stimulates the testicles to make testosterone. LHRH agonist currently being used are Leuprolide acetate (Lupron®), Goserelin acetate (Zoladex®) or Triptorelin pamoate (Trelstar® LA)[71].
LHRH antagonist drug can be used in place of LHRH agonists to reduce the testosterone level in the body. LHRH antagonists work by directly inhibiting LHRH so that there is no more production of testosterone. In contrast, the LHRH analogs stimulate the LHRH receptor and cause initial production of testosterone for one to two weeks which is then exhausted[48]. LHRH antagonists currently being used are Abarelix.
Double Hormone Blockade - typically uses LHRH agonist + an Anti-androgen drug. Anti-androgen drugs block androgen receptors and prevents T and DHT from stimulating Prostate Cancer growth. Anti-androgen drugs currently being used are Bicalutamide (Casodex®), Flutamide (Eulexin®), Nilutamide (Nilandron®, and Cyproterone acetate (Androcur®)[71].
Triple Hormone Blockade - uses three agents, LHRH agonist + Anti-androgen + 5-alpha reductase (5-AR) inhibitor. 5-AR inhibitor blocks conversion of testosterone to DHT (dihydrotestosterone) which is a more potent prostate cancer growth stimulator than testosterone. 5-alpha reductase (5-AR) inhibitor drugs currently being used are Finasteride (Proscar®) and Dutasteride (Avodart®)[71].
Patients who exhibit progressive disease and who were initially treated with monotherapy using an LHRH agonist or orchiectomy, should consider the use of combination finasteride (Proscar) + flutamide (Eulexin).The pros and cons of for specific drugs to be used individually or in combination need to be throughly discussed with your doctor[71].
Orchiectomy is an operation that removed the testicles, which produces 95% of the body's testosterone[48].
Estrogen Therapy Administration of estrogen hormones lowers testosterone production and has some direct apoptotic effects on both androgen-dependent and androgen-independent prostate cancer cells. Estrogen drugs currently being used are diethylstilbestrol (DES), Stilphosterol® (stilbestrol diphosphate), Honvan® (fosfestrol tetrasodium), Estradurin® (polyestradiolphosphate), Estraderm® patch (estradiol)-only a small scale trial has investigated the benefit of delivering estrogen through the skin to block testosterone production in men with prostate cancer. In that study, the patch was successful in reducing testosterone levels, with fewer cardiovascular or other side effects (gynomastia). Phase III trials are currently comparing the effects of patch and injected forms of estrogen in men with prostate cancer[48].
P450 Enzyme Inhibitors The P450 enzymes are involved in the synthesis of several hormones, including testosterone, that stimulate prostate cancer cell growth. Inhibitors of these enzymes can decrease the levels of testosterone and adrenal androgens, and have direct cytotoxic effects on prostate cancer cells.
P450 Enzyme inhibitors currently being used are Ketoconazole (Nizorol®)[48].
Common side effects of hormone therapy:
(listed in order of most to least common)
Videos
| Click Image to play video | Topic | Presenter(s) |
|---|---|---|
 | Management of Side Effects Related to ADT Video | Richard Lam, MD |
| Hormonal Therapy of Prostate Cancer At All Stages Video | Steven Tucker, MD |
Patient's Perspective on Chemotherapy
Prostate cancer that is no longer responsive to hormone therapy is referred to as hormone-resistant prostate cancer or androgen-independent prostate cancer. There is currently no cure for hormone refractory prostate cancer. However, several therapies can extend life and reduce pain and discomfort. Treatment of hormone-resistant prostate cancer that has metastasized (Stage N+ and M+) may require systemic radiation therapy or chemotherapy[48].
Chemotherapy is a cancer treatment that uses drugs to stop the growth of cancer cells, either by killing the cells or by stopping them from dividing. When chemotherapy is taken by mouth or injected into a vein or muscle, the drugs enter the bloodstream and can reach cancer cells throughout the body (systemic chemotherapy). When chemotherapy is placed directly into the spinal column, an organ, or a body cavity such as the abdomen, the drugs mainly affect cancer cells in those areas (regional chemotherapy). The way the chemotherapy is given depends on the type and stage of the cancer being treated [29].
Chemotherapy is the administration of powerful toxic drugs that circulate throughout the body and eliminate rapidly growing cancer cells. Chemotherapy also affect rapidly growing healthy cells, which can lead to side effects hence it is reserved for patients with advanced stage cancer (Stage M+) that does not respond to hormone therapy.
Advantages of Chemotherapy:
Disadvantages of Chemotherapy:
Currently available chemotherapy drugs:
Videos
| Click Image to play video | Topic | Presenter(s) |
|---|---|---|
| Treating Androgen Independent PC Without Chemotherapy Video | Mark Scholz, M.D. |
| Chemotherapy for Prostate Cancer Video | Jacek Pinski, MD, PhD |
| Novel Therapies for Prostate Cancer The Future is Now Video | Mitchell Gross, MD, PhD |
Patient's Perspective on Anemia
Anemia of androgen deprivation may occur especially in men > 73. Anemia if severe or symptomatic can be treated with Epogen or Procrit[73].
Patient's Perspective on Muscles wasting
Muscle wasting with prolonged use > 1 year of hormone therapy can be diminished or prevented by exercise and weight lifting[73].
Patient's Perspective on Hot Flashes
Hot flashes can be treated with homeopathic agents like Lachesis or Chinese herbs like TCB 3 and TCB 7. If patients are severely affected the use of depo-provera injection can be considered after discussion with the patient about potential concerns of the use of a progestin. This concern may not be justified but should be explored. The injection of depo-provera, 200-400 mg im can eliminate hot flashes. The issue is whether the effect of this drug is due to its metabolism to androstenedione or to an effect on a receptor that involves the mechanism for hot flashes i.e. the LHRH receptor. Perhaps depo-provera may stabilize the LHRH receptor[73].
Patient's Perspective on Osteoporosis/Arthritis
Hormone therapy may cause arthritic symptoms possibly due to acute osteoporosis. Osteoporosis/Arthritis may be prevented and treated with
Patient's Perspective on Memory Loss
Memory loss could possibly be helped by the use of Gingko at 60 mg three times a day. Agents such as Hydergine could be used as well as Nicotine gum to increase cerebral blood flow. Other smart drugs such as Deprenyl, Piracetam or Vinpocetin could be tried. Clinical studies are needed[73].
Patient's Perspective on Weight Gain
Cholesterol/triglyceride increases could be managed by exercise and a low fat diet[73].
Patient's Perspective on Rectal Irritation
Erectile dysfunction (ED) has been a major problem because a high percentage of men treated with radical prostatectomies, radiation therapy, and cryosurgery have traditionally become impotent as a result[74] .
Erectile dysfunction can be treated with:
Patient's Perspective on Erectile Dysfunction
Patient's Perspective on Incontinence
Loss of bladder control (urinary incontinence) after prostate surgery is a devastating complication, which has a significant negative impact on quality of life. Normally, as the bladder fills to capacity, there is very little change in bladder pressure and the sphincter remains closed allowing the man to stay dry. When incontinence occurs following prostatectomy, this normal balance of bladder and sphincter function is disturbed[77].
Three main causes of post-prostatectomy incontinence (ppi) based on urodynamic findings in men with ppi:
Treatment for post-prostatectomy incontinance related to high bladder pressure:
Treatment for post-prostatectomy incontinance related to sphincter damage:
Options for treatment of sphincter damage include biofeedback, injection therapy (which is generally not successful), the artificial urinary sphincter, and more recently the male sling procedure.
Patient's Perspective on LHRH agonist
LHRH (Luteinizing hormone-releasing hormone) agonist can prevent the testicles from producing testosterone.
Patient's Perspective on Leuprolide Acetate (Lupron®, Viadur®)
The acetate salt of a synthetic nonapeptide analogue of gonadotropin-releasing hormone. Leuprolide binds to and activates gonadotropin-releasing hormone (GnRH) receptors. Continuous, prolonged administration of leuprolide in males results in pituitary GnRH receptor desensitization and inhibition of pituitary secretion of follicle stimulating hormone (FSH) and luteinizing hormone (LH), leading to a significant decline in testosterone production; in females, prolonged administration results in a decrease in estradiol production. This agent reduces testosterone production to castration levels and may inhibit androgen receptor-positive tumor progression [79].
| Synonyms | Leuprorelin, Leuprorelin Acetate |
| US brand names | Lupron,Lupron Depot, Lupron Depot-3 Month, Lupron Depot-4 Month, Lupron Depot-Ped, Viadur®, Eligard® |
| Foreign brand names | Carcinil, Enanton, Enantone, Enantone-Gyn, Ginecrin, Leuplin, Lucrin, Lucrin Depot, Procren, Procrin, Prostap, Trenantone, Uno-Enantone |
Patient's Perspective on Goserelin acetate (Zoladex®)
A synthetic decapeptide analog of luteinizing hormone-releasing hormone (LHRH) with antineoplastic activity. Goserelin binds to and activates pituitary gonadotropin releasing hormone (GnRH) receptors. Prolonged administration of goserelin inhibits the secretion of pituitary gonadotropin, thereby decreasing levels of testosterone (in males) and estradiol (in females). Administration of this agent in a depot formulation may result in the regression of sex hormone-sensitive tumors and a reduction in sex organ size and function [79].
| US brand names | Zoledex |
Patient's Perspective on Triptorelin pamoate (Trelstar® LA)
The pamoate salt of triptorelin, a synthetic decapeptide agonist analog of luteinizing hormone releasing hormone (LHRH). Possessing greater potency than endogenous LHRH, triptorelin reversibly represses gonadotropin secretion after prolonged administration. After chronic, continuous administration, a sustained decrease in LH, FSH and testicular and ovarian steroidogenesis is observed. The serum testosterone concentration may fall to levels typically seen in surgically castrated men [79].
| Synonyms | Pamorelin |
| US brand names | Trelstar Depot, Trelstar LA |
Patient's Perspective on LHRH Antagonists
LHRH antagonists work by directly inhibiting LHRH so that there is no more production of testosterone. In contrast, the LHRH analogs stimulate the LHRH receptor and cause initial production of testosterone for one to two weeks which is then exhausted[48]. LHRH antagonists currently being used are Abarelix.
Patient's Perspective on Abarelix (Plenaxis)
A synthetic decapeptide and antagonist of naturally occurring gonadotropin-releasing hormone (GnRH). Abarelix directly and competitively binds to and blocks the gonadotropin releasing hormone receptor in the anterior pituitary gland, thereby inhibiting the secretion and release of luteinizing hormone (LH) and follicle stimulating hormone (FSH). In males, the inhibition of LH secretion prevents the release of testosterone. As a result, this may relieve symptoms associated with prostate hypertrophy or prostate cancer, since testosterone is required to sustain prostate growth [79].
| US brand names | Plenaxis |
Patient's Perspective on Anti-androgen
Antiandrogens can block the action of androgens (hormones that promote male sex characteristics).
Patient's Perspective on Bicalutamide (Casodex®)
A synthetic, nonsteroidal antiandrogen. Bicalutamide competitively binds to cytosolic androgen receptors in target tissues, thereby inhibiting the receptor binding of androgens. This agent does not bind to most mutated forms of androgen receptors [79].
| Us brand names | Casodex |
| Foreign brand names | Cosudex |
Patient's Perspective on Flutamide (Eulexin®)
A toluidine derivative and nonsteroidal antiandrogen that is structurally related to bicalutamide and nilutamide. Flutamide and its more potent active metabolite 2-hydroxyflutamide competitively block dihydrotestosterone binding at androgen receptors, forming inactive complexes which cannot translocate into the cell nucleus. Formation of inactive receptors inhibits androgen-dependent DNA and protein synthesis, resulting in tumor cell growth arrest or transient tumor regression [79].
| Synonyms | Flucinom, Flugerel, Niftolid |
| US brand names | Eulexin |
| Foreign brand names | Apimid, Chimax, Drogenil, Euflex, Eulexine, Flucinome, Fluken, Flulem, Flutabene, Flutacan, Fluta-Gry, Flutamex, Flutamin, Flutan, Flutaplex, Fugerel, Grisetin, Oncosal, Profamid, Prostacur, Prostadirex, Prostica, Prostogenat, Tafenil, Tecnoflut, Testotard |
Patient's Perspective on Nilutamide (Nilandron®)
A synthetic, nonsteroidal agent with antiandrogenic properties. Nilutamide preferentially binds to androgen receptors and blocks androgen receptor activation by testosterone and other androgens; this agent may inhibit androgen-dependent growth of normal and neoplastic prostate cells [79].
Patient's Perspective on Cyproterone acetate (Androcur®)
The acetate salt of a synthetic steroidal antiandrogen with weak progestational and antineoplastic activities. Cyproterone binds the androgen receptor (AR), thereby preventing androgen-induced receptor activation in target tissues and inhibiting the growth of testosterone-sensitive tumor cells. This agent also exerts progestational agonist properties at the level of the pituitary that reduce luteinizing hormone (LH), resulting in reductions in testicular androgen secretion and serum testosterone levels. Treatment with cyproterone alone results in incomplete suppression of serum testosterone levels [79].
| Synonyms | cyproterone |
| Foreign brand names | Androcur, Cyprone, Cyprostat, Dianette |
Patient's Perspective on 5-alpha reductase (5-AR) inhibitor
Limits the formation of testosteron into dihydrotestosterone (DHT) which is 4x more potent form of testosteron. Prostate cancer cells depends on both testosterone and DHT to survive, so blocking the formation of DHT is a anti-cancer precaution [79].
Patient's Perspective on Finasteride (Proscar®)
A synthetic 4-azasteroid compound. Finasteride competitively binds to and inhibits steroid type II 5-alpha-reductase in the prostate gland, liver, and skin, thereby interfering with the enzymatic conversion of testosterone to 5-dihydrotestosterone (DHT) and reducing serum DHT levels. The reduction in serum DHT levels results in diminished stimulation of androgen receptors in the nuclei of prostate cells and, so, diminished prostate cell proliferation [79].
| US brand names | Proscar |
| Foreign brand names | Finastid, Pro-Cure, Prostide, Uprosan |
Patient's Perspective on Dutasteride (Avodart®)
A synthetic 4-azasteroid compound. Dutasteride competitively and specifically binds to isoenzymes 1 and 2 of 5-alpha-reductase, forming stable enzyme complexes and inhibiting the conversion of testosterone to 5α-dihydrotestosterone (DHT); the reduction in DHT activity may mitigate or prevent enlargement of the prostate gland. The type 2 5-alpha-reductase isoenzyme is primarily active in the reproductive tissues, while the type 1 isoenzyme is also active in skin and the liver [79].
| US brand names | Avodart |
Patient's Perspective on Diethylstilbestrol (DES)
DES; the acronym for diethylstilbestrol, a synthetic, nonsteroidal form of estrogen. A well-known teratogen and carcinogen, DES inhibits the hypothalamic-pituitary-gonadal axis, thereby blocking the testicular synthesis of testosterone, lowering plasma testosterone, and inducing a chemical castration[79].
| Synonyms | Diethylstilbenediol, Diethylstilbestrol Dipropionate, Diethylstilbestrolum, Diethylstilboestrol, Sinestrol, Stilboestrol Dipropionate |
| US brand names | Acnestrol, Cyren A, Deladumone, Diastyl, Domestrol, Estrobene, Estrobene, Estrosyn, Fonatol, Makarol, Milestrol, Neo-Oestronol I, Oestrogenine, Oestromenin, Oestromon, Palestrol, stilbestrol, Stilbetin, Stilboestroform, Stilboestrol, Synestrin, Synthoestrin, Vagestrol |
| Foreign brand names | Antigestil, Apstil, Boestrol, Bufon, Distilbene, Estrogenine, Estromenin, Grafestrol, Microest, Oestromensyl, Serral, Sexocretin, Sibol, Stilboefral, Stilkap |
Patient's Perspective on Ketoconazole (Nizorol®)
A synthetic derivative of phenylpiperazine with broad antifungal properties and potential antineoplastic activity. Ketoconazole inhibits sterol 14-a-dimethylase, a microsomal cytochrome P450-dependent enzyme, thereby disrupting synthesis of ergosterol, an important component of the fungal cell wall[79].
| Us brand names | Nizoral |
| Foreign brand names | Fungarest, Fungoral, Ketoderm, Ketoisdin, Orifungal M, Panfungol |
Patient's Perspective on Erectile Dysfunction Drugs
PDE-5 inhibitors drugs used to treat erectile dysfunction are Viagra®, Levitra® and Cialis®. All three of these medications work in a similar fashion by blocking the breakdown of the enzyme, cyclic GMP, which is responsible for the smooth muscle relaxation and trapping blood in the penile tissue when a man is sexually stimulated[80][81][82].
Basic common similarities include:
Patient's Perspective on Sildenafil Citrate (Viagra®)
The citrate salt of a pyrazolopyrimidinone derivative structurally related to zaprinast. Sildenafil selectively inhibits cyclic guanosine monophosphate (cGMP)-specific type 5 phosphodiesterase, resulting in vasodilation in the corpus cavernosum of the penis and penile erection[79].
| Us brand names | Viagra® |
Approximately a 4-5 hour half-life allowing for sexual activity for up to six hours or longer. Viagra® should be taken about one hour before use if on an empty stomach (up to two hours after a fatty meal or with alcohol)[75][74].
Patient's Perspective on Vardenfil HCL (Levitra®)
LEVITRA® is an oral therapy for the treatment of erectile dysfunction. This monohydrochloride salt of vardenafil is a selective inhibitor of cyclic guanosine monophosphate (cGMP)-specific phosphodiesterase type 5 (PDE5) [79].
| Us brand names | Levitra® |
Approximately a 4-5 hour half-life allowing for sexual activity up to six hours or longer. It may be taken with a low fat meal and alcohol one hour before expected relations. With a high fat meal, a man should take it two hours before sexual relations[75][74].
Patient's Perspective on Tadalafil (Cialis®)
A carboline-based compound with vasodilatory properties. Tadalfil selectively inhibits the cyclic guanosine monophosphate (cGMP)-specific type 5 phosphodiesterase- (PDE-5)-mediated degradation of cGMP, which is found in the smooth muscle of the corpus cavernosa and corpus spongiosum of the penis. Inhibition of cGMP degradation by tadalfil results in prolonged muscle relaxation, vasodilation, and blood engorgement of the corpus cavernosa, and, so, prolonged penile erection[79].
| Us brand names | Cialis® |
It has a 17.5 hour half-life with double blind studies showing activity up to 36 hours. A man can take Cialis® earlier in the day or on a Friday evening and choose to have sexual relations at the most natural or convenient time. This time freedom is attractive to both men and women because sex appears to be more natural and not dictated by the clock[75][74].
Patient's Perspective on Mitoxantrone Hydrochloride (Novantrone®)
The hydrochloride salt of an anthracenedione antibiotic with antineoplastic activity. Mitoxantrone intercalates into and crosslinks DNA, thereby disrupting DNA and RNA replication. This agent also binds to topoisomerase II, resulting in DNA strand breaks and inhibition of DNA repair. Mitoxantrone is less cardiotoxic compared to doxorubicin.
| Synonyms | dihydroxyanthracenedione, Dihydroxyanthracenedione Dihydrochloride, mitoxantrone dihydrochloride, mitoxantrone HCl,
Mitoxantroni Hydrochloridum, Mitozantrone |
| US brand names | Novantrone |
| Foreign brand names | Mitroxone, Neotalem, Onkotrone, Pralifan |
Patient's Perspective on Docetaxel (Taxotere®)
A semi-synthetic, second-generation taxane derived from a compound found in the European yew tree, Taxus baccata. Docetaxel displays potent and broad antineoplastic properties; it binds to and stabilizes tubulin, thereby inhibiting microtubule disassembly which results in cell- cycle arrest at the G2/M phase and cell death. This agent also inhibits pro-angiogenic factors such as vascular endothelial growth factor (VEGF) and displays immunomodulatory and pro-inflammatory properties by inducing various mediators of the inflammatory response. Docetaxel has been studied for use as a radiation-sensitizing agent.
| US brand names | Taxotere® |
Docetaxel is approved by the Food and Drug Administration (FDA) to be used alone or with other drugs to treat certain types of breast and non-small cell lung cancer (NSCLC). It is also approved to be used with other drugs to treat squamous cell carcinoma of the head and neck (SCCHN) and certain types of gastric and prostate cancer.
Patient's Perspective on Paclitaxel (Taxol©)
A compound extracted from the Pacific yew tree Taxus brevifolia with antineoplastic activity. Paclitaxel binds to tubulin and inhibits the disassembly of microtubules, thereby resulting in the inhibition of cell division. This agent also induces apoptosis by binding to and blocking the function of the apoptosis inhibitor protein Bcl-2 (B-cell Leukemia 2).
| US brand names | Taxol |
| Foreign brand names | Anzatax, Asotax, Bristaxol, Praxel, Taxol Konzentrat |
Patient's Perspective on Estramustine (Emcyt®)
The orally available disodium salt, monohydrate, of estramustine phosphate, a synthetic molecule that combines estradiol and nornitrogen mustard through a carbamate link. Estramustine and its major metabolite estramustine bind to microtubule-associated proteins (MAPs) and tubulin, thereby inhibiting microtubule dynamics and leading to anaphase arrest in a dose-dependent fashion. This agent also exhibits anti-androgenic effects.
| Synonym | Estramustine Phosphate |
| US brand names | Emcyt |
| Foreign brand names | Estracyt |
Patient's Perspective on Doxorubicin (Adriamycin®)
The hydrochloride salt of doxorubicin, an anthracycline antibiotic with antineoplastic activity. Doxorubicin, isolated from Streptomyces peucetius var. caesius, is the hydroxylated congener of daunorubicin. Doxorubicin intercalates between base pairs in the DNA helix, thereby preventing DNA replication and ultimately inhibiting protein synthesis. Additionally, doxorubicin inhibits topoisomerase II which results in an increased and stabilized cleavable enzyme-DNA linked complex during DNA replication and subsequently prevents the ligation of the nucleotide strand after double-strand breakage. Doxorubicin also forms oxygen free radicals resulting in cytotoxicity secondary to lipid peroxidation of cell membrane lipids; the formation of oxygen free radicals also contributes to the toxicity of the anthracycline antibiotics, namely the cardiac and cutaneous vascular effects.
| Synonym | ADM, ADR, Adria |
| US brand names | Adriamycin |
| Foreign brand names | Adriacin, Adriblastina, Rubex |
Patient's Perspective on Cyclophosphamide (Cytoxan® Neosar®)
A synthetic alkylating agent chemically related to the nitrogen mustards with antineoplastic and immunosuppressive activities. In the liver, cyclophosphamide is converted to the active metabolites aldophosphamide and phosphoramide mustard, which bind to DNA, thereby inhibiting DNA replication and initiating cell death.
| Synonym | Ciclofosfamida, Ciclofosfamide, Claphene, CP monohydrate, CPM, Cyclophospham, Cyclophosphamid monohydrate, Cyclophosphamidum, Cyclophosphan, Cyclophosphanum, Cytophosphane, Mitoxan, Syklofosfamid, Zytoxan |
| US brand names | Clafen, Cytoxan, Neosar |
| Foreign brand names | Carloxan, Cicloxal, Cycloblastin, Cycloblastine, CYCLO-cell, Cyclostin, Cyclostine, Cytophosphan, Endoxan, Endoxana, Enduxan, Fosfaseron, Genoxal, Ledoxina, Procytox, Sendoxan |
Patient's Perspective on Carboplatin (Paraplatin®)
A second-generation platinum compound with a broad spectrum of antineoplastic properties. Carboplatin contains a platinum atom complexed with two ammonia groups and a cyclobutane-dicarboxyl residue. This agent is activated intracellularly to form reactive platinum complexes that bind to nucleophilic groups such as GC-rich sites in DNA, thereby inducing intrastrand and interstrand DNA cross-links, as well as DNA-protein cross-links. These carboplatin-induced DNA and protein effects result in apoptosis and cell growth inhibition. This agent possesses tumoricidal activity similar to that of its parent compound, cisplatin, but is more stable and less toxic.
| Synonym | Carboplatin Hexal, Carboplatino |
| US brand names | Paraplat, Paraplatin |
| Foreign brand names | Blastocarb, Carboplat, Carbosin, Carbosol, Carbotec, Displata, Ercar, Nealorin, Novoplatinum, Paraplatin AQ, Paraplatine, Platinwas, Ribocarbo |
Patient's Perspective on Thalidomide (Thalomid®)
A synthetic derivative of glutamic acid (alpha-phthalimido-glutarimide) with teratogenic, immunomodulatory, anti-inflammatory and anti-angiogenic properties. Thalidomide acts primarily by inhibiting both the production of tumor necrosis factor alpha (TNF-alpha) in stimulated peripheral monocytes and the activities of interleukins and interferons. This agent also inhibits polymorphonuclear chemotaxis and monocyte phagocytosis. In addition, thalidomide inhibits pro-angiogenic factors such as vascular endothelial growth factor (VEGF) and basic fibroblast growth factor (bFGF), thereby inhibiting angiogenesis.
| Synonym | Alpha-Phthalimidoglutarimide, N-Phthaloylglutamimide, N-Phthalylglutamic Acid Imide |
| US brand names | Synovir, Thalomid |
| Foreign brand names | Contergan, Distaval, Kevadon, Neurosedyn, Pantosediv, Sedoval K-17, Softenon, Talimol |
| Click Image to play video | Topic | Presenter(s) |
|---|---|---|
| | Management of Side Effects Related to ADT Video by Dr. Lam | Richard Lam, MD |
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| Hormonal Therapy of Prostate Cancer At All Stages Video by Dr Tucker | Steven Tucker, MD |
