I would presume your original Consultant looked at the research at that time and came back with
24 weeks as you’re F4 with a very high score -I presume the fact you’re UD from early on and the latest
research suggesting the extra 12 weeks has very little bearing on the end outcome he’s now telling
you 12 weeks is fine.

If you’d all ready paid for 24 weeks Id stay the course and do at least another 4 with your score Id
probably do the extra 12 you have zero to lose.

You consultant’s advice would appear to be referencing this recent small study:

http://www.ncbi.nlm.nih.gov/pubmed/26786792

Where you can read the words “all …. svr …. regardless of duration”

However you might also read it more closely and see

ALL = 19

DURATION = 12 or 24

If they randomly divided the 58% F4s into 12 and 24 week groups we would have exactly 5 people in 1 group and 6 in the other.

If 1 F4 person had failed in the 12 week group that would have reduced the success to 80%!

GT2 is probably the easiest to treat given that Sof+Riba will get a 97% SVR rate – much higher than for GT1 or GT3.

That said you are cirrhotic so you really want to get this right the first time.

If at some point in the future a decent sized study comes out showing that F4 GT2 patients get the same results on 12 vs 24 weeks the worst case outcome is that you have taken 12 unnecessary weeks and wasted $1500 AUD.

Psychologically if you are one of the small minority that don’t SVR at least you won’t be beating yourself up for not taking 24 weeks.

If it was me I would do 24 weeks.

The entire knowledge base for GT2 is small. If you use the decision support tool at http://fixhepc.com/hcv and put in your data in the results section there is a button called [Show Trials] – here is everything I could find prior to that new small study.

Sofosbuvir Ribavirin

NAIVE
default: svr: 95%, trials: FISSION 97% (58/59) FUSION (12wk) 96% (25/26) POSITRON 92% (85/92) VALENCE 97% (29/30) Aggregate 95.1% (197/207)
w16: svr: 100%, trials: FUSION (16wk) 100% (23/23)
F4
default: svr: 83%, trials: FISSION 91% (10/11) FUSION (12wk) 60% (6/10) POSITRON 94% (16/17) VALENCE 100% (2/2) Aggregate 82.9% (34/41)
w16: svr: 78%, trials: FUSION (16wk) 78% (7/9)
FAIL
default: svr: 92%, trials: FUSION 92% (24/26) VALENCE 91% (30/33) Aggregate 91.5% (54/59)
w16: svr: 96%, trials: FUSION 96% (23/24)
F4
svr: 88%, trials: VALENCE (7/8 )

Sofosbuvir PegIFN-α Ribavirin

NAIVE
default: svr: 95%, trials: LONESTAR 96% (22/23) BOSON 94% (15/16) Aggregate 94.8% (37/39)

Sofosbuvir Daclatasvir

NAIVE
default: svr: 92%, trials: UN-NAMED http://www.ncbi.nlm.nih.gov/pubmed/24428467 92% (24/26)
w24: svr: 96%, trials: AI444040 (24wk) 96% (25/26)

So the entire body of knowledge for Sof+Da is only 71 patients small…. Of that 26 + those in the new study did 24 weeks. The impact of F4 and Past Treatment experience are just not known, so need to be extrapolated from other genotypes.

In time your specialist may be proven right – or wrong. The problem is that right now we (doctors) don’t know precisely so are all just making guesstimates.

No worries.

Yes, I can write scripts, and yes I am seeing patients, just booked out at the moment. Send me an email james at etc and I will fit you in somewhere.

Your clinic has a duty of care; If you choose to take on board another Dr’s opinion they
will and have to continue too monitor you.