my ALT is now rising.. i do hope in a flare and eag conversion.. I still wonder how can I still be EAG+,. I'm aovbut 30yo and docs said many eag serocnversions happen betweeen 30/40..
sorry forgot what was wrong, it was the few weeks time to be wrong then
ideally we need a marker to show us when pegintf add on is ok, i noticed they added ip10 on the trials i guess tey are checking if ip10 can be a good marker for pegintf add on.1-2 years of hbvdna und must be the minimum, trials are requiring a minimum of 12 months for now
no Stef you're wrong.
i started TDF first and after some weeks I had added IFN (before DNA was completely UND).. so the approach was correct,,,
I think sequential PEG and TDF is better than together.
it s the opposite to be good tdf then peg add on, grmr actually had the worst combination, started with pegintf and added tdf when pegintf response started, so the little immune response started by peg was abolished by tdf
so it is known we rescue hbv cd8 response by potent antivirals tdf or etv and then add on pegintf to rescue nk and nkt cells too....i have no idea why the opposite in this combination does not work
normal BMI.. no fatty liver. 1 beer (33cl) week... In the latest days to be honest I had a lot of cakes/desserts/salami and some fried meals..
what is your weight. Do you have fatty liver? This can cause a slightly elevated ALT. I think sequential PEG and TDF is better than together.
i'll get againg hbsag quant in few weeks and will report.
Just cchecked now, my ALT is now 50 (1-47) while 2 wks ago was 22... so scared they start rising again
can you report your vitd levels, hbsag levels, fibroscan on the other thread about vit d.it ll be very interesting to put all data together and see if there is any correlation with high vit d
so i'll have a fibroscan soon and report here outcome.. docs exepct vey low stiffness even it dna is increasing (now 55000 iu) and ALT AST are normal
no sides both courses.. i was on ifn+tdf for almost 15 months..
That right Sfefano. They are salesman aren't they, hospitals and doctors. Don't get me wrong, they do a marvellous job for the community and society but maybe too much self interest.
Any side effects in Interferon grmr? and how long were you on TDF/PEG?
biopsy may read f0-f1 fibrosis better but only regarding the sample they take, nobody can predict if the sample is the same as the whole liver but
if alt s higher than 200 the doctors are right to use biopsy instead fibroscan
maybe the new fibroscan+ultrasound machine, which i dont remember the name, will solve this problem
i also agree that in your case therapy is useless, we can see very clear the difference between corrupt doctors in other countries and italian doctors, our point is cure hbv or cure a damaged liver and not sell antivirals, fibroscan or biopsy will tell if antivirals will ever be necessary since most never develop damaged liver despite active hbv
my DNA was UND after 1monto of TDF and ALT dropped form >500 to normal level during tx... I stopped TDF 3 months ago and DNA will relapse for sure...
I have Ultrasound done every 6 months and all of them are ok so far...
I am not a doctor. The purpose of treatment is not to lower HBsAg, but to lower hbvdna and normalize ALT. If these have been achieved with your treatments, then it is likely liver disease progression will be minimal and fibrosis will not advance and should regress. So I have difficulty in understanding why another biopsy is necessary A baseline biopsy is helpful because there is no previous history, so the state of the liver is often unknown and when treatment with Interferon is considered then it is prudent to make sure that liver is no cirrhotic before starting Interferon treatment.
I would ask the doctor what is the purpose of another biopsy It is true that a high ALT will increase the Fibroscan score as the liver is inflamed. But your biopsy/Fibroscan is scheduled for next year.