Hep C Discussion Forum

Hey John,

That blood work schedule is fairly standard and correct as written. I agree with your doc, SVR 12, even SVR 4 has proven to be accurate of a sustained viral response, as in dead Dragon. The old SOC's were more prone to relapse during treatment and nearly always by EOT +4, if it was going to happen. These new DAA's work differently and I've seen more success with them than ever before. I do have a friend that completed 12 weeks of Harvoni, and didn't achieve her undetected status until EOT +12. She tested "Detected but <15" from about week 8, if memory serves me. She was convinced that she would relapse, but her EOT +12 viral load came back undetected and she has remained that way for two years now. So I always tell people, it's the +12 week viral load that counts. Of course it's always nice to see that result come back undetected as soon as possible and usually does before the end of treatment, but it doesn't always work out that way. The large, round person doesn't sing until EOT +12!

Good luck! We've got some proven advice when you're ready to rock n roll... I look forward to your progress!

Hi L.,

Oh dear! I was sorta hoping I wouldn't hear you say what I was suspecting (about "costs"), but alas, it is very true. How tough and horrid that system IS down there, when there is this big out of pocket aspect. And that there is no in-country choice about it, that for you the "improved" choice ended up being ... having to spend out of pocket about $5000.00, already! Nasty, but ... worth the cure mind you. I cannot say our system up here is all that people think it's cracked up to be either, I could go on about the nuances and realities of health care in Canada, but it's too long and convoluted to do justice to that topic in a post. Suffice to say, not necessarily access to "treatment" alone, but more so drug "choice" that has been and still is too slow to come and people have and can experience "limitations" on the public "system" for various reasons, especially when you get down to the "fine-print" sometimes. A couple of Canadian folk we know, right around here, not so very long ago either, had to get their own (superior choice) drugs out of country due to this very problem. Sad, that cost/access (of sorts) are problems that can still be found "in the way".

Your doc sounds good, I agree wholeheartedly with all your doc has done and expressed. I fancy and venture to say I feel the "early" crashings we witness (that you have also noted about being on these new/good/potent DAA's) only heralds/spells the success of a person's outcome! We seem to see this early crashing with quite a few of the newer DAA's (but i think especially so with VEL) - I could well be "over"-optimistically generalizing too much, but I'm mostly just counting the early crashed VEL heads on this site as an example. I believe the early crashings (the potency of these new DAA's) carries a lot of weight - I am not so much relying on or dwelling on "stats about relapse/late relapse" these days anymore (especially in your case, period), and certainly not beyond SVR 12, in this era of these powerfully effective drugs! 

My interest is only in having you know that your fibroisis will reassuringly be followed and for you to be able to obtain your Fscore regression feedback (that I personally found soooo rewarding), I would be ecstatic if your next fibroscan occured at one year post-treatment, as long as it does get continued following. That was my only impetus in pushing for SVR 24 following - we'll all be just as happy to help celebrate your 1 year SVR especially knowing your (by then likely) reduced Fscore and evidence of other improvements! You may just end up pleasantly surprised how much resolution/regression you gain!

I was lucky to get in a further trial (after my drug trial), where i am followed at no cost by the drug company (well... relatively no cost to me, in theory!) - dif story if one has to pay out of pocket for everything, or rely on standard bureaucratic bean-counter systems to try to get max. following. The drug trial companies seem to be more motivated to spend the money on you to follow you. I am a big believer in good following. I get many checks (every 6 months for the next some years) to follow my health and fibrosis levels. Fibroscans/and many bloods included/I've also had one CAT scan and one U/S so far as well. I was not thought to have a higher Fscore than F4/12.6 kPs's pre-treatment. 

So, aside from your 2 week VL/bloods, you did not have today, and will not have any further VL/bloods done until the EOT one?

Did he express an opinion to you about what best to take for pain? 

It must be such a relief for these docs, to be able to give to us, and see us getting these good drugs these days! C.

Hi lamassu,

Oh that's great, you reported back right away! Sounds like a good visit with your doc! 

So, did you have (or will you be getting) a 4 week blood draw done for VL and LFT's (aside from the 2 week one you had done)?

I assume from what you say, you two do have planned another EOT VL and then a EOT+12 week VL. (Yes, some docs are not doing SVR24 week VL's, when you have had early UND's at 4 weeks and at EOT and have a SVR12). 

Still, at F3, kPa 12.4, that is still significant fibrosis (which WILL in all likelihood regress and resolve/improve - which has probably already started to improve by just being on treatment!) which (as part of your health following) I (personally) would have another "health" check-up done at the EOT+24 week mark, (and if it were me) I would still throw in another VL along with standard LFT's (just because) AND have a re-assessment of my fibrosis levels by fibroscan or other blood markers, just so that you can follow your post-treatment improvements. If your hep doc cuts you loose after SVR12, you can always avail yourself on your GP for requisitons for VL/bloods and a fibroscan at the EOT+24 week mark, perhaps another U/S as well, if there were any abnomalities at all noted from your first U/S, just to see if things look to be resolving there too. It would be good to have this kind of feedback at the EOT+24weeks mark, to know your liver is resolving it's prior 12.4 kPa. I would still ask your hep doc for a repeat fibroscan to be done, at EOT+24 weeks, even if he does not think a VL is required then. 

Here's one kPa scoring range scale (many other scoring charts do NOT consider cirrhosis to be occuring until you are in the 14 or more kPa range):

https://encrypted-tbn0.gstatic.com/images?q=tbn:ANd9GcSFWbc6KXXW5JQRtv-iopGpwe5SJTorGZPeOaLTjqBj2Q-3VKyW1g

Interesting, your doc's stat on 10-15% of his GT2's being 2a/2c's! Thanks for inquiring. You are unique, but not rare eh!?  

No doubt! your doc is pleased with your good response to epclusa, a mighty early "crash" of your VL, within 2 weeks, you gotter made bro. I am glad your visit with him made you feel good and reassured about all your good news!  Epclusa IS a VERY effective drug, Gilead created a wonderful NS5A (VEL), I'm so glad you got it and I am sure your doc is glad he could give it to you.  C.

BTW - you mentioned (prior) that (luckily) now being on medi-care that this opened the door for you to get treatment (whereas before, treatment was unattainable/unaffordable) - did that mean your cost was only "reduced", that you still had to pay something for epclusa? 

Sounds all good. I hear ya about the period of heavy fatigue. But so glad things have improved since then! That's what we like to hear - good pills, good food and water!  Yay today - "week 4" under your belt already! Congrats. Wishing you a good visit with your doc tomorrow. C.

Hi lamassu,

Hey, nice sig line BTW!  Interesting and good your pre-treatment ALT/AST was nice and low - one very good thing!

How's it all goin'? 

You had mentioned that for the about 6 months prior to tretament that you had been having fatigue get in the way, and that you sense some relief on that front already since starting the epclusa - how nice, I wish I had experienced some of that while on treatment, I was not lucky to sense that for quite a while until after treatment, it's quite a rewarding bonus. I had to be pleased with just my stellar virological response to the magic vel and other drugs Gilead so kindly created for me, and with watching my labs improve miraculously! I am still reveling in my improvements! I thank my lucky stars, everyday, for wining a seat in my trial and for Gilead and my doc for curing me.

Hey, did your doc ever elaborate to you on your unique GT2a/2c status? Just curious if he defined or explained anything on this interesting subject to you.

Hope you are continuing to feel OK, and are drinking that LOTS of water! Are you taking your epclusa with a meal or without? Later,  C.

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Canuck wrote:

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Hi lamassu,

You have it right, to always inquire, then you with your doc can doc make the best decisions.

There are subtleties in the effects with drug to drug interactions, and even things as simple as an "antacid" or "food" that you can eat, that can have an effect on drug absorbtion.

The bottom line for epclusa, is that a patient may take epclusa with food or without, but, if you read through the epclusa monograph carefully you will see how thoroughly drug to drug and other interactions have been studied.

http://www.gilead.ca/application/files/3415/0695/6820/Epclusa_English_PM_e186388_GS-002.pdf

See: (Regarding even a simple antacid) - "Table 7".

See: (Regarding food) - "Action and Clinical Pharmacology" -  aprox. page 29 - "Effects of Food". Note that there IS an effect of food (moderate/high fat/versus no food) on the "extent" of absorbtion, and/or the "delay" of absorbtion, but that the bottom line is that there is NO "SIGNIFICANT" reason to advise a pt. to take epclusa with or without food.

My regime was different than yours, I had a NS3/4A added (VOX) - the "Vosevi" monograph dictates I should take my med with a meal. 

Just thought I would bring to your attention all of these other things, being that we were exploring "interactions".

 

Here's that link I spoke of previousy, regarding differing GT's and their "clades": About Genotype/Subtype - Lists - Geographical Locations , there is also a story around here about some of Gileads early trials where they were wishing to recruit only certain limited GT's for an epclusa trial, one fellow got started in the trial, along with all the rest, identified as the appropriate GT - only by happenstance with further admission genetic following was it discovered that his prior GT was REALLY, in fact, uncovered, to reveal he was truly a GT6! No GT 6's were supposed to be recruited for inclusion in this particular trial. He was (luckily) included and of course cured. Bonus for Gilead was that they now had to include this cured GT6 fellow, which only helped to boast (earlier than planned) how panogenic their epclusa was! There can and have been other odd cases of "mistaken identity" when it comes to genotyping! So, it's a good rule, determine GT, then pick the best treatment.

BTW - did your doc thoroughly check your hep A/B immunity levels prior to your epclusa start?

Sorry, to hear about your arthritic discomforts. Hope you and your doc get that covered well enough.  C.

 

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 Yes he is very thorough. I had been vaccinated against both hep B and A years ago and immunity levels were fine.

Tig wrote:

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I would give Kratom a pass while youre on treatment. You can go 12 weeks without it. Youre right to discuss it with your doctor, there are no experts here, especially when the question is as serious as this. There could be a serious drug interaction between the three medications, Kratom, Sofosbuvir and Velpatasvir. You dont want to interfere with the absorption or excretion pathways. Too much or too little of either could have some severe results. The rule is to avoid any and all supplements and use only approved medications with these DAAs. Thats just a knowledgeable opinion. Hope it helps.

 P-gpinducersand/ormoderatetopotentCYPinducers(e.g., rifampin, St. Johns wort, carbamazepine): May decrease concentrations of sofosbuvir and/or velpatasvir. Use of EPCLUSA with P-gp inducers and/or moderate to potent CYP inducers is not recommended

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Well reasoned advice Tig thank you kindly. In my experience you can put up with almost anything for three months. Those who had to endure the earlier treatment options for Hep C might take issue with that though. When I talk to my specialist next week I will see what he thinks is best to moderate my chronic pain from arthritis but would not interfere with Epclusa.

Canuck wrote:

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Hey, neat lamassu, to hear back from you already.

Thanks for all the info. 

Ya, I caught on that the F3 WAS by fibroscan (just like you had written the first time - had I not overlooked it at first!) but good to know that you have not had a fibrotest in addition? 

Maybe, aside from the kPa number from the fibroscan, you could also inquire whether they additionally did a fibrotest that was not mentioned as yet.

Good about the U/S, but it is not just cancers (or HCC) they look for, just a simple U/S can provide them a wealth of info about your spleen, gallbladder, pancreas, kidneys, liver (sizes/shapes/conditions) even indications of fatty livers etc., so very good you had one. If you are curious, you could ask for a copy of the radiologists interpretive report (his impressions) regarding your U/S, and see the written description of what the radiologist notes/sees.

I agree with folks who have posted to you here, about water drinking and about how stellar your (now) liver function test (LFT) numbers are!! Really good news that they are within normal limits. Do you have a "pre-treatment" ALT/AST to compare back to? 

Sorry about this, but am I ever tickled about knowing the nuance of your GT2! I have heard of/read about people possessing more than one "sub-type" but as far as I know we (until now) have not known a multiple on this site! Very exciting for some of us who are nerdy interested! There are some fairly rarely occurring things (and amazingly interesting things, to me!) one can read about many of the various GT's - some GT's that "can change", other GT's that mimick other GT's, differing GT's that are "co-related" to other GT's , and others who possess two sub-types such as in your case. Very interesting to me. (We were discussing this in a prior thread once, I'll see if I find that again and later link it to you here). As a GT2a/2c you are unique, but it will NOT be any kind of an obstacle whatsoever as far as your treatment, so no need to fret on that account.

So, with you going back to the doc next week for an appointment, I am thinking he might be doing a 4 week VL on you (maybe) in addition to your 2 week VL already done. Look forward to as many as he will do for you through treatment, the feedback is always reassurring. You should also get a VL near or at end of treatment (EOT) - week 12.

Other than HCV, do you have any other health issues for which you are having any ongoing treatment/being followed for?

Glad you have met a few of us here now, we are glad to keep company with you!  C.

 

 

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Hi Canuck,

The only other concern is osteoarthritis pain. OTC meds don't help much I do have an rx for tramadol when I have a bad day but for some reason tramadol does not work well for me. Hydrodocone does and I can get a script but I do not want to become dependent on pain killers.

This may sound off the wall but at the urging of a good friend I tried Kratom for arthritis pain and got surprisingly good results. I stopped kratom before Epclusa based on this information but will talk to my specialist about kratom use with Epclusa next week. I certainly can not risk any med that would interfere with the Epclusa clearing the virus.

Any experts here on this forum with an opinion on Kratom alkaloids interacting with Epclusa? Thanks.

Welcome from me too.

Im super excited for you to be feeling better already...and those numbers are amazing. Yay

A

Canuck wrote:

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Hi lamassu, 

Welcome here, glad you joined in.

Very glad you finally succeeded in getting a treatment, and a very good treatment at that too I must say.

Sorry about your reasons for delay along the way since the '90's. I know what you mean, about the lack of confidence in the meds available until Harvoni-times. And sorry about the difficulties in accessing/affording the new DAA's, but thank goodness about getting on Medicare and how that opened the door for you. A long wait, but you'll be OK now!

Epclusa is your new best friend, and you have friends here too, just fire away if you have any questions or want to discuss anything.

I was lucky enough to get epclusa as well, but mine was via a trial and I also had another (third) drug added (vox) - I was on "vosevi". I would have never got it had I not been successful in pursuing my trial seat.

You and i are lucky to have recieved Gilead drugs (me as a GT3a and you as a GT2), very good your doc got it for you. I know how you felt with your first viral load (VL) returning at a puny 50! Same for me, felt miraculous.

Do you happen to know what your ALT/AST/billirubin or AFP lab results are? Did you have an abd. ultrasound (U/S) done? Was your F3 determined by blood test or by fibroscan? So your first VL was done at 2 weeks, so then how many more blood tests/VL's will you have done  during your 12 weeks of treatment?

As a non-cirrhotic and a GT2 you will do well on epclusa. Very nice you are feeling some better already! Truly miraculous eh?

Drink LOTS of water!!! And were not kidding about that. 

Feel free to post any questions or comments you feel like.  C.

PS (aha!, I should read twice /write once - just noticed you DID say your F3 WAS by fibroscan, do you happen to know what the fibroscan kPa number was as well?)

 

 

-- Edited by Canuck on Friday 30th of March 2018 12:33:45 AM

-- Edited by Canuck on Friday 30th of March 2018 12:43:10 AM

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Hi Canuck,

Thanks for your encouraging words.

F3 determined by fibroscan not fibrotest. Don't have the kPa at present but can get from my specialist when I see him next week and will know more about additional blood tests/VL at that time.

ALT is 12 U/L
AST is 21 U/L
Bilirubin is 0.3 mg/dL
AFP tumour marker was 1.5 ng/mL

So all tests WNR. I am 2a2c by the way. I did have an abdominal ultrsound and my liver specialist says negative for cancer.