My personal experience in being HCV/HIV co-infected & how I cured hepatitis C.I have had HIV HIV (Human Immunodeficiency Virus), either of two closely related retroviruses that invade T-helper lymphocytes and are responsible for AIDS. There are two types of HIV: HIV-1 and HIV-2. HIV-1 is responsible for the vast majority of AIDS in the United States. for 20 years and was infected with the hepatitis C virus
abbr. hepatitis C virus HCV 1 Hepatitis C virus, see there 2. Human coronavirus. See Coronavirus. ) at least 20 years ago. So I was co-infected. The reason I say "was" is that I am no longer co-infected; that is, I don't have HCV anymore. I successfully finished my second course of treatment for HCV about 2 years ago I eradicated HCV, or "cured" it. This essay is about me and my experience in addressing my HCV. RITA RITA Cardiology A clinical trial–Randomized Intervention Treatment of Angina–comparing the outcome of PCTA vs CABG in Pts with angina. See Angina, Angioplasty, CABG, Percutaneous transluminal angioplasty. ! asked me to write this article about my experience to help others in dealing with HCV. I agree that others can learn from my experience, so I hope this helps. I strongly suspected that I had HIV 20 years ago because I had been injecting drugs for years. So I tested for HIV and was positive. But I did not realize that I might have HCV. In 1995, with the advent of protease inhibitors Protease Inhibitors Definition A protease inhibitor is a type of drug that cripples the enzyme protease. An enzyme is a substance that triggers chemical reactions in the body. , which I believed would lead us to control of HIV, I started the National AIDS Treatment Advocacy Project (NATAP NATAP National AIDS Treatment Advocacy Project NATAP North American Trade Automation Prototype ) whose sole mission was to educate people about HIV treatment and help people to improve treatment decision-making. I knew HIV could be beaten, and the answer was simply to make good treatment decisions. About 9 years ago, I figured out that I could also have HCV, not because my doctors told me but because I realized this on my own. I was tested and as suspected, I had HCV. Of course, I had a liver biopsy Liver Biopsy Definition A liver biopsy is a medical procedure performed to obtain a small piece of liver tissue for diagnostic testing. Liver biopsies are sometimes called percutaneous liver biopsies, because the tissue sample is obtained by going immediately, as the liver biopsy is the most reliable way to diagnose the stage of liver disease Liver Disease Definition Liver disease is a general term for any damage that reduces the functioning of the liver. Description The liver is a large, solid organ located in the upper right-hand side of the abdomen. . Liver enzyme tests (ALT, AST (AST Computer, Irvine, CA) A PC manufacturer founded in 1980 by Albert Wong, Safi Quershey and Tom Yuen (A, S and T). It offered a complete line of PCs that sold through its dealer channel. ) are not reliable barometers of the stage of liver disease. It is usually crucial to know your stage of liver disease in deciding when to begin HCV treatment. Unfortunately, I was told I had an advanced stage of liver disease--cirrhosis. There is no way to know how long I had HCV, but I believe I had it for at least 12 years and perhaps 15 years. Having HIV probably accelerated the progression of my HCV disease. I went into action against HCV just like I did with HIV. I very quickly started therapy with standard interferon plus ribavirin ribavirin /ri·ba·vi·rin/ (ri?bah-vi´rin) a broad-spectrum antiviral used in the treatment of severe viral pneumonia caused by respiratory syncytial virus, particularly in high-risk infants; also used in conjunction with interferon . At the time, pegylated (peg-) interferon was not available yet, so I self-injected the interferon 3 times per week. I was genotype 2, so I expected a great response to therapy. Unfortunately, I had absolutely no response. I anticipated attempting re-treatment with peginterferon plus ribavirin, but I had to wait for its availability. I couldn't wait very long because my ALTs were increasing to over 200, and I had an uncomfortable feeling around my liver. I suspected 1 needed to be treated rather quickly. Once you have cirrhosis, the risk of progression to a serious stage called "decompensated cirrhosis" is up to 4% per year. To gain access to peginterferon, I traveled over 1000 miles from my hometown in New York City New York City: see New York, city. New York City City (pop., 2000: 8,008,278), southeastern New York, at the mouth of the Hudson River. The largest city in the U.S. to enter a study. I was the second study participant and took once weekly injections of peginterferon plus 800 mg ribavirin daily. At first, I had to travel every week from New York New York, state, United States New York, Middle Atlantic state of the United States. It is bordered by Vermont, Massachusetts, Connecticut, and the Atlantic Ocean (E), New Jersey and Pennsylvania (S), Lakes Erie and Ontario and the Canadian province of to the study site for drug pick-up and bloodwork. Alter about 1 month, the visits were less often, every 23 weeks. And after several months, I could begin to increasingly space out my visits. My first viral load test Viral load test A new blood test for monitoring the speed of HIV replication in AIDS patients. The viral load test is based on PCR techniques and supplements the CD4+ cell count tests. was alter 6 weeks on therapy and it was undetectable. When 2 weeks passed, I tested my liver enzymes and they had declined appreciably, so I knew I was responding well. Seeing such a good early response is an important signal that you have a good chance to achieve a "sustained virologic response" (SVR Noun 1. SVR - Russia's intelligence service responsible for foreign operations, intelligence-gathering and analysis, and the exchange of intelligence information; collaborates with other countries to oppose proliferation of weapons of mass destruction, terrorism and ). Studies show that 99% of patients who achieve an SVR are "cured." Every piece of research data confirms that HCV is "curable cur·a·ble adj. Capable of being cured or healed. ," which means simply that HCV can be eradicated. Studies have followed several thousand patients with SVR for about 4 years and about 100 patients with SVR for as long as 10 years. No sign of virus has been found in the blood or the liver of either group. It's been 2 years since I completed my second course of HCV therapy with peginterferon plus ribavirin, and I have not felt better in more than 20 years--I feel great. Just as studies have found in patients who achieve and sustain an SVR, I have much improved energy and mental skills, I didn't realize how much HCV was affecting me until after therapy when I saw the improvement. I started to feel more energy and noticed improved mental skills shortly after finishing therapy, but since then I have continued to experience incremental improvements over the past 2 years. I feel very lucky. The best decision I made was to start therapy and to stick with it. Of course therapy is difficult to tolerate as you may be aware of; but for me it wasn't as bad as I thought it would be. It affects everyone differently. For some patients, the side effects Side effects Effects of a proposed project on other parts of the firm. are not so bad and for others they might be worse. But for me it was well worth it. The only way for me to evaluate the condition of my liver now post-treatment is to do another liver biopsy, but I am not planning to perform a biopsy. An improvement in the condition of one's liver is to be expected along with an SVR. So I expect that any liver disease--my cirrhosis--is reversing and improving. The latest studies show that cirrhosis IS reversible. Of course, the best approach is not to delay therapy until you have cirrhosis. Response rates to therapy are best when therapy is started at earlier stages of disease. You have to be very careful if you have HIV and HCV because HIV can accelerate HCV disease progression by 2 times. So, if you have a liver biopsy performed and even if you only have stage 1 or 2 (stage 3 is bridging cirrhosis and stage 4 is cirrhosis, depending on the system and test used), I suggest starting therapy. For a decision about treatment, there are a few things I recommend considering. There is no way to figure out if you will respond well to therapy unless you try it. You can always stop therapy. After 12 weeks of therapy, you can evaluate your chances for a "cure." The early viral response (EVR EVR Enhanced Vapor Recovery EVR Electronic Video Recording EVR Equine Viral Rhinopneumonitis EVR Extravehicular Robotics EVR Expanded Virtual Register EVR Exudative Vitreoretinopathy, Familial, Autosomal Dominant EVR Eläinten Vapautus Rintama ) formula tells us that if after 12 weeks there is a 2-log decline in viral load viral load n. The concentration of a virus, such as HIV, in the blood. viral load, n a measure of the number of virus particles present in the bloodstream, expressed as copies per milliliter. or an undetectable viral load, the chances of achieving an SVR or cure are good, 60% to 70%. If this status is not achieved by 12 weeks, the chance for success with therapy is very low and you can consider stopping therapy. Good adherence is crucial to achieving an SVR. Studies show that greater than 80% adherence significantly improves response rates. Because therapy is only for 12 months, there is no excuse (in my opinion) to miss any doses. One additional point regarding my therapy: although the standard duration of therapy for co-infected individuals is 12 months, I continued therapy for an extra 6 months for a total of 18 months. The reason I did this is because results from several studies suggest that if you see an EVR and if your viral load is undetectable by week 24, you are more likely to achieve an SVR if you prolong therapy an extra 6 months. So I did this. I suggest you consider this if your circumstances are similar. An important point to also consider is that interferon has certain properties that allow it to slow down liver disease progression even if the viral load is not reduced. This is important because in about 4 years, new drugs being developed now will start to become available. It's crucial to prevent progression to cirrhosis while waiting for these new drugs, so be careful about delaying initiation of therapy. Undue delay in starting therapy may put you in a bad situation. HCV disease might progress. As well, if you think by waiting you can avoid taking interferon, think again. Even if we have a new drug of 2 in several years, peginterferon will most likely have to included as part of the regimen. In conclusion, I am very fortunate to have had success with HCV therapy and eradicated HCV. This has given me a whole new life. Of course, I have used the improved energy I have by increasing the amount of work that I do. If you don't know Don't know (DK, DKed) "Don't know the trade." A Street expression used whenever one party lacks knowledge of a trade or receives conflicting instructions from the other party. what I do, NATAP provides up-to-date HIV and hepatitis treatment information and education through our website at natap.org, our HIV and HCV newsletters and HCV Handbook, and our community forums that we hold in cities throughout the US. Please access our website or call us toll free at 888.26.NATAP for information and newsletters. Jules Levin is the Founder and Director of NATAP. |
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