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HBV Therapy & Approaches to Cure Jordan J. Feld MD MPH Toronto Centre for Liver Disease Sandra Rotman Centre for Global Health University of Toronto

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Page 1: HBV Therapy & Approaches to Cure - Virology Educationregist2.virology-education.com/2017/18AntiviralPK/12...Cirrhosis Goals of Therapy • Cure the infection – True cure = all traces

HBV Therapy & Approaches

to Cure

Jordan J. Feld MD MPH

Toronto Centre for Liver Disease

Sandra Rotman Centre for Global Health

University of Toronto

Page 2: HBV Therapy & Approaches to Cure - Virology Educationregist2.virology-education.com/2017/18AntiviralPK/12...Cirrhosis Goals of Therapy • Cure the infection – True cure = all traces

Disclosures

• Research: Abbvie, Gilead, Janssen, Merck, Wako

• Consulting: Abbvie, Contravir, Gilead, Janssen,

Merck

Page 3: HBV Therapy & Approaches to Cure - Virology Educationregist2.virology-education.com/2017/18AntiviralPK/12...Cirrhosis Goals of Therapy • Cure the infection – True cure = all traces

Outline

• Goals of therapy

• Why do we need new treatment?

• Approaches to new treatment

– Virological targets

– Immunological targets

Page 4: HBV Therapy & Approaches to Cure - Virology Educationregist2.virology-education.com/2017/18AntiviralPK/12...Cirrhosis Goals of Therapy • Cure the infection – True cure = all traces

What are the goals of therapy?

Learning from natural history

0

100

80

60

40

20

0 5 10 15 20 25

Su

rviv

al p

rob

ab

ilit

y (

%) Inactive CHB

HBeAg-/HBV DNA+

or HBeAg reversion

HBeAg+ persistence

Time (years)

• Very inactive disease and ideally HBsAg loss associated with excellent long-term and cancer-free survival

• A good goal for therapy

Fattocvich Gut 2008, Yang NEJM 2002

sAg + /eAg +

sAg + /eAg -

sAg - /eAg -Cu

mu

lati

ve H

CC

In

cid

ence

(%

)

Survival HCC

Page 5: HBV Therapy & Approaches to Cure - Virology Educationregist2.virology-education.com/2017/18AntiviralPK/12...Cirrhosis Goals of Therapy • Cure the infection – True cure = all traces

Jaundice

Fluid RetentionAscites

Esophageal Varices

HepaticEncephalopathy

Liver Cancer

What we’re trying to prevent

Cirrhosis

Page 6: HBV Therapy & Approaches to Cure - Virology Educationregist2.virology-education.com/2017/18AntiviralPK/12...Cirrhosis Goals of Therapy • Cure the infection – True cure = all traces

Goals of Therapy• Cure the infection

– True cure = all traces of HBV gone from the liver (ie. like HCV)

– This is VERY difficult (if not impossible) cccDNA

• Functional cure

– Use the markers of excellent natural history…

1. HBsAg loss (ideally with anti-HBs)

2. Possibly…sustained off treatment inactive disease without

HBsAg loss (HBeAg –ve, DNA undetectable, normal ALT,

normal histology)

Cure not so simple…reasons lie in the virology

Page 7: HBV Therapy & Approaches to Cure - Virology Educationregist2.virology-education.com/2017/18AntiviralPK/12...Cirrhosis Goals of Therapy • Cure the infection – True cure = all traces

Potent HBV DNA suppression

TDF vs TDF/FTC in LAM-R HBV

Long-term therapy with potent nucs leads to suppression in almost all patients (even after resistance)

Chang Hepatology 2010, Fung J Hep 2017

Long-term ETV in eAg +ve HBV

% s

up

pre

ssed

HB

V D

NA

% s

up

pre

sse

d H

BV

DN

A

Page 8: HBV Therapy & Approaches to Cure - Virology Educationregist2.virology-education.com/2017/18AntiviralPK/12...Cirrhosis Goals of Therapy • Cure the infection – True cure = all traces

Suppressive therapy is not a cure

1378 Korean patients on LAM/ETV vs 1014 inactive CHB

Cho Gut 2014

Complete respondersInactive

CHB

p<0.001 p<0.015

Non-cirrhotic Cirrhotic

Cu

mu

lati

ve in

cid

en

ce o

f H

CC

Cu

mu

lati

ve in

cid

en

ce o

f H

CC

Complete responders

Inactive CHB

• Treatment reduces but does not eliminate risk of HCC• Spontaneous (immune) control better than suppressing

HBV DNA with treatment

Page 9: HBV Therapy & Approaches to Cure - Virology Educationregist2.virology-education.com/2017/18AntiviralPK/12...Cirrhosis Goals of Therapy • Cure the infection – True cure = all traces

Why don’t nucs lead to cure?

O-

5’Cap (A)n 3’

Translocation

dAdAdG

new (-) strand DNA synthesis

pgRNA

DNA Synthesis

Encapsidationof pg RNA

Golgi complex

Release

CCC DNA

DNArepair

HBV RNATranscripts

PregenomicRNA

Attachment andPenetration

S Ag

e Ag

HBV Virion

EnvelopeProteins

S, M, L

e Ag

PolymeraseProteinCore

Protein

uncoating

transport to cellnucleus

• Persistence with potent nuc treatment means there is a leak

Page 10: HBV Therapy & Approaches to Cure - Virology Educationregist2.virology-education.com/2017/18AntiviralPK/12...Cirrhosis Goals of Therapy • Cure the infection – True cure = all traces

The leakIntrahepatic HBV DNA during long-term TDF therapy in HIV/HBV co-infection

• Very slow decline and persistence of cccDNA long-term +

detectable intrahepatic non-cccDNA support ongoing

replication despite ‘complete suppression’’ ie the leak!

• cccDNA replenishment - re-circulation + de novo infection

• Implication: Cure requires VERY long-term therapy

cccDNA Total intrahepatic

HBV DNA

Boyd J Hep 2016

Page 11: HBV Therapy & Approaches to Cure - Virology Educationregist2.virology-education.com/2017/18AntiviralPK/12...Cirrhosis Goals of Therapy • Cure the infection – True cure = all traces

Why do we need new treatment?

Nucleoside Analogues

• Effective suppression of HBV DNA

• Minimal or no effect on immune control

• High risk of relapse with stopping before HBsAg loss

• Low rates of HBsAg loss long-term therapy– Safety

– Costs

– Monitoring

– Access in most of the world limited

Interferon

• Higher rate of HBsAg loss

but still low

• Finite therapy but poorly

tolerated

• Patients and providers

don’t want to use it!

Page 12: HBV Therapy & Approaches to Cure - Virology Educationregist2.virology-education.com/2017/18AntiviralPK/12...Cirrhosis Goals of Therapy • Cure the infection – True cure = all traces

Considerations for cureHCV

• Ineffective, poorly

tolerated therapy

• Multiple lifecycle targets

• No long-lasting nuclear

reservoir or integration

• Limited involvement of

immune system

HBV

• Well tolerated, very

effective therapy – high

bar

• Single viral enzyme

• cccDNA very persistent

and hard to reach

• Immune control important

…flaresBottom line…it won’t be as easy to cure HBV as it

was to cure HCV!

Page 13: HBV Therapy & Approaches to Cure - Virology Educationregist2.virology-education.com/2017/18AntiviralPK/12...Cirrhosis Goals of Therapy • Cure the infection – True cure = all traces

Approaches to therapyViral targets - DAA

• Viral entry

• cccDNA

formation/transcription/de

gradation

• RNA intermediates

• Encapsidation

• DNA replication

• Assembly

• Release

Immunomodulators

• Innate immune response

– IFN

– TLR agonists

– RIG-I agonists

• Adaptive immune

response

– Anti-antagonists

(checkpoint inhibitors)

– Vaccination

Page 14: HBV Therapy & Approaches to Cure - Virology Educationregist2.virology-education.com/2017/18AntiviralPK/12...Cirrhosis Goals of Therapy • Cure the infection – True cure = all traces

Potential targets in the lifecycle

O-

5’Cap (A)n 3’

Translocation

dAdAdG

new (-) strand DNA synthesis

pgRNA

DNA Synthesis

Encapsidationof pg RNA

Golgi complex

Release

CCC DNA

DNArepair

HBV RNATranscripts

PregenomicRNA

Attachment andPenetration

S Ag

e Ag

HBV Virion

EnvelopeProteins

S, M, L

e Ag

PolymeraseProteinCore

Protein

uncoating

transport to cellnucleus

Block Entry

Target cccDNA- Destruction- Inactivation

Target HBV RNA

Target packaging

Target DNA synthesis

Target Assembly/Export

Stimulation of innate and/or

adaptive immunity

Page 15: HBV Therapy & Approaches to Cure - Virology Educationregist2.virology-education.com/2017/18AntiviralPK/12...Cirrhosis Goals of Therapy • Cure the infection – True cure = all traces

Potential targets in the lifecycle

O-

5’Cap (A)n 3’

Translocation

dAdAdG

new (-) strand DNA synthesis

pgRNA

DNA Synthesis

Encapsidationof pg RNA

Golgi complex

Release

CCC DNA

DNArepair

HBV RNATranscripts

PregenomicRNA

Attachment andPenetration

S Ag

e Ag

HBV Virion

EnvelopeProteins

S, M, L

e Ag

PolymeraseProteinCore

Protein

uncoating

transport to cellnucleus

Block Entry

Target cccDNA- Destruction- Inactivation

Target HBV RNA

Target packaging

Target DNA synthesis

Target Assembly/Export

Stimulation of innate and/or

adaptive immunity

Page 16: HBV Therapy & Approaches to Cure - Virology Educationregist2.virology-education.com/2017/18AntiviralPK/12...Cirrhosis Goals of Therapy • Cure the infection – True cure = all traces

HBV Entry: Discovery of HBV

receptor to the first entry blocker

Primary Human Hepatocytes • Pre-S1 of HBsAg binds to sodium taurocholate co-transporting peptide – NTCP

• Predominantly expressed in liver

• Myristylated lipopeptidecontaining aa 2-48 of HBV large surface antigen Myrcludex B

• Blocks HBV and HDV entry

Yan eLife Science 2012 Gripon PNAS 2002, Urban J Virol 2005, Glebe Gastro 2005, Schutze Gastro 2007

Page 17: HBV Therapy & Approaches to Cure - Virology Educationregist2.virology-education.com/2017/18AntiviralPK/12...Cirrhosis Goals of Therapy • Cure the infection – True cure = all traces

Clinical data for Myrcludex B

Bogolomov J Hep 2016, Urban AASLD 2016

• Modest HBV DNA decline (0.8 log), no effect on HBsAg, safety concerns but ALT normalization (55%) and greater effect in HDV

• Not likely enough on its own but maybe an adjunct therapy…

Myrcludex 10 mg OD x 24 weeks in HBV and HDV

HDV HBV

Page 18: HBV Therapy & Approaches to Cure - Virology Educationregist2.virology-education.com/2017/18AntiviralPK/12...Cirrhosis Goals of Therapy • Cure the infection – True cure = all traces

If sAg loss is the goal…we

should be sure we are always

talking about the same thing…

Page 19: HBV Therapy & Approaches to Cure - Virology Educationregist2.virology-education.com/2017/18AntiviralPK/12...Cirrhosis Goals of Therapy • Cure the infection – True cure = all traces

Caveats with sAg loss

CCC DNA

HBV RNATranscripts

PregenomicRNA

EnvelopeProteins (sAg)

S, M, L

e Ag

PolymeraseProtein

Core Protein

1. Loss of sAg = loss of sAg transcription silent/absent cccDNA = our goal

Page 20: HBV Therapy & Approaches to Cure - Virology Educationregist2.virology-education.com/2017/18AntiviralPK/12...Cirrhosis Goals of Therapy • Cure the infection – True cure = all traces

Caveats with sAg loss

HBV RNATranscripts

PregenomicRNA

EnvelopeProteins (sAg)

S, M, L

e Ag

PolymeraseProtein

Core Protein

1. Loss of sAg = loss of sAg transcription silent/absent cccDNA = our goal

Elimination

Page 21: HBV Therapy & Approaches to Cure - Virology Educationregist2.virology-education.com/2017/18AntiviralPK/12...Cirrhosis Goals of Therapy • Cure the infection – True cure = all traces

Caveats with sAg loss

CCC DNA

HBV RNATranscripts

PregenomicRNA

EnvelopeProteins (sAg)

S, M, L

e Ag

PolymeraseProtein

Core Protein

x x

1. Loss of sAg = loss of sAg transcription silent/absent cccDNA = our goal Transcriptional

Silencing

Page 22: HBV Therapy & Approaches to Cure - Virology Educationregist2.virology-education.com/2017/18AntiviralPK/12...Cirrhosis Goals of Therapy • Cure the infection – True cure = all traces

Caveats with sAg loss

CCC DNA

HBV RNATranscripts

PregenomicRNA

EnvelopeProteins (sAg)

S, M, L

e Ag

PolymeraseProtein

Core Protein

xx

1. Loss of sAg = loss of sAg transcription silent/absent cccDNA = our goal

2. Loss of sAg = loss of sAg translation siRNA…unclear what this means…may still be very helpful but unknown if the same as 1 (our usual sAg loss)

TranslationalSilencing

(siRNA)

Page 23: HBV Therapy & Approaches to Cure - Virology Educationregist2.virology-education.com/2017/18AntiviralPK/12...Cirrhosis Goals of Therapy • Cure the infection – True cure = all traces

Caveats with sAg loss

CCC DNA

EnvelopeProteins (sAg)

S, M, L

HBV RNATranscripts

PregenomicRNA

e Ag

PolymeraseProtein

Core Protein

sAgx x

1. Loss of sAg = loss of sAg transcription silent/absent cccDNA = our goal

2. Loss of sAg = loss of sAg translation siRNA…unclear what this means…may still be very helpful but unknown if the same as 1 (our usual sAg loss)

3. sAg may still be made from integrated HBV DNA –makes 1 and 2 hard to confirm!

Integration

Page 24: HBV Therapy & Approaches to Cure - Virology Educationregist2.virology-education.com/2017/18AntiviralPK/12...Cirrhosis Goals of Therapy • Cure the infection – True cure = all traces

Potential targets in the lifecycle

O-

5’Cap (A)n 3’

Translocation

dAdAdG

new (-) strand DNA synthesis

pgRNA

DNA Synthesis

Encapsidationof pg RNA

Golgi complex

Release

CCC DNA

DNArepair

HBV RNATranscripts

PregenomicRNA

Attachment andPenetration

S Ag

e Ag

HBV Virion

EnvelopeProteins

S, M, L

e Ag

PolymeraseProteinCore

Protein

uncoating

transport to cellnucleus

Block Entry

Target cccDNA- Destruction- Inactivation

Target HBV RNA

Target packaging

Target DNA synthesis

Target Assembly/Export

Stimulation of innate and/or

adaptive immunity

Page 25: HBV Therapy & Approaches to Cure - Virology Educationregist2.virology-education.com/2017/18AntiviralPK/12...Cirrhosis Goals of Therapy • Cure the infection – True cure = all traces

cccDNA – Approaches

1. Formation- RC to cccDNA- HBV DNA recycling

3. Transcription- pgRNA - replication- mRNA – Ag production

2. Degradation- Destroy existing pool

Boucle Clin Liv Dis 2016

Page 26: HBV Therapy & Approaches to Cure - Virology Educationregist2.virology-education.com/2017/18AntiviralPK/12...Cirrhosis Goals of Therapy • Cure the infection – True cure = all traces

cccDNA - approaches

1. Formation– DSS – disubstituted sulfonamides – rc to cccDNA

– Early days but interesting…

2. Degradation– CRISPR/Cas9

– Directly cleave cccDNA• Mutation or degradation

• Delivery, off-target effects

3. Transcription– Prevent RNA transcription

• pgRNA no replication

• mRNA no proteins (sAg, xAg)

– Histone acetyltransferase inhibitor• Specificity?

Cai Antimicrob. Agents Chemother 2012Lin Int J Mol Sci 2015, Tropberger PNAS 2015

Page 27: HBV Therapy & Approaches to Cure - Virology Educationregist2.virology-education.com/2017/18AntiviralPK/12...Cirrhosis Goals of Therapy • Cure the infection – True cure = all traces

Potential targets in the lifecycle

O-

5’Cap (A)n 3’

Translocation

dAdAdG

new (-) strand DNA synthesis

pgRNA

DNA Synthesis

Encapsidationof pg RNA

Golgi complex

Release

CCC DNA

DNArepair

HBV RNATranscripts

PregenomicRNA

Attachment andPenetration

S Ag

e Ag

HBV Virion

EnvelopeProteins

S, M, L

e Ag

PolymeraseProteinCore

Protein

uncoating

transport to cellnucleus

Block Entry

Target cccDNA- Destruction- Inactivation

Target HBV RNA

Target packaging

Target DNA synthesis

Target Assembly/Export

Stimulation of innate and/or

adaptive immunity

Page 28: HBV Therapy & Approaches to Cure - Virology Educationregist2.virology-education.com/2017/18AntiviralPK/12...Cirrhosis Goals of Therapy • Cure the infection – True cure = all traces

Target RNA - siRNA

• Overlapping reading frames = conserved regions• siRNA targeting can eliminate all HBV gene products

- sAg, pol, core immune function - pgRNA (replication)

Woodell Mol Ther 2013, Arrowhead

Page 29: HBV Therapy & Approaches to Cure - Virology Educationregist2.virology-education.com/2017/18AntiviralPK/12...Cirrhosis Goals of Therapy • Cure the infection – True cure = all traces

Clinical Data with RNAi

sAg

crAg

eAg

HBeAg -ve

HBeAg +ve

Placebo

HBV Protein reduction with ARC520 sAg decline eAg + vs -

• Effective knockdown of all HBV proteins• Much more effective in HBeAg + than HBeAg -

• e+ - initial 1.6 log to 2.9 log cccDNA?• e- - initial 0.5 log to 1.2 log integrated?

• Well tolerated but safety concerns…new delivery system? FDA HOLD• ALT rise off RNAi…?restored immune response?

Yuen AASLD 2015, Yuen EASL 2017

Page 30: HBV Therapy & Approaches to Cure - Virology Educationregist2.virology-education.com/2017/18AntiviralPK/12...Cirrhosis Goals of Therapy • Cure the infection – True cure = all traces

A different RNAi, different results

0.50

0.00

–0.50

–1.00

–1.501* 29* 57* 85

Day

HB

sAg

(lo

g 10

IU/m

L)

HBeAg-negative ARB-1467 0.2 mg/kgHBeAg-negative ARB-1467 0.4 mg/kgHBeAg-postive ARB-1467 0.4 mg/kgPlacebo

Efficacy

*Dosing

e+e-

e-

Different RNAi combination effective with single & multi-doseNo difference between eAg +ve and –ve (but slightly lower sAg decline)

Streinu-Cercel A, et al. EASL 2017, Amsterdam. #SAT-155

ARB-1467 0.2 or 0.4 mg/kg in NA-suppressed patients monthly IV infusion

Page 31: HBV Therapy & Approaches to Cure - Virology Educationregist2.virology-education.com/2017/18AntiviralPK/12...Cirrhosis Goals of Therapy • Cure the infection – True cure = all traces

Bottom line on siRNA for HBV

• Attractive approach

– Inhibits viral protein reduction immune restoration

(need to prove this)

– Inhibits viral replication directly (pgRNA)

– Pan-genotypic, relatively high barrier to resistance

• Major challenges

– Delivery

– Effect in eAg –ve ?integrated sAg

– Safety

Page 32: HBV Therapy & Approaches to Cure - Virology Educationregist2.virology-education.com/2017/18AntiviralPK/12...Cirrhosis Goals of Therapy • Cure the infection – True cure = all traces

Potential targets in the lifecycle

O-

5’Cap (A)n 3’

Translocation

dAdAdG

new (-) strand DNA synthesis

pgRNA

DNA Synthesis

Encapsidationof pg RNA

Golgi complex

Release

CCC DNA

DNArepair

HBV RNATranscripts

PregenomicRNA

Attachment andPenetration

S Ag

e Ag

HBV Virion

EnvelopeProteins

S, M, L

e Ag

PolymeraseProteinCore

Protein

uncoating

transport to cellnucleus

Block Entry

Target cccDNA- Destruction- Inactivation

Target HBV RNA

Target packaging

Target DNA synthesis

Target Assembly/Export

Stimulation of innate and/or

adaptive immunity

Page 33: HBV Therapy & Approaches to Cure - Virology Educationregist2.virology-education.com/2017/18AntiviralPK/12...Cirrhosis Goals of Therapy • Cure the infection – True cure = all traces

Core protein – Attractive target

• Highly conserved

• Lots of functions– Transport to the nucleus

– Uncoating of HBV DNA

– Packaging

– Capsid assembly

– Modulate reverse transcription

– Interacts with sAg

– May also modulate cccDNA and export viral RNA

• All allosteric regulation…1 molecule that affects any function will affect them all!

Page 34: HBV Therapy & Approaches to Cure - Virology Educationregist2.virology-education.com/2017/18AntiviralPK/12...Cirrhosis Goals of Therapy • Cure the infection – True cure = all traces

Capsid Assembly Modulators (CpAMs)

Feld Antivira Res 2007Katen Chem Bio 2010

Phenylpropanamides (AT130) inhibit packaging – empty capsids

• Not capsid inhibitor – actually accelerate capsid formation• But empty capsids – no RNA or polymerase inside!• Better agents in the pipeline…

Page 35: HBV Therapy & Approaches to Cure - Virology Educationregist2.virology-education.com/2017/18AntiviralPK/12...Cirrhosis Goals of Therapy • Cure the infection – True cure = all traces

Potential targets in the lifecycle

O-

5’Cap (A)n 3’

Translocation

dAdAdG

new (-) strand DNA synthesis

pgRNA

DNA Synthesis

Encapsidationof pg RNA

Golgi complex

Release

CCC DNA

DNArepair

HBV RNATranscripts

PregenomicRNA

Attachment andPenetration

S Ag

e Ag

HBV Virion

EnvelopeProteins

S, M, L

e Ag

PolymeraseProteinCore

Protein

uncoating

transport to cellnucleus

Block Entry

Target cccDNA- Destruction- Inactivation

Target HBV RNA

Target packaging

Target DNA synthesis

Target Assembly/Export

Stimulation of innate and/or

adaptive immunity

Page 36: HBV Therapy & Approaches to Cure - Virology Educationregist2.virology-education.com/2017/18AntiviralPK/12...Cirrhosis Goals of Therapy • Cure the infection – True cure = all traces

New nucs…TAF Tenofovir alofenamide (TAF)

• Very similar kinetics in the blood

• Unclear what is happening in the liver…

• Faster ALT normalization is interesting…

• Unlikely to be ‘the cure’ but may be combined with other agents

improved safety and possibly more potent

• Adding RNaseH activity may improve potency

• Multiple others (TDF variants) in late-stage development…

HBeAg -ve HBeAg +ve

Buti EASL 2016, Chan EASL 2016

Page 37: HBV Therapy & Approaches to Cure - Virology Educationregist2.virology-education.com/2017/18AntiviralPK/12...Cirrhosis Goals of Therapy • Cure the infection – True cure = all traces

Potential targets in the lifecycle

O-

5’Cap (A)n 3’

Translocation

dAdAdG

new (-) strand DNA synthesis

pgRNA

DNA Synthesis

Encapsidationof pg RNA

Golgi complex

Release

CCC DNA

DNArepair

HBV RNATranscripts

PregenomicRNA

Attachment andPenetration

S Ag

e Ag

HBV Virion

EnvelopeProteins

S, M, L

e Ag

PolymeraseProteinCore

Protein

uncoating

transport to cellnucleus

Block Entry

Target cccDNA- Destruction- Inactivation

Target HBV RNA

Target packaging

Target DNA synthesis

Target Assembly/Export

Stimulation of innate and/or

adaptive immunity

Page 38: HBV Therapy & Approaches to Cure - Virology Educationregist2.virology-education.com/2017/18AntiviralPK/12...Cirrhosis Goals of Therapy • Cure the infection – True cure = all traces

Antigen & Virion SecretionGlucosidase Inhibitors• HBV proteins heavily glycosylated

• Mimic glycosylated residues on viral proteins leading to inhibition of α-glucosidase

• Inhibit secretion of HBsAg and HBV virions in vitro and in woodchucks

• Recognized a long time ago…no progress

Newer Approaches• REP 9’AC – blocks secretion of empty HBsAg (not virus)

– Promising HBsAg loss data…but mechanism obscure

– Too good to be true?

• Triazolopyrimidines – also block HBsAg secretion

Block 1998 Nat Med, Mahtab Hepatol 2012, Yu JMC 2011

Page 39: HBV Therapy & Approaches to Cure - Virology Educationregist2.virology-education.com/2017/18AntiviralPK/12...Cirrhosis Goals of Therapy • Cure the infection – True cure = all traces

Potential targets in the lifecycle

O-

5’Cap (A)n 3’

Translocation

dAdAdG

new (-) strand DNA synthesis

pgRNA

DNA Synthesis

Encapsidationof pg RNA

Golgi complex

Release

CCC DNA

DNArepair

HBV RNATranscripts

PregenomicRNA

Attachment andPenetration

S Ag

e Ag

HBV Virion

EnvelopeProteins

S, M, L

e Ag

PolymeraseProteinCore

Protein

uncoating

transport to cellnucleus

Block Entry

Target cccDNA- Destruction- Inactivation

Target HBV RNA

Target packaging

Target DNA synthesis

Target Assembly/Export

Stimulation of innate and/or

adaptive immunity

Page 40: HBV Therapy & Approaches to Cure - Virology Educationregist2.virology-education.com/2017/18AntiviralPK/12...Cirrhosis Goals of Therapy • Cure the infection – True cure = all traces

Immune response to HBV

Hepatocyte

NK(T)

DC

IFN

Viral

replication

activation

BAnti-HBe, HBc, HBs

Hepatocyte

lysis

Viral

replication

neutralization

Innate immunity Adaptive immunity

CD4+

CD8+

Rehermann Nat Rev Immun 2005, Woltman Gut 2010

Page 41: HBV Therapy & Approaches to Cure - Virology Educationregist2.virology-education.com/2017/18AntiviralPK/12...Cirrhosis Goals of Therapy • Cure the infection – True cure = all traces

ImmunotherapiesInnate

• Cytokine therapy

– IFN

• TLR agonists

– TLR7

• RIG-I agonists

Adaptive

• Therapeutic vaccine

• Checkpoint inhibitors

– PD-1

– PD-L1

Immune restoration through inhibition of viral antigens

Page 42: HBV Therapy & Approaches to Cure - Virology Educationregist2.virology-education.com/2017/18AntiviralPK/12...Cirrhosis Goals of Therapy • Cure the infection – True cure = all traces

Immune restoration with NAs

HC HBV0

20

40

60

80

100 **

IFN p

ro

du

cin

g c

ell

s (

%)

t=0 t=60

20

40

60

80

100 *

CD

69 (

%)

t=0 t=60

25

50

75 *

IFN p

rod

ucin

g c

ell

s (

%)

NK cell

CD69+

CD69+

IFN+IL-12

IL-18

Viral suppression with ETV restores NK cell response activation

and cytokine production

ETV Tx ETV Tx

Tjwa et al. J Hepatol 2011

Page 43: HBV Therapy & Approaches to Cure - Virology Educationregist2.virology-education.com/2017/18AntiviralPK/12...Cirrhosis Goals of Therapy • Cure the infection – True cure = all traces

Would this justify adding a nuc

to IFN?ETV-suppressed patients randomized to ETV continuation vs adding PegIFN

-0 .4

-0 .2

0 .0

2 4 3 6 4 8

W e e k s

HB

sA

g d

ec

lin

e (

log

IU

/mL

)

-2 .0

-1 .5

-1 .0

-0 .5

0 .0

2 4 3 6 4 8

W e e k s

HB

V D

NA

de

cli

ne

(lo

g I

U/m

L)

ETV +PEG-IFN

ETV

ETV +PEG-IFN

ETV

P<0.001P<0.001

HBV DNA HBsAg

Improved DNA & HBsAg decline BUT no IFN monotherapy arm and only 18% off-treatment response…intriguing but not the answer

Sonneveld J Hep 2015

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TLR7 Agonist

Led to IFN production, few systemic side effects

TLR7- Pathogen recognition receptor- Triggers IFN production – antiviral

response- GS-9620 – oral, nanomolar potency- Active in vivo – chimps, humans

Lanford Gastro 2013

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TLR7 in chimps

• Mean max HBV DNA decline 2.2 logs, HBeAg decline

• ALT flares occurred; but limited IFN systemic effects

• Ongoing phase 2 trial in patients on TDF

Lanford Gastro 2013

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ImmunotherapiesInnate

• Cytokine therapy

– IFN

• TLR agonists

– TLR7

• RIG-I agonists

Adaptive

• Therapeutic vaccine

• Checkpoint inhibitors

– PD-1

– PD-L1

Early days…so far limited effects seen

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ImmunotherapiesInnate

• Cytokine therapy

– IFN

• TLR agonists

– TLR7

• RIG-I agonists

Adaptive

• Therapeutic vaccine

• Checkpoint inhibitors

– PD-1

– PD-L1

Early days…so far limited effects seen

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Therapeutic vaccines

Tarmogen- Modified yeast expressing HBV protein- Scalable- Ongoing studies…

Other approaches:- Adeno or AAV vector with HBV proteins- Improved adjuvant- Add TLR agonist to vaccine…- Lots of ideas – limited data

- Results generally disappointing to date

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Checkpoint inhibitors

Bertoletti HBV Endpoints 2016

Excessive co-stimulatory signals T cell exhaustion/deletion

• Checkpoint inhibitors – taking off the brake…• leads to immune activation ?control?

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Promising target in oncology

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PD1 relevant in HBV

• PD1 most relevant checkpoint inhibitor for HBV• Expressed on HBV-specific T cells• PDL1 (ligand for PD1) on liver cells during hepatitis

Bengsh J Hep 2014

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PD1 Blockade

Baseline Week 4 Week 16Week 12

Nivolumab 0.3 mg/kgSentinel B, n=2

Sentinel A, n=2 Nivolumab 0.1 mg/kg

Cohort A, n=10 Nivolumab 0.3 mg/kg

Cohort B, n=10 +GS-4774 40 YU

Nivolumab 0.3 mg/kg

NA-suppressed e-neg patients treated with nivolumab +/- GS-4774 (Tarmogen vaccine)

Gane E, et al. EASL 2017

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Efficacy

-5

-4

-3

-2

-1

-0 .8

-0 .6

-0 .4

-0 .2

0 .0

0 .2

-5

-4

-3

-2

-1

-0 .8

-0 .6

-0 .4

-0 .2

0 .0

0 .2

Nivolumab0.1 mg/kg

Nivolumab0.3 mg/kg

Nivolumab0.3 mg/kg+ GS-4774

Week 12 Week 24

HB

sAg

Ch

ange

fro

m B

L, L

og 1

0 IU

/mL

Nivolumab0.1 mg/kg

Nivolumab0.3 mg/kg

Nivolumab0.3 mg/kg+ GS-4774

• High receptor occupancy despite relatively low dose• Very modest decline in HBsAg overall…but 1 patient…

Gane E, et al. EASL 2017

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Learning from 1 patient

1

1 0

1 0 0

1 0 0 0

1 0 0 0 0

0

1 0 0

2 0 0

3 0 0

1 4 8 12 16 20 242 3B L

HB

sAg,

IU/m

L ALT, U

/L

IFN-γ Sp

ots/ 1

06

Ce

lls

Week

• Cleared HBsAg, stopped TDF 4 weeks after dosing • 8 months later – remains HBsAg-negative and anti-HBs positive• Interesting proof of concept – very low dose given (but pretty big flare…)

Gane E, et al. EASL 2017

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It’s not just choosing the right

target/compound…• Other MAJOR issues

1. Correct population

• Highest need?

• Easiest to show an effect?

• Immuntolerant/e+/e-/inactive/NA suppressed…

2. Correct endpoint

• Is sAg loss the same with an NA as with an siRNA?

• Do we need to look in the liver? Do we need new biomarkers –HBV RNA, HBV crAg others?

3. Correct combinations

• Lots of possibilities – a huge matrix!!

4. Safety!

• A major concern…especially with immunotherapies

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Combination Approaches

Viral target

A+ Viral target

A NA + NA

Viral target

A+ Viral target

B NA + RNAi

Immune

Target A +TLR7 + Vaccine

Immune

Target B

Viral target

A+

NA + TLR7

Immune

Target A

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Attractive combinations

Nuc

HBV DNAsuppression

+Viral protein

Depletion(s, x, core)

+Immuno-therapy

RNAi

Nucleic Acid Polymers

cccDNAi

+/- cccDNAi

+/- entry inhibitor

+/- RNAi

+/- CpAM

TLR/RIG-I agonist

αPD1/PDL1

Therapeutic

vaccine

May not need all 3 ‘classes’…may need more…mix and match

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Summary for HBV cure• Many virological targets (but all with challenges…)

– Entry

– cccDNA formation/degradation/transcription

– Capsid

– Secretion

• Fewer immunological targets

– Innate – TLR, RIG-I

– Adaptive – Therapeutic vaccine, checkpoint inhibitors

• Much more challenging than HCV…both scientifically

and clinically (much higher bar, difficult to study)

• Interesting times ahead…