That is wonderful news. Congratulations on being UND.
Congratulation on being und.
Good luck with the rest of tx.
The first doctor I talked to about viral loads, groaned.
She said, " I almost want to stop taking them. They're only relevant when in treatment to measure how it's working. Viral loads vary, up and down, and have nothing to do with liver damage"
Well, I'm "negative" for the tests after 8 weeks. The nurse said the positive/negative test is more sensitive than the viral load test, so this is good news.
Platelets are 62
Hemo 102
WBC 1.7
ALT 58 (was 92 before start of treatment)
AST 65 (was 73 before start of treatment)
My weight came down 12 pounds in those first 8 weeks.
Now coming to the end of my 10th week, my 11th injection is tomorrow.
Thanks, Pooh. I'll know the results of the Mar 9 tests sometime late next week.
Wishing you the best results, Peter.
Had my 8 week appointment and blood tests today.
I asked about IL-28B and CC, CT, and TT. Except for one lab in an Eastern province, Nova Scotia they do not test for it in Canada. The test has never been done here in British Columbia, although BC has (rarely) sent blood to Nova Scotia to be tested.
They say I am very likely not a TT because it occurs most often in black people and is found only rarely in whites. Most Asians are CC and white people are usually either CC or CT.
My white blood cell count is dropping quite low so it's something that has to be watched. My platelets and red blood cells have also dropped but are still well above the level of concern.
The nurse took some blood to test for the 8 week viral load, and they are sending it to the provincial lab. However, she said they may refuse to analyze it because the guidelines call for only one test at 4 weeks because of the cost. British Columbia has the highest rate of Hep C in Canada because of Vancouver's heroin addicts and because so many baby boomers moved here who had experimented with drugs in their teens, so the cost to the government is higher than elsewhere in Canada.
Well, I have my 8 week appointment tomorrow.
I'm not feeling bad these days, since I now have the nasty rash under control with the ointment and strong antihistimines I got with prescription.
Since I'm 9 years older than I was when I had the rebetron treatment, I'm surprised that I have a bit more energy with pegatron this time, at least so far. But then again, in 2003 the most severe fatigue didn't hit until around 10-12 weeks, so the worst may be yet to come.
I requested about ten days ago that my viral load count or at least a positive/negative test should be done tomorrow, but they said they are not sure it's possible. I'd feel a lot more confident in my chances of SVR if I could be sure I'm now undetectable.
Since you seem to be determined to finish your 24vweeks, it probably would be a waste of US$300+ to have the test done now. For myself it would be imoportant if my chances were 87%, 67%, or 29% - especially if I started having problems midway through tx, But I'm a whiny wimp with a lot of (subjetive) extreme sx, even though my blood counts stayed close to norm. The doctor may, in fact, have you pegged as a CT, which would be in line with his "over 50%" statement.
If, in fact, he has not done the test and just pulling fugures out of ,,,,,, well you know, this could also be valuable info in so far as you're being able to trust your docs tx decisions.
If you get or have gotten the test, hope you're CC. Good luck.
I'll ask the doctor about CC, CT, and TT on March 9 when I go for my 8 week blood tests and appointment. I know they took a lot of tests before approving me for my current treatment, and I've had numerous tests in past years, so perhaps he already knows.
Honestly, maybe I'm being overly optimistic, but I feel I became undetectable at week 5 or 6 anyway, so I don't think the 44 result at week 4 will make a huge difference.
I have a gut feeling that if I meticulously follow the treatment and complete week 24, I have a good chance of SVR. My gut feelings have never been wrong before.
If your doctor tells you 50% without knowing this information he's just guessing.
It would make a huge diference to me which IL28B genotype I was if I were geno3 and did not RVR.
"Differences between IL-28B genotypes were greatest among patients who failed to attain RVR (VD24 SVR rates: CC, 87%; CT, 67%; and TT, 29%"
I would seriously consider having the test done.
http://www.gastrojournal.org/article/S0016-5085(10)00841-3/abstract
Background & Aims
Polymorphisms in the region of the interleukin (IL)-28B gene on chromosome 19 have been associated with peginterferon-alfa–induced clearance of genotype 1 hepatitis C virus (HCV); there are no data for patients with genotype 2 or 3 HCV. We evaluated the effects of IL-28B polymorphisms on response to treatment with peginterferon and ribavirin in a well-characterized cohort of genotype 2/3 patients.
Methods
DNA was analyzed from 268 patients (Caucasian: genotype 2, 213; genotype 3, 55). Patients were randomly assigned to groups that received standard duration (24 wk; n = 68) or variable durations of therapy. Patients who received variable durations (VD) and had a rapid virologic response (RVR) were treated for 12 weeks (VD12; n = 122); those without an RVR were treated for 24 weeks (VD24; n = 78). IL-28B genotypes (rs12979860) were analyzed for association with treatment response.
Results
The frequencies of the IL-28B genotypes were as follows: CC, 37%; CT, 48%; and TT, 15%; 82% of patients with the CC genotype achieved a sustained virologic response (SVR), compared with 75% with the CT and 58% with the TT genotypes (P = .0046). Differences between IL-28B genotypes were greatest among patients who failed to attain RVR (VD24 SVR rates: CC, 87%; CT, 67%; and TT, 29%; P = .0002). Among patients with RVRs (61%), the IL-28B genotype was not associated with SVR (>70% for all IL-28B genotypes). In a multivariable logistic regression model, IL-28B genotype predicted SVR (odds ratio, 1.76; 95% confidence interval, 1.16–2.7).
Conclusions
An IL-28B polymorphism was associated with an SVR in patients infected with genotype 2/3 HCV who did not achieve a RVR. Analysis of IL-28B genotype might be used to guide treatment for these patients.
I made a mistake - I misread it as > 2.
I have stage 4 cirrhosis - still, I think if I've not achieved SVR after 24 weeks, there's no sense in prolonging my torment and possibly be more disappointed later on. But I will discuss it with the doctor on March 9.
I'm confused. Up above you said you have stage 4 cirrhosis, but you also said that your fibrosis score is <2. I don't understand, that seems contradictory. If you truly have stage 4 cirrhosis, you may want to ask your doctor about the possibility of treating longer than 24 weeks. I don't know very much about genotype 3 though.
Advocate1955
The rash did indeed get worse the past few days, last night I felt like I was covered by a thousand ants. I have been prescribed hydroxyzine and betamethasone by my family doctor.
I also talked to the Lair Center nurse today and she said she will see if it's possible to do a viral load or at least a positive/negative test next week, but she said it is very expensive in Canada to test for viral load.
Hi Peter. Maybe at this point don"t get to caught up in the facts and figures on chances of success and just do your best with treatment.
Hopefully the next PCR will show UND(as you are so close now)
Good luck ..
Will
Thanks for the comments. I am concerned and so I will discuss it with my doctor. The plan is for no test for negative/positive until the 24th week.
I think there are flaws in how we are treated at the Lair Center here in Vancouver .They seem extremely reluctant to do viral load tests. Before treatment began, the doctor told me my chances of SVR are 80 to 85%, but I did some research and found it's much lower - about 50% - for people my age with stage 4 cirrhosis. The doctor also seemed to ignore my diabetis and when I told him about the very unpleasant side effects of the rebetron in 2003, he still pushed for me to go ahead with this Pegatron treatment.
I felt much worse after rebetron in 2003. I had been physically very fit and energetic prior to 2003, despite having Hep C, but I gained weight even during treatment because I became much less physically active, and continued to gain after treatment so my clothes didn't fit. I became unable to feel really rested. I thought the reason for the fatigue was the increase in viral load (I know it was 250,000 pre-rebetron to 2,400,000 two years later). But a specialist nurse at the Lair Center said viral loads fluctuate all the time and so are not a good indicator of anything.
If I were you I would first try to reach true undetectability by very sensitive
PCR before you start estimating your SVR chances.
The fact is you don`t have RVR and you are still detectable.
Also being borderline diabetic you are propably insulin resistant
combined with advanced disease and previous tx failure
I would try everything in my power to improve glucose metabolism
and I would try to tx as long as my Dr. is willing to rx and insurance is
willing to pay unless you have serious sides preventing you from doing so.
just my two cents.....
b
(Geno4,no RVR,60wk,SVR)
Age < 40 years : I'm 56
Female gender : male
White race : yes
Body weight < 85 kgs : I'm close to 95
Absence of diabetes mellitus : I have type II diabetes, but just over borderline, not serious yet
Absence of steatosis on liver biopsy - not sure - I have stage 4 cirrhosis
Fibrosis on liver biopsy ≤ 2 : yes
IL 28B polymorphisms : ?
rs12979860 (CC allele) : ?
rs8099917 (TT allele) : ?
Viral load : 250,000 in 2003, 2,400,000 in 2005
I think I have about a 50% chance of SVR, because the nearly undetectable viral load shows the drugs are working. From the studies I've seen on the internet, for older people with cirrhosis and genotypes 2 or 3, weeks 17 to 24 are absolutely crucial. There's not much difference in the rates of SVR of 80 to 85% or so for young people with genotypes 2 and 3 with a 16 week or 24 week treatment, but the difference for older people with stage 3 or 4 cirrhosis is something like 18% SVR after 16 weeks to 52% after 24 weeks.
What kind of coffee is that you're drinking Will?
Advocate1955
I'll have some of what Will is having, please -)). The 3 cups of coffee sound pretty good as well.
Nope ..won"t type in the number for some reason..sorry ..however it is in the link
still not right..
Having a low VL 3 cups of coffee per day
There......I think I have it.....
sorry. The info on the last line of my post seems to say you should take 3 cups a day of your viral load??
It should have read.."having a low viral load 3 cups of coffee a day
Will
I know we are different Genotypes, but I was <43 but still Detectable at 4 weeks. I was happy to be able to continue treatment but disappointed I was not UND. However, at 8 weeks I was UND. and that helped boost my spirits. I am doing 48 weeks so I know what it means to have to extend the time of treatment.
Of course this is a very personal decision and you will have to come to this decision with your doc. but I hope you will treat long enough to have your best shot at reaching SVR. You are only 56 and potentially have 25-35 years left for living a happy and productive life.
I wish you the very best.