Hep C Discussion Forum

Hello mcmaklin,

Just to add a bit to the good advice you have already been given here. Possibly to relieve your fears somewhat of Vosevi being successful for your particular situation,I have linked below a "Reviewer's Report in depth on the Pharmacology of Vosevi.

It is thick ,heavy reading ,however if you go straight to page 38 you will notice that in the last Vosevi trial (Polaris1) more than half of the 1b patients(24 of them) had resistance at the L31 position and all 24 SVR'd (100%).(page 40)

That is not surprising as L31M and V have <2.5 EC50 Fold to Velpatasvir( So basically No Resistance)

Any physician knowlegable in treating HCV would prescribe you Vosevi for 12 weeks and rightfully feel confident ina successful outcome.

There is no data that 16wks.and/or the addition of Riba would have a better outcome,however that is a discussion you would obviously have with your physician.

Good luck

https://www.accessdata.fda.gov/drugsatfda_docs/nda/2017/209195Orig1s000MicroR.pdf

Thank you - and what does it mean in the chart Ombitasvir / substitution in scored position L31M? It was a test for how drugs work for me

i hope Vosevi will work - otherwise there will be no other options?

Hello, thank you again for ALL CARE about me.

1. How many people from the forum where taking Vosevi for genotype 1b? Do you know anyone, any real-time data? If you know anyone on the forum please let me know.

2. I am trying to explain WHY Viekira+Exviera did not work for the L31M. Is it supposed not to work for this well? 

3. There is a table down in my letter from my blood tests after treatment-  what does it mean

   Ombitasvir    |substitution on scored position  |       31M

Does it mean that Ombitasvir that I was taking did not work for L31M?

From my findings:

NS-3 condones covered 1-181

NS3 region (w.r.t M58335) - S7A, V48I, A66G, P86Q, K87A, P89S, F147L, V170l

Ns3 region (w.r.t H77) - I35V, T42S,T61S, R62K, I64L, S66G, V71I,I72T, P86Q, Q89S, , S91A, I132V, A147L, L153I, N174S, L175M

Resistance Analysis

Drug   |  Predicition | Scored mutations

Asunaprevir.   |  suspecitble | none

Boceprevir susbstituion on second position.      170I

Grazoprevir suspectible none

Paritaprevir suspectible none

Simeprevir substitution on scored position     170l

Telaprevir substitution on scored position 170I

NS5A condons covered. 1-104

NS5A Region (w.r.t. D90208). - K6R, S17A, L31M, L34V, L37F,  G49A, Q54H, K68R, S101A

NS5A region (w.r.t. H77) I8V, E14T, S17A, K24Q, A25S, M28L, Q30R, L31M, I34V, V37F, R44K, G49A, R56T, H58P, E62Q, K68R, T71S, R78K, R81S, M83T, S85H, L101A

Resistance Analysis

Drug              Prediction                                           Scored mutations

Daclatasvir    reduced suspectibility                        31M

Elbasvir          resistant                                             31M

Ledipasvir      suspectible                                        31M

Ombitasvir |   substitution on scored position    |     31M

Velpatasvir      supsectible                                       none

Hello- what experience do you have here- you Want to say that inspite I have been told to come in October I may not to get it? Shall I go to a private visit for example to Royal Free? Will it help anything ? It should be available after 3 months NICE has announced it. Please help me I am confused what to do and why you are sceptic ?

-- Edited by mcmaklin on Thursday 26th of April 2018 05:46:25 PM

Hi Mak,

I must agree with the comments by RC and Canuck, regarding the Vosevi. It’s a pangenotypic combination of drugs that is effective across all genotypes, for both naive and treatment experienced patients. It’s effective against RAV/RAS’s, so don’t spend any time worrying about that. As Canuck mentioned, give your doctor time to make the determination of what should be included. If Vosevi is the decision, Riba is most likely unnecessary considering the extremely high rate of SVR with Vosevi alone.  

Mak,

We are not docs, we can only go by what we "think" we might know, or by reading/guessing/witnessing what has occurred in the past, or by trying to decipher the studies or docs opinions on things.

We do not know every nuance of you and your hx, or your current health. That alone makes it hard for us to figure out things/to be guessing things, everything from why you might have failed your prior treatment, to what would best ensure success on your next treatment.

Your sig line data is likely not all-inclusive or up to date - What is your CURRENT VL, what is your CURRENT Fscore (by fibroscan) or by bloodtest(s)? What are some of your CURRENT LFT's, ALT/AST/Bili? Your sig line indicates your last VL was over 100,000 aprox. May 2016, and your sig. line indicates an F score of F1 aprox Nov 2015? We do not know by what method your 2015 F1 score was determined, by fibroscan or by blood test? And we do not know what your current Fscore is, and also by what method a current Fscore might have been done. (I do believe I saw you write within one of your posts, buried somewhere in here, that you "thought" a perhaps more current Fscore was aprox. F1-2?) So, what are your firm, current VL and LFT numbers and what test method(s) have they been using in you to determine your Fscores.

Have you been having abdominal ultrasounds all along to check for of hep C signs? What are the results of your abdominal U/S's?

Since your first treatment with Viekira + Exviera, have you had any other health conditions/disease processes for which you have been on treatment for, or for which they are following in you? Kidneys disease, cardiac issues, psychiatric issues, blood disorders, etc?  

Basic background info is always helpful.

___________________________________________________________________

It "sounds" as though you and your doc HAVE? decided Vosevi is the right treatment for you? Is that right, are the two of you firmly in agreement on this now? 

If so, then according to you, your only other problem (other than Vosevi availabilty) is if he insists you also do riba with it, in that case he has to show you WHY he thinks you should have riba added to your vosevi, and you would need to show him why you think it should not be added  (if you are reluctant to do riba, and/or do not think it will give you a significantly higher chance of cure).

My unprofessional opinion, speaking only for myself (not for you) I would not honestly be wanting to do riba with my vosevi, (nor would I have wanted riba added to any treatment I might have done!), if I could have got away with avoiding it, simply because of it's unpleasantness, and, because I do not think the data shows that riba makes vosevi that much more effective, but ... had I not done vosevi, say I only had sof/dac available to me as a GT3, and riba was strongly recommended, I WOULD have considered taking the riba, based on data. If I had other circumstances going on conspiring against me, and we decided riba would have helped me with the sof/dac or any regimen, then I would have done it.  

You and your doc need to convince one another, one way or the other (add riba or not add riba).

All the studies and data, and North American recommendations we have been providing, reviewing and discussing here are not necessarily saying you must do riba with your vosevi, but we do not know as much about you as your doc does.

Take the studies to your doc, and ask him to show you his data, as to why he thinks you should add riba. 

____________________________________________________________________

In the past, for other people, on dif drugs, when riba was deemed "required" to be added, there have been some extentuating exceptions made, to not use it, but generally not based on the fear of sides from riba alone - there had to be some valid contraindication, the uncomfortable sides were not as important as the value the riba would provide. Riba might be contraindicated based on pre-existing conditions, such as cardiac/hepatic issues, blood problems such as pre-existing anemia issues or other blood disorders, psychiatric conditions (being under treatment for severe psychological states), but unless you have a pre-existing pre-emptive reason for not doing riba, then you and your doc have to base your decison on whether to do riba or not, solely on the likelihood of successful cure, with it or without it. 

We have sometimes seen docs ramp riba dosages upward in a graduated fashion, or downward (in response to the severity of sides like anemia say), some people have had it discontinued, many continue the full dosage for the duration of their other drugs as long as it is tolerated - it all depends on his thinking and how your body reacts to it.

_____________________________________________________________________

You are going to have to "pre"-arm yourself with facts, and have a good discussion with your doc about the pros and cons of adding riba to your vosevi.

Hi Mak,

This is part of what I wrote to you earlier in the week, I'm just repeating it here again:    

... PS - BTW - re: Mavyret ... Vosevi is a number one choice over Mavyret for re-treatment of a GT1 who is BOTH 5A/3/4A experienced. Vosevi DOES NOT restrict a 5A/3/4A experienced person from Vosevi use, but MAV DOES restrict a person who has had prior 5A/3/4A experience. Your prior treatment Viekirax/Exviera contained the 4 drugs ombitasvir/paritaprevir/ritonavir/dasabuvir, of which the ombi is a 5A and the parit is the 3/4A, this then makes you BOTH 5A and 3/4A experienced. The way I see it, no matter what 5A or 3/4A RAVs you may own, simply because you are 5A and 3/4A experienced person, Vosevi is your choice (perhaps with, or without riba, depending on your doc's view) ...

Now, in regard to adding riba to Vosevi? -aside from the studies provided to you thus far that were showing any significant benefit of adding riba to vosevi, and according to the AASLD guidelines, here is yet another "North American" view of the guidelines and recommendations (if you can get linked into this, to read everything within it, there you will find under DAA experienced people, the few times riba IS being recommended to add to a treatment (ie. specifically in the case of GT3's, who are cirrhotic, and who are NS5A experienced, then riba is suggested):

"CCO - Clinical Care Options - Hepatitis" -January 25, 2018 - HCV for Primary Care: Making It Easy With Simplified Guidance

I see that in your signature now. Once we start writing, the signature goes away. It's my opinion that your doctor is considering the addition of Ribavirin because you relapsed following the administration of a NS5A inhibitor. If the professional data is correct, and I have to believe it is, then Ribavirin is not indicated in your case. That's something you have to bring up with your healthcare team. Ultimately it's your decision after a conference with your doctor.

The following graphic presents the Polaris data. It doesn't leave much room for debate. The use of Ribavirin didn't provide any advantages. This is my opinion only...

Hi Mak,

I‘m going to add the official pharmaceutical information on Ribavirin at the bottom. It will simply provide you with the professional data on the drug. There is a requirement to avoid pregnancy the entire time you are exposed to the drug and (yes) 6 full months following cessation of the drug. That has been thoroughly studied and researched by the US FDA, as well as other global professional organizations. 

Ribavirin isn‘t a pleasant experience. I took 1200mg per day for 7 months and I won’t lie, it was tough. It was tolerable though and the side effects tend to escalate the longer you’re on it. One thing you can ask your doctor is whether you will be taking a dose based on your weight or a lower dose, such as 400, 600 or 800mg per day. The side effects are absolutely related to the dose and time taken. You may be allowed to take a lower dose for a lesser amount of time and still obtain some of the benefit. That’s going to be a decision made by your doctor. 

Your doctor seems to have some ideas, but hasn’t concluded what is the most effective route or treatment protocol. Do your research, compile a list of questions and ask your doctor to sit down and answer them. Vosevi isn’t a protocol known to use Ribavirin as part of the plan, but it has been done. If cost is a barrier, I’m not sure I follow the logic behind adding Sovaldi (Sofosbuvir) to Mavyret, even though it’s also being prescribed off label (atypical). Without going back through your old posts, I simply don’t understand why your doctors don’t simply test you for your current RAS/RAV status. Vosevi without Riba seems to be indicated in your case. I realize obtaining it is the obstacle right now, just stay on top of it and never give up.

If you use our search function at the top of the page, you can search the Ribavirin discussions we’ve had over the years here on the forum. Pay particular attention to posts by Mallani. He has presented some very good discussions on the topic.

Ribavirin Monograph

Hi Mak,

Ya know, I think you should re-read some of the info that we have already covered, right within this very thead! A lot of good discussion, and many answers to your different questions were attempted here prior. Some of it we are just repeating now. Look way back in this thread starting about Aug 26, 2016, some of the studies you are wondering about now, have already been discussed and are right there within this thread ... plus ... if you "search" the recent thread Tig mentions ALL ABOARD THE VOSEVI TRAIN , you will find some of the recent links Tig provided you there, or, if you search and re-read the thread SOF/VEL and SOF/VEL/VOX , you will find a lot of the Vosevi study data there too.  C.

Hello Please, I am not able to find it, I am trying for some time already. You sent me some data that we could read that with Vosevi Trials some people with Genotype 1 had worse results with cure than those who did not take ribavirin? This is about Voxilaprevir. And that Riba does not make much difference.. Please.

What are you relating to? 

"Tig has brought you up to speed again (in the re-presenting/re-reading of the old vosevi trial data) - with and without riba - and, he has already re-reviewed the good data we have already posted on the site in regard to how many relapsers with RAVs come to vosevi for very successful re-treatment, so I won't keep going there to that subject matter,"

Thank you - I wrote to HepcTrust and am on their mailing list. 

By the way - obviously I hope to get it soon in UK, but why you discourage to receive medicines from India when they become available - let us say from Natco or Mylan?

And the second question - I cannot see any way to get it from Australia, how?

Hi Mak, 

Tig has brought you up to speed again (in the re-presenting/re-reading of the old vosevi trial data) - with and without riba - and, he has already re-reviewed the good data we have already posted on the site in regard to how many relapsers with RAVs come to vosevi for very successful re-treatment, so I won't keep going there to that subject matter, I could just repeat a lot of what I said in my last post to you below (Nov 25), or from older posts that Tig and I and others have exchanged with you in the past but i will just stick to this instead ...

You are in UK, your doc is in UK, and you say you cannot get vosevi UNTIL you can access it generically out of country??

Are you sure about that? I would suss this, for sure, as access could be your largest impediment affecting your long term planning.

(Perhaps more so than anyone's focus on your 5A RAVs, or on your TT status), I am rather firstly concerned about your "access-to-vosevi" problem.

WHY do you and doc think you will not get vosevi in the UK SOONER than getting it via a generic route out-of-country?

Did you try to sleuth the UK Gilead contact I directed you to (from the Nov 25 post below), to see if anyone there could answer you about how soon you might be able to access vosevi in the UK?? I'll post it here again (below), it could be a useless dead end, but if I was having difficulty getting vosevi, being told I cannot get vosevi in the UK anytime soon, and if I were you, I would like to hear that from Gilead themselves, and to be able to ask them ... if not now, then when.

Contact address:

Gilead Sciences International Limited
Flowers Building
Granta Park
Abington
Cambridge
CB21 6GT
United Kingdom

Or, have you tried to seek info from any other Gilead contacts via any of our other Gilead links that are already found within our website here? PAYMENT ASSISTANCE PROGRAMS  All Gilead contacts listed in there are Canadian or USA contacts I believe, but perhaps they can link you better to someone for specific info about the vosevi situ in the UK.

There is also the UK resource Hep C Trust ( http://www.hepctrust.org.uk/about-us ) to inquire with about how soon vosevi may be available in the UK.  C.

PS - BTW - re: Mavyret ... Vosevi is a number one choice over Mavyret for re-treatment of a GT1 who is BOTH 5A/3/4A experienced. Vosevi DOES NOT restrict a 5A/3/4A experienced person from Vosevi use, but MAV DOES restrict a person who has had prior 5A/3/4A experience. Your prior treatment Viekirax/Exviera contained the 4 drugs ombitasvir/paritaprevir/ritonavir/dasabuvir, of which the ombi is a 5A and the parit is the 3/4A, this then makes you BOTH 5A and 3/4A experienced.

The way I see it, no matter what 5A or 3/4A RAVs you may own, simply because you are 5A and 3/4A experienced person, Vosevi is your choice (perhaps with, or without riba, depending on your doc's view).

Hello, for now my only option is to wait for Vosevi from India. 

I have some more news though to remind you:

 I am 2 years after failed Viekira+Exviera Genotype 1b. Do you think I need a Ribavirin? I assume Vosevi will be good for me and will work for this L31M

From my findings:

NS-3 condones covered 1-181

NS3 region (w.r.t M58335) - S7A, V48I, A66G, P86Q, K87A, P89S, F147L, V170l

Ns3 region (w.r.t H77) - I35V, T42S,T61S, R62K, I64L, S66G, V71I,I72T, P86Q, Q89S, , S91A, I132V, A147L, L153I, N174S, L175M

Resistance Analysis

Drug     Predicition Scored mutations

Asunaprevir suspecitble none

Boceprevir susbstituion on second position.      170I

Grazoprevir suspectible none

Paritaprevir suspectible none

Simeprevir substitution on scored position     170l

Telaprevir substitution on scored position 170I

NS5A condons covered. 1-104

NS5A Region (w.r.t. D90208). - K6R, S17A, L31M, L34V, L37F,  G49A, Q54H, K68R, S101A

NS5A region (w.r.t. H77) I8V, E14T, S17A, K24Q, A25S, M28L, Q30R, L31M, I34V, V37F, R44K, G49A, R56T, H58P, E62Q, K68R, T71S, R78K, R81S, M83T, S85H, L101A

Resistance Analysis

Drug              Prediction                                           Scored mutations

Daclatasvir    reduced suspectibility                        31M

Elbasvir          resistant                                             31M

Ledipasvir      suspectible                                        31M

Ombitasvir    substitution on scored position         31M

Velpatasvir      supsectible                                       none

Could you Please clarify? I do not understand - is anything worse to get than it was?

Unless Gilead cuts a deal with the generic manufacturers in Europe and Asia, I think it will be years before we see it. 

Unless Gilead cuts a deal with the generic manufacturers in Europe and Asia, I think it will be years before we see it. The patent dates have been extended out over a decade preventing the legal release of any authorized generic.

Vosevi generics [nope]

Hi Mak,

Glad to hear from you again.

In your country, have you already confirmed that vosevi (as a "rescue regime") has not been approved (in principal) for use???? And that it won't be, in the near future???

It would be best if vosevi was offered to you, in your country, by your country. If you have already exhausted EVER getting vosevi in your country, and you are thinking you can source it elsewhere (out-of-country - ie. India or UK that you were asking about) - there are people who can help you buy your own drugs out-of-country, but, as you are probably already aware, vosevi (sof/vel/vox) is not yet being sold like that (out of India). One can source epclusa (sof/vel) but not vosevi (yet), certainly not that I am aware of. And it may take quite some time before vosevi can be sourced this way, perhaps even longer than we saw it take for sof/vel to come out of India.

You have had a prior trip and physical consult in the UK with a UK doc there, (but unless you have dual citizenship, for your country AND for the UK) then I am not understanding the logistics of how you would be able to get a doc in the UK to prescribe and treat you with vosevi (even if the UK system chose to give a pt vosevi as a first choice). Have you re-checked with your "doc contact" in the UK again, about your wish to recieve vosevi treatment from him?

UK, Can and US have all had vosevi technically/officially "approved for use" but that does not necessarily mean the citizens of these countries will get it (even if the pt. is convinced that vosevi is the best rescue regime for them). Many variables/restrictions/conditions/limitations could apply, and residents of those countries may still be offered dif drugs first.

Whether it be UK, Can or US, it has really been only quite recently that citizens of these countries have been a bit more successful in more easily being offered even things like epclusa (even tho the epclusa approvals were fast-tracked and the approvals have been standing for quite some time now) people are still being offered lesser or dif regimes first. I can see the same thing happening with vosevi, although approved for use in a country, people may be slow to receive it. (ie. In the US, with vosevi being approved for use, and then rolled out available in August, I have still found it impossible to find out how many US people have actually been successful in obtaining their vosevi by prescription).

I do believe it will be quite some time yet before an out-of-country vosevi-like generic will be available for purchase. It will likely follow the same pattern as we saw happen with epclusa. I think the in-country roll-out use of vosevi is slow (maybe will be even slower than epclusa was), and that the out-of-country development of a vosevi-like generic version will be slower still than the out-of-country generic epclusa development was.

Good you have had your RAVs re-checked, and it's good that vel is not on your list of no-go's. 

You can double-check with AUS people like Greg Jeffreys and Dr. James Freeman and the "fixhepc" people,  or with that nice fellow Nirav Sangoi, about when they think out-of-county vosevi-like generics might be coming available.  

Aside from Gileads vosevi, I have not heard of any other pharmaceutical companies making any announcements about their own vosevi-like formulas being made available for sale soon. As well, I believe Gilead was just successful in having some of their licensing extended to something like the year 2023(?), so events like these may have a bearing on generic dvelopment. Gilead seem to have control of vox/vosevi right now.

I do not think you will find a source for out-of-country generic vosevi-like formulas yet, anywhere. There has been talk of  "Beacon" and about 4 other pharmaceutical companies exploring development of generic vox, but I do not think their generic vox will be sold seperately. I believe their generic vox will be sold (just as Gileads formula is), as a triple formula, an "all in one" pill, of sof/vel/vox.

Dr. Freeman has had at least 4 dif Redemption "trials" that have been occurring over time (accessed via "fixhepc"). They had various drug "trials" - this one, "Redemption Trial #4", was only for epclusa (sof/vel) - https://fixhepc.com/r/root/redemption/4

You can check resources such as Greg Jeffreys/Dr. Freeman to see if they have any plans for further Redemption "trials", specifically a vosevi one - I have not looked lately, but I did not see them offering a vosevi Redemption "trial" via this route as yet.

If you do get vosevi, it will just be up to your doc whether he thinks the addition of riba would benefit you further, or not. 

That's all I can think of for now, if I hear anything else, I will of course let you know. C.

Hi Mac,

RC is right, Vosevi is mentioned as the initial recommendation with Maviret a suggested alternative. The advantage of a 3 drug regimen is it hits three links in the chain. All you have to do is effectively break the cycle of replication at any point. The subject on RAV/RAS is complicated. If a particular variant is resistant to one drug, it may be susceptible to another drug in the combination. That's the benefit of a multi pronged approach NS3/4, 5A & 5B protocol.

Mac, My choice would be VOSEVI because you have lready treated with VIEKIRA PAK. VOSEVI is a rescue therapy drug that hits 3/4-5a-5b. And has a 98% SVR across the board.Viekira pak hits three also. Are you cirrhotic?  That could explain your relapse.It would be interesting to see if the MAVIRET hit the same spots as the Viekira-pak.   RC

Hey Mac,

Thanks for posting that resource, it's a good one and comprehensive. Just looking at the information briefly, it would appear to me that they are recommending 16 weeks of Maviret as a good option for you. It will take some additional reading to fully grasp all of that data, but they're getting closer to figuring out this RAS dilemma. 

The pangenotypic tablet includes the NS3/4A protease inhibitor glecaprevir and the NS5A inhibitor pibrentasvir. It lacks the NS5B inhibitor. It is still very effective without it. They call it Pangenotypic, it is good for all genotypes.

I second that Tig.  MCM may want a second oppinion.  RC

Hi again mcmaklin,

Nice to hear from you - we haven't heard from you in a while! - I can see you and Tig (and RC) have "gone deep" into RAV's and the "what will I/what should i end up with" for treatment again.

This is a good thing to do, to try to keep abreast of all the possibilites. It must be immensely frustrating not be able to have all therapies available to you or offered to you, and the waiting involved. So many people (TN and TE) are being so easily/quickly cured nowadays, I know you are happy for them, just as you were for your sister's success, but still, this must feel a very long unfair haul for you.

In reviewing the many posts we have all shared together over time - we keep hoping to hear that you are imminently being offered a good treatment. Maybe you are now closer with the likes of the newer Abby and Gilead doubles and triples that have or are coming to the fore.

Have you been doing ongoing searches of all the trials all this time? Didn't you or your doc see any Abby glec/pib trials over there (or in the UK), at any point? Did you and your doc follow the Merck ruz/uprif/grazo trials? 

I do recall you bringing this up long ago (about your doc mentioning some combo of adding Gileads sof to Abby's glec/pib), and I do "vaguely" recall something like that, but I could not find that particular sof use, nor did anyone else I think (back then at that time) - there was no solid ref. of a study to where sof was added to glec/pib. Easily found however, was riba being tested out added to glec/pib in Abby's older trials - but Abby went to market heavily touting how effective/pan Maviret is, with a special emphasis on it being "riba-free".

I like the theory behind triples, but I do not like riba much as a third or added drug tho! Especially palatable/acceptable are all the "new" NS5A's, NS5B's and 3/4A's that have come out or are coming out nowadays (as doubles OR triples) that are riba-less. The new drugs are becoming very competitively effective, very pan, more effective, powerfully proven to work well for TE and in many cases very close for TN alike.

The efficacies data IS in the trials, you just need access to the drug choices!, and then, your work-up "re-done" for your doc to select and confirm the best regime for your re-treatment.

Man, I hope a doc (in UK OR home country) can find you access to your best drug choices. When was the last time you saw your doc to ask about getting Vosevi (or another regime he feels would be the best for you)? Keep banging on the doors, in UK and home, one IS going to open, soon I hope. C.

The repeated RAV testing is kind of a waste until you're ready to start treatment. The RAV's you mentioned, the L31M (common) and Q54H (not so common) are both susceptible to current drugs, but you have to remember, these new drugs are coming at us regularly and one never knows what will be offered next or with what. That's why testing for RAV's now and waiting 6 months or a year to treat serves little purpose. NS5A/B RAV's are long term, but nobody really knows how long term. Could be a year, could be five, don't know. What they can tell is what drugs are more effective and what isn't against not only the virus, but resistance profile to existing RAV's. If during the year wait, one of these variants should disappear or weaken, then your options might change. 

Basically, you're right. Vosevi and Maviret are both very effective treatments. Given adequate exposure to either of the drug regimens, I'm confident that you will kill the virus. Remember what RC said about the tire spokes? If you had zero RAV's, then it wouldn't matter how many spokes on the wheel you removed, it would stop the virus from replicating. Since you do have two known RAV's at this time, using a drug regimen that attacks 3 spokes instead of Maviret's 2 spoke attack, your odds theoretically should be better. "Should" is the key word here. Like I said, they are both good regimens and both appear to be recommended for you at this time. If you can obtain Maviret, I certainly wouldn't turn it down. All you have to do is have one of the drugs do it's job and the virus will cease to replicate. You must expose yourself long enough for the drugs to work and even though you have an RAV that will cause some "resistance" to the treatment, it doesn't mean it won't work. If it said "prevents" the intended drug action, then for sure you wouldn't want to use it. They can tell the strength of a particular RAV and the likelihood of success given a certain protocol. Your doctors should be able to ascertain the correct drug regimen and protocol for you quite easily once you are ready to start. 

This can be terribly confusing for all of us and I wish I had a perfect explanation for you. This stuff is complicated, but we're learning about it all the time. I'm confident that with the proper testing at the the correct time, it will allow your doctors to determine the best regimen for you. A good specialist will steer you in the right direction. When the opportunity presents itself, and your doctor recommends a particular regimen, do it. You have to place trust in your doctor. Together we can offer discussion and debate here, which will give you the chance to ask some knowledgeable questions. If you aren't getting the right answers, then you have to make a decision based on that. The new DAA's are quite effective and if you take them long enough, you're going to win the battle. I'm pretty sure of that....