Tag: Cancer Treatment

Diagnosis Decisions: Is Active Surveillance the Right Prostate Cancer Treatment Choice for You?

jch9011We’re launching a new blog series to help provide some direction to the decision making process that typically follows a cancer diagnosis.

To kick off the series, we sat down with Dr. Jim Hu, one of our internationally-renowned urologists, to determine some of the factors that should go into the decision to pursue active surveillance as a prostate cancer treatment approach.  

A cancer diagnosis typically involves much more than just detecting the presence of cancer in the body. Additional information about the nature of the cancer and where it started and may have spread helps physicians recommend the best course of treatment, especially since depending on cancer type (very low, low, intermediate or high risk), there can be a wide ranging degree of aggressiveness.

For most types of cancers, there are different standards used to “grade” or assess this aggressiveness on a common scale. Usually this information is then used in conjunction with information about whether the cancer has already spread or metastasized to other parts of the body. It can also be used alongside other genetic and molecular information about the cancer that tells us whether this specific cancer is likely to respond to a certain treatment and the rate at which the cancer is likely to spread.

For a long time, prostate cancer has been known as an “indolent” or slow-growing cancer relative to other cancers such as pancreatic or lung cancers. The aggressiveness or rate at which it is likely to grow is measured by studying the appearance of the cancer cells under a microscope to determine the grade. For prostate cancers, we refer to this as the Gleason score. The lowest prostate cancer grade is currently Gleason 3+3=6. Grade 6 prostate cancer is thought to be non-aggressive and unlikely to spread to other places in the body.

However, there are cases when more aggressive cancer may have been hidden and then subsequently discovered. The challenge is that in 75% of cases, prostate cancer is multi-focal, meaning that it grows within several areas of the prostate. This makes it difficult to accurately stage the tumor entirely, as only one section of the cancer is being analyzed to determine its aggressiveness. As a result, the decision to pursue active surveillance or careful monitoring and watching in patients with low-grade tumors on the Gleason scale depends on several factors. These factors include a man’s overall health, life expectancy, the age of diagnosis, and personality type.

The rationale for this approach is that low-risk prostate cancer grows very slowly and some question whether it ever spreads. Therefore the majority of these cancers may not be life threatening within a 10 year time frame, so men can avoid prostate cancer therapies that may affect quality of life. For this group, active surveillance is an alternative to the over-treatment of prostate cancer and potential side effects that can come along with it For example, in men who have numerous medical conditions and a shorter life expectancy, active surveillance is a reasonable treatment option, even with Gleason 3+4=7 prostate cancer, or intermediate risk disease.

With active surveillance, it is important to be monitored regularly by a urologist who will test your PSA levels and perform digital rectal examinations of the prostate. Imaging with Magnetic Resonance Imaging (MRI) and targeted biopsy of suspicious areas should also be part of the routine to accurately assess prostate cancer severity.

Targeted biopsies use ultrasound fused to the MRI to guide the procedure, greatly increasing the accuracy and likelihood that the tissue sample is of the most suspicious section of the prostate. A guided biopsy takes approximately 10 minutes and carries a small risk of infection or bleeding (like a standard biopsy). Many academic medical centers, including Weill Cornell Medicine/NewYork-Presbyterian Hospital offer targeted biopsies, but many community practices do not. Additionally, there is a learning curve to the procedure, so the experience of the urologist is critical.

There are also biomarkers that have recently been developed to evaluate the need for a prostate biopsy. These include the 4K test and Prostate Health Index (PHI), which are blood tests that assess the likelihood that prostate cancer may be contributing to a rise in PSA level.

Additionally, for men diagnosed with low risk prostate cancer, there are new tests that assess the genetics of the tissue to determine whether more aggressive disease may have been missed on the biopsy, and present in other parts of the prostate. These assays are called Oncotype Dx, Decipher and Polaris.

We offer all of these tests at Weill Cornell and NewYork-Presbyterian, and together they paint a much more complete picture of the prostate cancer and whether it is progressing. This comprehensive, big picture is what we use to make recommendations for your overall course of prostate cancer treatment, including whether it would be a good idea to pursue active surveillance.

Meet the Newest Member of Our Team: Dr. Bishoy Faltas

Bishoy_Faltas_HeadshotWe’re pleased to announce that the Genitourinary (GU) Oncology Program is expanding! Dr. Bishoy Faltas joined us on July 1st as an Instructor in Medicine and as an Assistant Attending Physician. He will see patients with bladder, prostate, testicular, and kidney cancers.

Dr. Faltas may already be a familiar face and name because he completed his Hematology and Medical Oncology Fellowship here at Weill Cornell Medicine and NewYork-Presbyterian Hospital in 2015. Additionally, he recently finished a one-year research fellowship in the laboratory of Dr. Mark A. Rubin and the Institute for Precision Medicine.

As part of the Genitourinary Oncology Program, Dr. Faltas will focus his research on urothelial carcinoma, the most common type of bladder cancer, and specifically on genetic mutations and drug-resistance. He has presented groundbreaking work on genomic alterations before and after chemotherapy and the potential clinical implications. He will also be building upon his prior research examining how patients with bladder cancer respond to immunotherapies.

He has already received numerous research awards for his work, is a member of the Bladder Cancer Advocacy Network, and we are very excited to officially welcome Dr. Faltas to the GU team!

8 Tips to Combat Chemo-Related Sun Sensitivity

Sunblock Cream Reflect UVSummertime often means vacations and more time outdoors. This also comes with increased exposure to the sun – which isn’t such a “sunny” thing if you’re feeling sensitive to it.

A side effect of chemotherapy that many cancer patients express they feel the most is sun sensitivity. This “photosensitivity” occurs because agents in chemotherapy are radiosensitizers which help to impact treatment, but also increase the body’s sensitivity to UV rays (the radiation from the sun that reaches the earth).

A little bit of sunshine can be beneficial, since the sun provides Vitamin D for strong bones, but too much exposure during chemotherapy can be dangerous and increase your risk of sunburn. Here are 8 tips to protect yourself from the sun’s harmful rays during and after chemotherapy:

  • Chemo and the sun don’t get along. Photosensitivity can start immediately after your first treatment and last for a few months post-treatment. Several kinds of medications (for cancer and non-cancer alike) can also increase sun sensitivity; so ask your physician and pharmacist if you’re taking any medications that fall in this category.
  • Watch the clock. Avoid mid-day sun exposure when the sun’s rays are most intense. In most places, the sun is the strongest between 10am-4pm.
  • Pay to attention SPF. SPF stands for Sun Protection Factor and represents the theoretical amount of time you can stay in the sun without getting burned. It is important to use sunscreens with protection above 30 SPF and to make sure the SPF includes protection against both UVA and UVB rays (labeled as “broad spectrum”). These two different types of rays can both cause sunburn.
  • Lather up! Reapply sunscreen every two hours or even more frequently if you’re sweating or swimming.
  • Bald is beautiful, but protect your head. Wear a wide-brimmed hat in addition to sunscreen if you have lost your hair, and in general to help protect your ears, neck and face further.
  • Stylize with shades. Wear sunglasses with UV protection to protect your eyes any time the sun is out. If your wear prescription eyeglasses, consider getting transitional lenses so that you don’t have to worry about carrying an extra pair.
  • Cover-ups are key. Cover your exposed skin as much as possible. Wear long-sleeve shirts and pants so that your body is not directly hit by the sun. Many companies now make sun protective clothing which are light, breathable and offer excellent sun protection without the need for constant re-applying of sunscreen to the covered areas.
  • Don’t forget the small spots. Ears, eyelids, feet, and lips can be easily forgotten but need extra protection. Use lip balm with SPF to protect your lips, inquire with your oncologist or dermatologist regarding sunscreens for sensitive areas, and don’t forget to put sunscreen on your ears and top of your feet (two areas that are directly hit by the sun).

In the case of a sunburn, use cold compresses and aloe vera to ease discomfort. Contact your physician if redness persists or if your sunburn is severe.