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The Charcot Project: Antiviral Therapies for MS Gavin Giovannoni Version 2.0

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Page 1: The charcot project - antivirals to treat MS

The Charcot Project: Antiviral Therapies for MS

Gavin Giovannoni

Version 2.0

Page 2: The charcot project - antivirals to treat MS

Disclosures

Over the last 15 years I have received personal compensation for

participating in advisory boards in relation to clinical trial design, trial steering

committees, and data and safety monitoring committees from: Abbvie,

Almirall, Atara Bio, Bayer-Schering Healthcare, Biogen, Canbex, Eisai, Elan,

Fiveprime, Genzyme, Genentech, GSK, GW Pharma, Ironwood, MSD, Merck

Serono, Novartis, Pfizer, Roche, Sanofi, Synthon BV, Teva, UCB Pharma and

Vertex Pharmaceuticals

Page 3: The charcot project - antivirals to treat MS

The case for MS being due to a virus

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To cure MS do we need to know the cause?

EBV, HERVs, etc.

Vitamin D, Obesity (? diet)

Smoking, organic solvents

Genes(HLA,....)

Page 5: The charcot project - antivirals to treat MS

The MS dogma

immune activation

innate and adaptive responses

focal inflammation

BBB breakdown

oligodendrocyte toxicity & demyelination

Acute axonal transection and loss

“autoimmune endophenotype”

axonal plasticity &

remyelination

delayed neuroaxonal loss and gliosis

Gd-enhancement

T2 & T1 lesions

brain & spinal cord atrophy

release of soluble markers

Clinical Attack

Disease Progression

Clinical Recovery

pathobiology

clinical outcomes

biomarkersPremature Ageing

Genetics Environment Chance

VIRUS(EBV, HERVs)

Page 6: The charcot project - antivirals to treat MS

.

Epidemics or clusters of MS

• No documented cases of MS

on the Faroe Islands until

after World War II

• 55 cases since 1940

• Occupied during World War

II

• Authors concluded that this

was evidence of an MS

epidemic caused by an agent

introduced by the troops

• However a number of

concerns remain

The annual incidence of MS (per 100 000

inhabitants) in the Faroe Islands since 1940

Kurtze et al 1993

0

2

4

6

8

10

12

1940 1945 1950 1955 1960 1965 1970 1975 1980 1985 1990

Page 7: The charcot project - antivirals to treat MS

Relapsing and Remitting Multiple Sclerosis: Pathology of the Newly Forming Lesion

Barnett & Prineas. Ann Neurol 2004;55:458–468

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Magnetization Transfer Changes in the Normal Appearing White Matter Precede the Appearance of Enhancing Lesions in Patients with Multiple Sclerosis

Filippi et al. Ann Neurol 1998;43:809-814

Page 9: The charcot project - antivirals to treat MS

Bermel et al. Ann Neuol 2012.

Predictors of long-term outcome in MSers treated with interferon beta-1a

Page 10: The charcot project - antivirals to treat MS

REBOUND ACTIVITY AFTER NATALIZUMAB/FINGOLIMOD WITHDRAWAL

Rigau et al. Neurology 2012;79:2214-6.Alroughani et al. BMJ Case Rep. 2014 Oct 15;2014. pii: bcr2014206314.

Page 11: The charcot project - antivirals to treat MS

REBOUND AFTER NATALIZUMAB WITHDRAWAL

Rigau et al. Neurology 2012;79:2214-6.

Page 12: The charcot project - antivirals to treat MS

Serafini et al. J Neuroimmunol. 2017 Jun 15;307:14-17.

Massive intracerebral Epstein-Barr virus reactivation in lethal

multiple sclerosis relapse after natalizumab withdrawal.

● Highly-active RRMS, severe

neurologic impairment (EDSS 7)

● Treated with natalizumab - EDSS 4.5

● Due to severe depression, stopped

Nz after 37 infusions.

● 3½ months later rapid disease

worsening

● Brain MRI showed >50 T2-lesions,

mostly Gd-enhancing

● JCV-PCR -ve in CSF

● Rapidly worsened, died d17

● PM active MS rebound

● JCV-PCR -ve in brain

Page 13: The charcot project - antivirals to treat MS

Which virus?

Page 14: The charcot project - antivirals to treat MS

Infectious agents in MS

. Ramagopalan et al 2009

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MS IM

Ramagopalan et al, 2011

Pearson r = 0.70, p=0.000025

Infectious Mononucleosis and MS

Page 16: The charcot project - antivirals to treat MS

Infectious mononucleosis

Handel et al. 2010.

Small OR19,390 MS patients and 16,007 controls, p < 10-54

Page 17: The charcot project - antivirals to treat MS

EBV Seropositivity titres

99.2% vs 90.2%

. Ascherio et al, 2000

Page 18: The charcot project - antivirals to treat MS

Odds ratio of MS in subjects seronegative for EBV

Ascherio et al, 2007

Page 19: The charcot project - antivirals to treat MS

Primary infection with the EBV and risk of MS

• Nested case-control study including from over 8 million military personnel with serum stored in the Department of Defense Serum Repository.

Levin et al. Ann Neurol 2010.

MS

Controls N = 610

N = 30510/305 (3.3%) EBV –ve

32/610 (5.2%) EBV –ve 10/28 (35.7%) EBV –ve

10/10 (100%) EBV –ve

• MS risk is extremely low among individuals not infected with EBV, but it

increases sharply in the same individuals following EBV infection.

Page 20: The charcot project - antivirals to treat MS

.Levin et al. Ann Neurol 2010.

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“Evidence” or “lack of evidence”

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The ugly fact

“The great tragedy of Science; the slaying of a beautiful hypothesis by an ugly fact.”

Thomas Henry Huxley

Page 23: The charcot project - antivirals to treat MS

Viral serologies in children with MS

Banwell et al. Lancet Neurology, Sept. 2007

?

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Coherence with prior knowledge

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Compston & Coles, Lancet 2008.

Epidemiology

worldwide distribution & migration studies

Page 26: The charcot project - antivirals to treat MS

Genetics of MS: the rate of MS in females is increasing

1Orton SM et al. Lancet Neurol 2006;5:932–936.

Page 27: The charcot project - antivirals to treat MS

Smoking is a risk factor for MS

Handel et al. PLoS One. 2011 Jan 13;6(1):e16149.

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Ramagopalan et al. Arch Neurol 2011; 68:469-72.

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Biological plausibility

Page 30: The charcot project - antivirals to treat MS

EBV & Disease Activity

Farrell et al. Neurology 2009

EBNA-1

NOT

VCA or EA

Page 31: The charcot project - antivirals to treat MS

Dysregulated EBV infection in the MS brain

Serafini et al. J Exp Med. 2007 Nov 26;204(12):2899-912.

Page 32: The charcot project - antivirals to treat MS

Follow-up studies

1. Torkildsen O, et al. Upregulation of Immunoglobulin-related Genes in Cortical Sections

from Multiple Sclerosis Patients. Brain Pathol. 2009 Oct 16. [Epub ahead of print]

2. Willis SN, et al. Epstein-Barr virus infection is not a characteristic feature of multiple

sclerosis brain. Brain. 2009 Dec;132(Pt 12):3318-28.

3. Peferoen LA, et al. Epstein Barr virus is not a characteristic feature in the central nervous

system in established multiple sclerosis. Brain. 2010 May;133(Pt 5):e137. Epub 2009 Nov

16.

4. Lassmann et al. Brain. 2011 Sep;134(Pt 9):2772-86. Tzartos et al. Neurology. 2012 Jan

3;78(1):15-23.

5. Tzartos et al. Neurology. 2012 Jan 3;78(1):15-23.

6. Serafini et al. J Neuropathol Exp Neurol. 2014 Jul;73(7):729-31.

7. Serafini et al. Brain. 2013 Jul;136 (Pt7):e233. doi: 10.1093/brain/aws315.

8. Han et al. Molecular signature of Epstein-Barr virus infection in multiple sclerosis brain

lesions. ECTRIMS Online Library. Oct 27, 2017; 200600.

Page 33: The charcot project - antivirals to treat MS

Innate immune activation is a hallmark of the active MS lesions

Tzartos et al., Neurology 2012.

Page 34: The charcot project - antivirals to treat MS

Innate immune activation is a hallmark of the active MS lesions

Tzartos et al., Neurology 2012.

Page 35: The charcot project - antivirals to treat MS

Intrathecal oligoclonal IgG bands (OCBs)

1. Rand KH, et al. (1998) Molecular approach to find target(s)

for oligoclonal bands in multiple sclerosis. J Neurol

Neurosurg Psychiatry 65:48-55.

2. Bray PF, et al. (1992) Antibodies against Epstein-Barr

nuclear antigen (EBNA) in multiple sclerosis CSF, and two

pentapeptide sequence identities between EBNA and

myelin basic protein. Neurology 42:1798-804.

3. Cepok S, et al. (2005) Identification of Epstein-Barr virus

proteins as putative targets of the immune response in

multiple sclerosis. J Clin Invest 115:1352-60.

4. Rand KH, et al. (2000) Epstein-Barr virus nuclear antigen-1

(EBNA-1) associated oligoclonal bands in patients with

multiple sclerosis. J Neurol Sci 173:32-9. C+ / S-

Page 36: The charcot project - antivirals to treat MS

Analogy

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Axthelm et al. Ann Neurol 2010

Japanese Macaque Encephalomyelitis:

A Spontaneous Multiple Sclerosis–like Disease in a Nonhuman Primate

Page 39: The charcot project - antivirals to treat MS

HTLV-1 myelopathy

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Experimental evidence

Page 41: The charcot project - antivirals to treat MS

N Engl J Med 2008;358:676-88.

Please note rituximab is the only licensed anti-EBV drug!

Page 42: The charcot project - antivirals to treat MS

Baker et al. EBioMedicine. 2017 Feb;16:41-50.

Page 43: The charcot project - antivirals to treat MS

Saha & Robertson. DOI: 10.1158/1078-0432.CCR-10-2578 Published May 2011

EBV & B-cell

biology

Page 44: The charcot project - antivirals to treat MS

Sir Bradford-Hill: Criteria for Causation

Bradford-Hill A. The environment and disease: association or causation? Proc Royal Soc Med 1966; 58:295.

1. CONSISTENCY AND UNBIASEDNESS OF FINDINGS - Yes (not 100%)

2. STRENGTH OF ASSOCIATION – ? / Yes (RR ~ 2 to 3)

3. TEMPORAL SEQUENCE - Yes

4. BIOLOGICAL GRADIENT (DOSE-RESPONSE RELATIONSHIP) - ? (not relevant to infections)

5. SPECIFICITY – No (not 100% other putative autoimmune diseases also associated with

EBV)

6. COHERENCE WITH BIOLOGICAL BACKGROUND AND PREVIOUS KNOWLEDGE - No

7. BIOLOGICAL PLAUSABILITY - Yes

8. REASONING BY ANALOGY - Yes

9. EXPERIMENTAL EVIDENCE - No

EBV is the cause of MS, but we don’t know how it causes MS!

Page 45: The charcot project - antivirals to treat MS

Dual-viral hypothesis

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Charcot Project: viral aetiology

HIV and lower risk of MS: beginning to unravel a mystery using a record-linked database study

Nexø et al. Epidemiology 2013; 24:331-2

Treatment of HIV and Risk of Multiple Sclerosis

Gold et al. JNNP August 4, 2014 as 10.1136/jnnp-2014-307932.

Raltegravir → RRMS (INSPIRE STUDY)ClinicalTrials.gov ID: NCT01767701

Page 51: The charcot project - antivirals to treat MS

Endogenous retroelements and autoimmune disease

Volkman & Stetson. Nat Immunol 2014

Page 52: The charcot project - antivirals to treat MS

HERV-W-Env Protein Pathogenicity

HERV-W-Env protein

The envelope protein of HERV-W

Typically not expressed in healthy individuals.

Abnormal expression triggered by environmental factors (EBV…)

Appears to be involved in Multiple Sclerosis pathogenesis.

Activation of TLR4 pathway

by HERV-W-Env

Immune system

➢ Inflammation

➢ Autoimmunity

Non-immune cells

➢ Endothelial cells: inflammatory

responses

➢ Schwann cells: inflammatory

responses

➢ Oligodendrocytes precursor cells:

differentiation / remyelination blockade

GNbAC1A monoclonal humanized antibody

neutralizing HERV-W-Env

Successful Phase I and Phase IIa clinical trials in MS indication

Currently in Phase IIb efficacy clinical trial

HERV-W-Env

HERV-W-Env – TLR4 signaling pathway

Perron H et al. Virology. 2001;

Rolland A et al. J Immunol. 2006;

Kremer D, et al. Ann Neurol. 2013

Duperray A et al. Int Immunol. 2015;

Madeira et al. 2016, J Neuro Immunol;

Faucard et al. 2015, Ebiomedic;

Curtin et al. 2016, MS Relat DisordSlide courtesy : Hervé Perron

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▪ Phase I Study completed in January 2012/validated July 2012

Excellent safety profile; No immunogenicity; PK is dose linear; Half-life compatible with

monthly administration

GNbAC1 a Humanized IgG4 antibody

neutralizing HER-W Env in Clinical trials

Curtin et al. Clin. Ther. 2012

▪ Phase IIa 1 year Study in MS patients with monthly infusions completed in March 2014:

promising data for GNbAC1.

▪ Excellent safety profile; No immunogenicity; MRI stability and no progression, notably

in PMS

▪ Safe mode of action validated in patients: No modification of any physiological

immune function in one-year treated patients (Normal profile of immune cell sub-

popuplations and responses to Immunity test panel in all patients…)

▪ Beyond expected simple effects of an “toxin-neutralizing” antibody.

Curtin et al. Mult. Scler. 2014

▪ Phase IIb efficacy Study Started in 2016: 10 European countries; 320 patients;

ascending doses (6, 12, 18 mg/Kg) and placebo; 1 year Monthly injections;

patients.

▪ Final 1-year results expected in March 2018.

Slide courtesy : Hervé Perron

Page 54: The charcot project - antivirals to treat MS

HERV-W genomic structure as sequenced from MSRV virions

May antiretroviral drugs inhibit the expression of HERV-

W genome when activated ?

Slide courtesy : Hervé Perron

Page 55: The charcot project - antivirals to treat MS

HERV-W endogenous retroviruses and MS

Dolei, MSJ 2018, Vol. 24(1) 42–47.

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Targeting HERVs

BioEssaysVolume 35, Issue 9, pages 794-803, 17 JUL 2013 DOI: 10.1002/bies.201300049http://onlinelibrary.wiley.com/doi/10.1002/bies.201300049/full#bies201300049-fig-0001

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INSPIRE: Raltegravir (Isentress) Pilot Study in Relapsing MS

change in gradient

change

(in means)

V1

V2

(screening

before

visit)V3 V4 V5 V6 V7

V8 after

Raltegravir

dispensed

A statistically significant

change in means is not in

this situation consistentwith a reduction inoutcome values due to

intervention.Raltegravir → RRMS (INSPIRE STUDY)ClinicalTrials.gov ID: NCT01767701

Slide courtesy : Julian Gold

Page 58: The charcot project - antivirals to treat MS

PREVENTION

DISEASE

MODIFICATION

1. Epidemiologists

2. Virologists

3. Genomics

4. Bioinformatics

5. Immunologists

6. Neurologists

7. Pharmaceuticals

EBV

? mutations

Conclusion: ‘The Charcot Project’- EBV & HERVs

Early infection

Late infection

Asymptomatic

seroconversion

Infectious

mononucleosis

At risk MS

vD/Sunlight Obesity

Genetics

Vaccine

IM Rx

Anti-EBV

HAART

HERVs

GNbAC1

Smoking

Diet

Page 59: The charcot project - antivirals to treat MS

Arthur Schopenhauer

(1788 –1860)

All truth passes through three stages:

• It is ridiculed

• It is violently opposed

• It is accepted as self-evident

Page 60: The charcot project - antivirals to treat MS

Is there a “Black Swan” flying in?

Page 61: The charcot project - antivirals to treat MS

AcknowledgementsQMUL:

Ute Meier

Monica Marta

Sreeram Ramagopalan

Ruth Dobson

Jo Topping

Georgina Burrow

Cosimo Maggiore

Hadi Amir-Maghzi

Chris Hawkes

Klaus Schmierer

David Baker

Jack Cuzick

Nick Wald

David Holden

Oxford:

George Ebers

Sreeram Ramagopalan

Adam Handel

Giulio DeSanto

Epidemiology, Oxford:

Raph Goldacre

Michael Goldacre

David Yeates

The Albion Centre, Sydney:

Julian Gold

Hubert Maruszak

UCL:

Robin Weiss

Rachel Farrell

Jeremy Garson

VU Amsterdam:

Jaap Middeldorp

Sandra Amor

Edinburgh:

Dorothy Crawford

Karen McCauley

Aarhus University:

Tove

Christiansen