This article is more than 5 years old. Information may no longer be current.

International Liver Congress Offers Insight on the ‘Social Science’ of HCV

Issue: May 2018

ByIra M. Jacobson, MD

Add topic to email alerts

Receive an email when new articles are posted on

Please provide your email address to receive an email when new articles are posted on .

Subscribe

Added to email alerts

You've successfully added to your alerts. You will receive an email when new content is published.

Click Here to Manage Email Alerts

You've successfully added to your alerts. You will receive an email when new content is published.

Click Here to Manage Email Alerts

Back to Healio

We were unable to process your request. Please try again later. If you continue to have this issue please contact customerservice@slackinc.com.

Back to Healio

This month’s issue and the current issue of its sister publication HCV Next, highlights data on therapeutic regimens for hepatitis C presented at the International Liver Congress. The meeting highlighted how high is the summit to which we’ve climbed after years of a massive international effort to cure HCV, and how much the focus is shifting. We heard little about new HCV regimens and instead focused on real-world data sets on existing regimens and, equally important, the theme that HCV treatment has become as much of as social science as a medical one as we strive toward elimination. We saw an appropriate emphasis being placed on screening, linkage and access to care, including underprivileged and high-risk populations, on a national and global scale.

Data emerged from real-world studies where, despite the favorable data from one study of 8 weeks of therapy in genotype 3, these did not cry out for a shortening of our regimens our currently recommended for 12 weeks for this genotype.

It also remains apparent that genotype 3-infected patients with certain baseline resistant variants or resistance associated substitutions (RASs) appear to benefit from the addition of ribavirin, particularly treatment experienced cirrhotics, and we should remember that the AASLD guidelines still say we should add ribavirin in the case of baseline RASs for treatment-naive cirrhotics and even for treatment experienced non-cirrhotics.

Global View

I was impressed at the meeting with the national and global efforts to focus on needy populations such as IV drug users who clearly benefit from collaborations between HCV treaters and addiction medicine specialists, with very high SVR rates being attained in the presented models.

Such collaborations can ensure that recent or active drug users receive the opioid substitution therapy they need and that strategies geared toward harm reduction can continue to be implemented after the patient has finished with treatment to eliminate or minimize the risk of reinfection.

We also saw studies from places as diverse as the Punjab, Iceland and Georgia as well as several European countries which have implemented an EU funded project called HepCare Europe focusing on vulnerable patients, including the use of trained peers who can connect with underserved populations in effective ways.

Refinement, Benefits

One of the remaining important refinements of therapy that we need is strategies for how to treat patients who fail DAA regimens. We saw an interim report from TARGET, as well as some nice data on patients who were retreated with the same regimen with Sovaldi (sofosbuvir, Gilead Sciences). Though these retreatments may be expensive, payers should recognize that some sort of salvage therapy must be offered to the few patients who fail our current pangenotypic regimens. The overarching mantra should always be “no patient left behind.”

We also saw an abundance of follow-up data continuing to demonstrate the benefits that accrue to patients who had an SVR following DAA therapy. It is no surprise that the theme emerging from these studies mirrors what we saw in interferon therapy, which is that both liver-related and systemic benefits accrue. It was even suggested that DAA therapy is associated with a lower risk of subsequent non-hepatic cancers, a provocative notion that certainly deserves further attention.

As I read it, there continues to remain a preponderance of evidence suggesting that attainment of SVR in patients with a history of HCC treated with ablation or locoregional therapy do not have an increased risk of recurrence after virologic cure, but there do remain proponents of the countervailing view.

On the other hand, the notion put forward a couple years ago that de novo HCC may also be sparked by virologic cure seems to be firmly disproven. There is consensus, however, reflected in the society guidance documents, that patients with advanced fibrosis or cirrhosis who achieve SVR on DAA therapy need ongoing HCC surveillance with no well-defined stopping point at this time.

Hepatitis B

The EASL meeting represented an inflection point for me in terms of the greater amount of time I devoted to attending sessions on fatty liver disease and hepatitis B. Both of these fields are rapidly coming to dominate the investigative clinical trials arena and represent fascinating challenges and areas of major unmet need in the years to come.

The efforts in HBV center on the search for “functional cure,” interpreted by most observers as tantamount to clearance of HBsAg, since we have long since attained the capacity to effect long-term viral suppression. Unfortunately, we succeed in effecting HBsAg clearance in only a minority of patients, and long-term suppressive therapy is usually required.

We saw studies in several classes including capsid assembly modulators, or CAMs, of which there are two major classes. We are seeing data from agents in this class such as JNJ-56136379 (Janssen), and ABI-H0731 (Assembly Biosciences) and RO7049389 (Hoffman-La Roche) that show promising levels of viral suppression.

There were also promising data from the final results of a study on an entry inhibitor – Myrcludex (MYR Pharma) – a hepatitis B entry inhibitor being studied for both chronic hepatitis B and hepatitis D. The final results from Heiner Wedemeyer, MD, et al, of 6 months of treatment with this agent showed ongoing reduction of HDV RNA in the blood of infected patients at the 6-month time point and represents a new promise for these patients who have only interferon to rely upon with suboptimal results and considerable tolerability issues. It leaves us wondering if a more prolonged period of therapy will be able to suppress the virus completely, with the authors suggesting 2 to 3 years based on modeling.

NAFLD, NASH

The world of fatty liver disease continues to be characterized by an almost bewildering assortment of therapeutic targeting efforts and a plethora of clinical trials, a few of which are in phase 3 but most of which are phase 2 or earlier. Indeed, there was a host of studies on preclinical models in fatty liver.

What we are witnessing are pharmacologic attempts to target any one or more of the variety of pathways that cumulatively play a role in the pathogenesis of this complex disease. We are seeing a variety of approaches that support the further development of various drugs that can either improve or resolve the histologic features of steatohepatitis and/or have antifibrotic effects. Indeed, there is lively debate on whether steatohepatitis resolution or fibrosis regression should be our major endpoint; perhaps we should have the flexibility to allow for either or both, depending upon the putative mechanism of action of the agent being studied. We are now seeing the advent of combination therapy, which is how many predict the field is likely to evolve, given the several different metabolic, inflammatory or antifibrotic pathways of which we should be able to take advantage. There was a wealth of data about other agents from diverse classes too numerous to recount in the space available for this commentary. Stay tuned for a rich landscape of new developments in the next several years in the NAFLD field.

Editor’s Note: This Editorial has been adapted from its original form that can be seen in HCV Next.

• References:
• Asselah T. GS-006. Presented at: International Liver Congress; Apr. 11-15, 2018; Paris, France.
• Berg T, et al. GS-007. Presented at: International Liver Congress; Apr. 11-15, 2018; Paris, France.
• Chokkalingam A. PS-155. Presented at: International Liver Congress; Apr. 11-15, 2018; Paris, France.
• D’Ambrosio R, et al. GS-013. Presented at: International Liver Congress; Apr. 11-15, 2018; Paris, France.
• Harrison S, et al. FRI-487. Presented at: International Liver Congress; Apr. 11-15, 2018; Paris, France.
• Lok AS, et al. LBO-008. Presented at: International Liver Congress; Apr. 11-15, 2018; Paris, France.
• Mena de Cea A, et al. Abstract 418. Presented at: The International Liver Congress; April 11-15, 2018; Paris.
• Wedemeyer H, et al. GS-005. Presented at: International Liver Congress; Apr. 11-15, 2018; Paris, France.
• Wyles DS, et al. PS-040. Presented at: International Liver Congress; Apr. 11-15, 2018; Paris, France.