My TC Experience

Drug type: Bleomycin is an anti-cancer ("antineoplastic" or "cytotoxic") chemotherapy drug. This medication is classified as an "antitumor antibiotic." (For more detail, see "How this drug works" section below).

What this drug is used for:

Used in the treatment of squamous cell cancers, melanoma, sarcoma, testicular cancer, Hodgkin's and non-Hodgkin's lymphoma.
Also used to treat pleural effusion (build up of fluid in the space between the lining of the lung and the chest wall).

Side effects:

The following side effects are common:

Fever and chills (see flu-like symptoms).
Skin reactions: redness, darkening of the skin, stretch marks on the skin, skin peeling, thickening of the skin, ulceration.
Nail thickening, nail banding (see skin reactions).
Hair loss.
Nausea and vomiting.
Poor appetite and weight loss.
Mouth sores.
Lung problems: pneumonitis, rarely pulmonary fibrosis. The incidence of lung problems increases with age and pre-existing lung conditions. There is a maximum lifetime dose of bleomycin. Your health care professional will monitor the amount of bleomycin you receive as well as your lung function during treatment.
Occasionally this can cause "radiation recall" effect. (see skin reactions)

Less Common but significant side effects may include:

Vascular effects leading to heart attack or stroke - potentially life-threatening conditions, or Raynaud's phenomenon (a disorder of the small blood vessels that feed the skin, most commonly affecting the hands and feet).
Severe allergic reaction (anaphylaxis) immediate or delayed for several hours. You will be monitored closely for any signs of allergic reaction (rash, flushing, lowered blood pressure, difficulty breathing).

How this drug works:

Cancerous tumors are characterized by cell division, which is no longer controlled as it is in normal tissue. "Normal" cells stop dividing when they come into contact with like cells, a mechanism known as contact inhibition. Cancerous cells lose this ability. Cancer cells no longer have the normal checks and balances in place that control and limit cell division. The process of cell division, whether normal or cancerous cells, is through the cell cycle. The cell cycle goes from the resting phase, through active growing phases, and then to mitosis (division).

The ability of chemotherapy to kill cancer cells depends on its ability to halt cell division. Usually, the drugs work by damaging the RNA or DNA that tells the cell how to copy itself in division. If the cells are unable to divide, they die. The faster the cells are dividing, the more likely it is that chemotherapy will kill the cells, causing the tumor to shrink. They also induce cell suicide (self-death or apoptosis).

Chemotherapy drugs that affect cells only when they are dividing are called cell-cycle specific. Chemotherapy drugs that affect cells when they are at rest are called cell-cycle non-specific. The scheduling of chemotherapy is set based on the type of cells, rate at which they divide, and the time at which a given drug is likely to be effective. This is why chemotherapy is typically given in cycles.

Chemotherapy is most effective at killing cells that are rapidly dividing. Unfortunately, chemotherapy does not know the difference between the cancerous cells and the normal cells. The "normal" cells will grow back and be healthy but in the meantime, side effects occur. The "normal" cells most commonly affected by chemotherapy are the blood cells, the cells in the mouth, stomach and bowel, and the hair follicles; resulting in low blood counts, mouth sores, nausea, diarrhea, and/or hair loss. Different drugs may affect different parts of the body.

Bleomycin is classified as an antitumor antibiotic. Antitumor antibiotics are made from natural products produced by species of the soil fungus Streptomyces. These drugs act during multiple phases of the cell cycle and are considered cell-cycle specific. There are several types of antitumor antibiotics:

Anthracyclines: Doxorubicin, Daunorubicin, Mitoxantrone, and Idarubicin.
Chromomycins: Dactinomycin and Plicamycin.
Miscellaneous: Mitomycin and Bleomycin.

Etoposide

Drug type: Etoposide is an anti-cancer ("antineoplastic" or "cytotoxic") chemotherapy drug. This medication is classified as a "plant alkaloid" and "topoisomerase II inhibitor." (For more detail, see "How this drug works" section below).

What this drug is used for:

Testicular, bladder, prostate, lung, stomach, and uterine, cancers. Hodgkin's and non-Hodgkin's lymphoma, mycosis fungoides, Kaposi's sarcoma, Wilm's tumor, rhabdomyosarcoma, Ewing's sarcoma, neuroblastoma, brain tumors.
It also may be given as high-dose therapy in bone marrow transplant setting.

Side effects:

The following side effects are common:

Low white blood cell count. (This can increase your risk for infection).
Low platelet count (This can increase your risk of bleeding).

Nadir: Meaning low point, nadir is the point in time between chemotherapy cycles in which you experience low blood counts.

Onset: 5-7 days
Nadir: 7-14 days
Recovery: 21-28 days

Hair loss
Menopause (chemotherapy induced)
Loss of fertility. Meaning, your ability to conceive a child may be affected by etoposide. Discuss this issue with your health care provider.
Nausea and vomiting (especially at high-doses)
Low blood pressure (if the drug is infused too fast)

Less common but significant side effects:

Mouth sores (especially at high doses)
Diarrhea (especially at high doses)
Poor appetite
Radiation recall (see skin reactions)

Other side effects:

Metallic taste during infusion of drug
Inflammation at injection site
Peripheral neuropathy (numbness in your fingers and toes) may occur with repeated doses. This is a rare side effect but can be irreversible. Report numbness or tingling of feet or hands to your health care provider.

Delayed effects:

There is a slight risk of developing a blood cancer such as leukemia years after taking etoposide. Talk to your doctor about this risk.

Etoposide belongs to a class of chemotherapy drugs called plant alkaloids. Plant alkaloids are made from plants. The vinca alkaloids are made from the periwinkle plant (catharanthus rosea). The taxanes are made from the bark of the Pacific Yew tree (taxus). The vinca alkaloids and taxanes are also known as antimicrotubule agents. The podophyllotoxins are derived from the May apple plant. Camptothecan analogs are derived from the Asian "Happy Tree" (Camptotheca acuminata). Podophyllotoxins and camptothecan analogs are also known as topoisomerase inhibitors. The plant alkaloids are cell-cycle specific. This means they attack the cells during various phases of division.

Vinca alkaloids: Vincristine, Vinblastine and Vinorelbine
Taxanes: Paclitaxel and Docetaxel
Podophyllotoxins: Etoposide and Tenisopide
Camptothecan analogs: Irinotecan and Topotecan

Topoisomerase inhibitors (such as etoposide) are drugs that interfere with the action of topoisomerase enzymes (topoisomerase I and II). Topoisomerase enzymes control the manipulation of the structure of DNA necessary for replication.

Topoisomerase I inhibitors: Ironotecan, topotecan
Topoisomerase II inhibitors: Amsacrine, etoposide, etoposide phosphate, teniposide

Cisplatin

Trade names: Platinol^®, Platinol^®-AQ
Other names: CDDP

Drug type: Cisplatin is an anti-cancer ("antineoplastic" or "cytotoxic") chemotherapy drug. This medication is classified as an "alkylating agent." (For more detail, see "How this drug works" section below).

What this drug is used for:

Used to treat testicular, ovarian, bladder, head and neck, esophageal, small and non-small cell lung, breast, cervical, stomach and prostate cancers. Also to treat Hodgkin's and non-Hodgkin's lymphomas, neuroblastoma, sarcomas, multiple myeloma, melanoma, and mesothelioma.

Side effects:

The following side effects are common:

Nausea and vomiting. Nausea may last up to 1 week after therapy. Anti-nausea medication is given before the infusion, and a prescription is also given for use after.
Kidney toxicity, effects on kidney function are dose related, observed 10-20 days after therapy, and are generally reversible.
Blood test abnormalities: (low magnesium, low calcium, low potassium).
Low white blood cells (this may put you at increased risk for infection).
Low red blood cells (anemia).

Nadir: Meaning low point, nadir is the point in time between chemotherapy cycles in which you experience low blood counts.

Onset: 10 days
Nadir: 14-23 days
Recovery: 21-39 days

Less common but significant side effects:

Peripheral neuropathy: Although less common, a serious side effect of decreased sensation and paresthesia (numbness and tingling of the extremities) may be noted. Sensory loss, numbness and tingling, and difficulty in walking may last for at least as long as therapy is continued. These side effects may become progressively more severe with continued treatment, and your doctor may decide to decrease your dose. Neurologic effects may be irreversible.
High frequency hearing loss. Ringing in the ears.
Loss of appetite
Taste changes, metallic taste
Increases in blood tests measuring liver function. These return to normal once treatment is discontinued. (see liver problems).
Hair loss
Your fertility, meaning your ability to conceive or father a child, may be affected by cisplatin. Please discuss this issue with your health care provider.

Cisplatin is classified as an alkylating agent. Alkylating agents are most active in the resting phase of the cell. These drugs are cell cycle non-specific. There are several types of alkylating agents.

Mustard gas derivatives: Mechlorethamine, Cyclophosphamide, Chlorambucil, Melphalan, and Ifosfamide.
Ethylenimines: Thiotepa and Hexamethylmelamine.
Alkylsulfonates: Busulfan.
Hydrazines and Triazines: Procarbazine, Dacarbazine and Temozolomide.
Nitrosureas: Carmustine, Lomustine and Streptozocin. Nitrosureas are unique because, unlike most chemotherapy, they can cross the blood-brain barrier. They can be useful in treating brain tumors.
Metal salts: Carboplatin, Cisplatin, and Oxaliplatin.

Kojak for Halloween

6 Comments / Subscribe To Comments

Published: Oct.17.2005 @ 9:03 am

"Who loves you baby"

Tumor(s) growing...

BEP Chemotherapy to begin on October 31, 2005

3 cycles / 9 weeks

10/14/05

2 Comments / Subscribe To Comments

Published: Oct.13.2005 @ 4:00 pm

No Blogging on Friday

To all,

I will be at the University of Miami, Sylvester Cancer Center (no relation) all day tomorrow for tests & to visit with 'Dr. B'. I hope to find out what the next step in this adventure will be, but you never know...wish me luck!

-D

TC Causes & Prevention

2 Comments / Subscribe To Comments

Published: Oct.11.2005 @ 9:10 am

How many men get TC?

What causes TC?

Can TC be Prevented?

How Many Men Get Testicular Cancer?

There will be about 8,010 new cases of testicular cancer in the United States in 2005. This cancer is not common. A man’s lifetime risk of getting testicular cancer is about 1 in 300.

About 390 men will die of the disease in 2005. Testicular cancer is one of the most curable forms of cancer. The lifetime risk of dying from this cancer is 1 in 5,000.

What Causes Testicular Cancer?

While we do not know the exact cause of most cases of testicular cancer, we do know some of the risk factors linked to testicular cancer.

A risk factor is something that increases a person's chance of getting a disease. Different cancers have different risk factors. Some risk factors, such as smoking, can be controlled. Others, like a person's age or race, can't be changed. But having a risk factor, or even several, does not mean that a person will get the disease.

Scientists have found a few risk factors that make a man more likely to get testicular cancer. Even if a man has one or more risk factors for this disease, there’s no way to know for sure how much that contributed to causing the cancer. Also, most men with testicular cancer do not have any of the known risk factors. Research in this area is going on.

The risk of getting this cancer, even with risk factors, is very low.

Risk Factors for Testicular Cancer

Cryptorchidism (kript-OR-kid-izm): The main risk factor for testicular cancer is a problem called cryptorchidism, or undescended testicle(s). Before birth, the testicles normally develop in the belly and then move down (descend) into the scrotum. But in about 3% of boys, the testicles do not move into the scrotum. Sometimes the testicle stays inside the belly. In other cases, the testicle starts to come down, but gets stuck in the groin.

About 14% of testicular cancer cases occur in men who have had cryptorchidism. The risk is higher for men with a testicle in the belly as opposed to one that has moved down at least part way. Among men with a history of this problem, most cancers start in the testicle that has not moved down. But up to 25% of cases occur in the normal testicle. Because of this, some doctors think that cryptorchidism is not the direct cause of testicular cancer. They believe that some other problem causes both the cancer risk and the cryptorchidism.

Most testicles will descend on their own in the child's first year. Sometimes surgery is needed to bring the testicle down into the scrotum. Some experts believe that having this surgery before puberty may reduce the risk of developing some germ cell tumors.

Family history: A family history of testicular cancer increases the risk. If a man has the disease, there is an increased risk that his brothers or sons may also develop it. However, very few cases of testicular cancer are actually found to occur in families.

Certain types of moles: Recent studies have shown that an unusual condition that causes many spots or moles on the skin is linked to an increased risk of testicular cancer. The moles are found on the back, chest, belly and face.

HIV infection: There is some evidence that men infected with HIV (human immunodeficiency virus) have an increased risk of testicular cancer. This may be especially true for men who have AIDS. No other infections have been shown to increase testicular cancer risk.

CIS (carcinoma in situ): CIS is a condition in which germ cells grow into a tumor but do not yet invade normal tissues. CIS in the testicles may become cancer over a number of years. CIS does not cause a lump or any symptoms. It is sometimes found when a man is tested for infertility. It may also be found when a man has a testicle removed because of cryptorchidism.

Cancer of the other testicle: Men who have been cured of cancer in one testicle have an increased risk (about 3% to 4%) of getting cancer in the other testicle.

Race and ethnicity: White American men are about 5 to 10 times more likely to get testicular cancer than are African-American men. Whites have more than twice the risk of Asian-American men. The risk for Hispanics falls between that of Asians and non-Hispanic whites. The reason for this difference is not known. The testicular cancer rate has increased in both whites and blacks, although the rate of increase is greater in white men.

Body size: A recent study from Sweden found that body size was a risk factor. The highest risk was seen in tall, slim men. But testicular cancer is not a common disease. So the health benefits of being slim outweigh any concern about this cancer.

Can Testicular Cancer Be Prevented?

Cryptorchidism, white race, and a family history of the disease are the main known risk factors of this cancer. None of these factors can be prevented because they are present at birth. Also, many men with testicular cancer have no known risk factors. For these reasons, there is no way to prevent most cases of this disease.

But it is wise to correct cryptorchidism in boys. And knowing he has a risk factor may cause a young man to be more watchful and to check his testicles, making it more likely a cancer will be found early.

What is Testicular Cancer?

0 Comments / Subscribe To Comments

Published: Oct.11.2005 @ 9:05 am

What is Testicular Cancer?

What Is Testicular Cancer?

Testicular cancer is cancer in one or both testicles. It usually occurs in young men. This type of cancer can be treated and very often cured.

The testicles (or testes) are part of the male reproductive system. Each one is normally somewhat smaller than a golf ball. They are held in a sac of skin called the scrotum. The scrotum hangs beneath the base of the penis.

The testicles make male hormones, most of which is testosterone (tes-TOSS-ter-own). They also produce sperm. Sperm cells are carried from the testicles through small tubes (vas deferens) in the body to the seminal vesicles. Fluid from the vesicles and from the prostate gland is added. During ejaculation, the fluid (now called semen) travels through a tube (urethra) in the center of the penis and out of the body.

The testicles have several kinds of cells. The different cells may develop into one or more types of cancer. These types of cancer are treated differently. They also differ in the chance of survival for the patient (prognosis). The 3 main types of testicular cancer are:

Germ cell tumors: This is the most common type of testicular cancer. Germ cell tumors grow in the cells that make sperm.

Stromal tumors: These tumors grow in other parts of the testicles, such as the cells that make hormones.

Secondary testicular tumors: These tumors develop from cancer that has spread to the testicles from other parts of the body.

Each of the 3 types is explained in more detail below.

Germ Cell Tumors

More than 9 out of 10 of cancers of the testicles start in the germ cells. As used here, "germ" means seed. These are the cells that make sperm.

The 2 main types of germ cell tumors are seminomas and nonseminomas.

Seminomas start from the sperm-producing germ cells of the testicle. Within this group there are also subtypes. Seminomas usually happen in men when they are between their late 30s and early 50s.

Nonseminomas tend to develop earlier in life than seminomas. They are often found in men between their late teens and early 40s. There are 4 main subtypes. Most tumors are mixed, having at least 2 different types. But all nonseminoma germ cell cancers are treated the same way, so the exact type is not that important.

Stromal Tumors

Tumors can also grow in the cells that make hormones and in the supportive tissues, or stroma, of the testicles. Stromal cell tumors are often benign (not cancer). They usually do not spread beyond the testicle and can be cured by surgical removal. But a few stromal cell tumors spread to other parts of the body (metastasize). Metastatic stromal cell tumors have a poor outlook because they do not respond well to chemotherapy or radiation therapy. The 2 main types of stromal tumors are Leydig cell tumors and Sertoli cell tumors.

Secondary Testicular Tumors

Secondary testicular tumors start in another organ and then spread to the testicle. Lymphoma is the most common cancer of this type. Among men over age 50, testicular lymphoma is more common than tumors that start in the testicle. Their outlook depends on the type and stage of lymphoma. The usual treatment is to remove the testicle. Surgery is followed by radiation and/or chemotherapy.

In children with acute leukemia, the leukemia cells can sometimes form a tumor in the testicle.

Cancers of the prostate, lung, skin, kidney, and other organs can also spread to the testicles. The outlook for these cancers is usually poor. That’s because these cancers have generally spread widely to other organs as well. Treatment depends on the exact type of cancer.

Revised: 7/20/2005

What the heck is Cancer?

0 Comments / Subscribe To Comments

Published: Oct.11.2005 @ 9:03 am

What is Cancer?

Cancer occurs when cells in a part of the body begin to grow out of control. Normal cells divide and grow in an orderly fashion, but cancer cells do not. They continue to grow and crowd out normal cells. Although there are many kinds of cancer, they all have in common this out-of-control growth of cells.

Different kinds of cancer can behave very differently. For example, lung cancer and breast cancer are very different diseases. They grow at different rates and respond to different treatments. That’s why people with cancer need treatment that is aimed at their kind of cancer.

Sometimes cancer cells break away from a tumor and spread to other parts of the body through the blood or lymph system. They can settle in new places and form new tumors. When this happens, it is called metastasis (meh-tas-tuh-sis). Cancer that has spread in this way is called metastatic cancer.

Even when cancer has spread to a new place in the body, it is still named after the part of the body where it started. For example, if prostate cancer spreads to the bones, it is still called prostate cancer. If breast cancer spreads to the lungs, it is still breast cancer. When cancer comes back in a person who appeared to be free of the disease after treatment, it is called a recurrence.

Feelings, wo wo wo feeeelings

4 Comments / Subscribe To Comments

Published: Oct.07.2005 @ 8:36 am

Just thought I'd share...I just want to express myself, like Madonna said to...

This waiting is really annoying me. I'll have to wait and stay tuned until next friggin' friday to possibly find out if the node(s)' growing, just what the hell is going on inside of me. It's a sinister plot to make me more anxiety-riddled than I already am normally, I tell you. For god's sake (why do people always say for god sakes...makes no sense), my stomach is producing more acid than vendors at a Grateful Dead concert, I've got headaches every day and on top of that, my face is breaking out!

Ok, I'm done for now. I'll stop. I swear. It's just hard you know. Hey why are you still reading? I said I was done.

Dr. Benedetto (Oncology)

2 Comments / Subscribe To Comments

Published: Oct.04.2005 @ 3:28 pm

Where Cancer becomes reality

Jackson Memorial Hospital - University of Miami Sylvester Comprehensive Cancer Center

Pasquale W. Benedetto, MD - Medical Oncology (Specialty: Testicular Cancer)

With all of the gray areas, varieties of staging, etc...I knew I needed a specialist, one who may have seen a case or two of this rare form of cancer. He is just that, and a whole lot more so far. He's very knowledgeable, personable and spends as much time as needed during each appointment (the only downside of that is it's about a 2 hour wait getting in to see him.) One major distinction between Dr. B and others who treat this disease is that Dr. B does not believe in doing the RPLND surgery, just right into Chemotherapy when needed. He'd rather see you skip this major surgery, especially since almost 50% of the patients end up having to do adjuvant chemo post-surgery.

I'm going to skip the details on all of the tests, CT scans, blood test follow ups, PET scan, etc...It's all about where I'm at know...

At this point, the markers have gone down to 'normal' level, unfortunately though they're not too reliable in detecting disease when results are not positive. When they are positive (higher than normal range), then it is accurate...you know you're ready for treatment. The other issue is that I have one node in the abdomen which is highly suspicious of being cancerous, but it's not real big at this point. I believe Dr. B is erring on the conservative side, since there is a small chance that the node could go away, although that would be unlikely. It also happens to be in the exact spot the cancer typically travels & spreads to.

The other issue is that there are some patch spots on my lungs (the lungs are usually the next place the cancer would travel to, and it is said that the Embryonal type has a knack for skipping right into the lungs.) The doctor is not quite sure what it is yet, since cancer there usually just looks like nodes, not patch white stuff. In a nutshell (sorry), I am in limbo, which really sucks...I just want to either hear that somehow it's all gone, or start the friggin treatment, pick up some lolipops and get it over with!

The doc is right though, he wants to just keep checking it and if the node doesn't go away/gets bigger, markers go up, lung picture becomes 'clearer', or any of these things happen...then we'll start treatment.

Next appointment with Dr. B. is next Friday, October 14th...We'll do another CT Scan, blood tests and then see what's what...Wish me luck.

Follow up with Dr. Tookmyball

2 Comments / Subscribe To Comments

Published: Oct.04.2005 @ 1:40 pm

Tests all in...Oncology-bound

Blood markers were elevated (AFP=27) pre-orchiectomy, went down to 10 post-orchiectomy (which is what you want since the serum half-life of AFP is approximately 4-5 d after orchidectomy). One more week and the AFP was 3.5 - doing what it should so far.

The bad news was that it looks like there is a node in abdomen which is typically where spread begins from the Lymph Nodes. It is not large, approx. 1.5 cm. There is possible spread to the lungs, but the tests are not conclusive on those thusfar.

The next step as indicated by Dr. Marks (and logic), was to find an Oncologist to go on to the next step in the process.

Enter Pasquale Benedetto, MD. (Not as cool a name as Trapper, but pretty good in it's own right)...

Pathology of the little bugger

0 Comments / Subscribe To Comments

Published: Oct.04.2005 @ 1:26 pm

NSGCT

The pathology, blood tests (markers) & CT Scan results:

PATHOLOGY:

NSGTC (Non-seminomatous Germ Cell Tumor)- comprised of 99% Embryonal Carcinoma, with a splash of Choriocarcinoma (see Lance Armstrong).

Embryonal Carcinoma:

2.3% of testicular germ cell tumors
40% of all germ cell tumors have some embryonal component
87% of non-seminomatous germ cell tumors
Average about 2.5 cm
Embryonal carcinoma is characterized by rapid and bulky growth and by spread via lymphatic and hematogenous routes to distant viscera (eg, lungs, liver). More than 60% of patients have metastases at the time of presentation. Pain is a common feature in these patients.

I had to get the kind that spreads like butter on a corn muffin! The doctors guage the chance of spreading by the percentage of Embryonal Cell within the original tumor. Since mine is pretty much 'pure embryonal cell', you can see where we're at there! Oh well, hopefully I got it early enough that metastases would be limited.

Stay tuned...

Current Page 1
1 2 | > >>

| Report Member |

Free Blog BlogText.org

BEP

No Blogging on Friday

How many men get TC?

What causes TC?

Can TC be Prevented?

How Many Men Get Testicular Cancer?

What Causes Testicular Cancer?

Can Testicular Cancer Be Prevented?

What is Testicular Cancer?

What is Cancer?