understanding gene and cell therapy approaches for dmd november 6 2015

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Understanding Gene and Cell Understanding Gene and Cell Therapy Approaches for DMD Therapy Approaches for DMD November 6 2015 November 6 2015

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Page 1: Understanding Gene and Cell Therapy Approaches for DMD November 6 2015

Understanding Gene and Cell Therapy Understanding Gene and Cell Therapy Approaches for DMDApproaches for DMD

November 6 2015November 6 2015

Page 2: Understanding Gene and Cell Therapy Approaches for DMD November 6 2015

Overview

Annemieke Aartsma-Rus

• What does dystrophin do?

• What happens when there is no dystrophin?

• How does drug development work

• What genetic approaches are in development to replace dystrophin?

• How do they work

• Challenges/opportunities

Page 3: Understanding Gene and Cell Therapy Approaches for DMD November 6 2015

Some basic biology: genes & proteins

Annemieke Aartsma-Rus

• Proteins are building blocks of our body

• Genes contain blueprint for proteins

• Mistake in gene mistake in protein

• Genes have a volume switch (protein only produced in proper tissue)

• Dystrophin protein has a function in muscle

• Mistake in dystrophin Problems in muscle

Page 4: Understanding Gene and Cell Therapy Approaches for DMD November 6 2015

Muscles

Annemieke Aartsma-Rus

• 30-40% of our body is muscle

• >750 different muscles

• Muscles can grow bigger or smaller

• Muscles use a lot of energy

• Only maintained when needed

• Muscles are damaged when used too much

• Muscles have efficient system to repair damage and prevent future damage (grow bigger)

Page 5: Understanding Gene and Cell Therapy Approaches for DMD November 6 2015

Muscle contraction

Annemieke Aartsma-Rus

Page 6: Understanding Gene and Cell Therapy Approaches for DMD November 6 2015

Muscle fibers

Annemieke Aartsma-Rus

SkeletonSkeleton

Connective tissueConnective tissue

Page 7: Understanding Gene and Cell Therapy Approaches for DMD November 6 2015

Dystrophin

Annemieke Aartsma-Rus

• Dystrophin provides stability to muscle fibers during contraction

• Connects skeleton of muscle fibers to connective tissues surrounding muscle fibers

• No dystrophin Connection lost

• Muscle more sensitive to damage

• Chronic damage: repair system cannot keep up

• Loss of muscle tissue and function

Page 8: Understanding Gene and Cell Therapy Approaches for DMD November 6 2015

Dystrophin

Annemieke Aartsma-Rus

DystrophinDystrophin

Page 9: Understanding Gene and Cell Therapy Approaches for DMD November 6 2015

Duchenne: no functional dystrophin

Annemieke Aartsma-Rus

Page 10: Understanding Gene and Cell Therapy Approaches for DMD November 6 2015

What happens without dystrophin

Annemieke Aartsma-Rus

InflammationRepair

Muscle damage

Fibrosis

Less blood flow Too much Ca2+

Oxidative stress Mitochondria damaged

Loss of muscle tissueLoss of muscle function

Page 11: Understanding Gene and Cell Therapy Approaches for DMD November 6 2015

What are muscle cross sections?Muscle cross sectionsMuscle cross sections

Annemieke Aartsma-Rus

H&E stainingH&E stainingFibers pinkFibers pinkNuclei blueNuclei blue

Page 12: Understanding Gene and Cell Therapy Approaches for DMD November 6 2015

Dystrophin stainingDystrophin immune staining

Annemieke Aartsma-Rus

Healthy Mdx mouse Duchenne

Page 13: Understanding Gene and Cell Therapy Approaches for DMD November 6 2015

Revertant fibers & trace amounts

Annemieke Aartsma-Rus

Revertant Fibers

Trace amounts

Untreated DMD muscle

Page 14: Understanding Gene and Cell Therapy Approaches for DMD November 6 2015

Western blotting

Western blotWestern blot• Proteins isolated from muscleProteins isolated from muscle• Separated by sizeSeparated by size• Stain for dystrophinStain for dystrophin

Annemieke Aartsma-Rus

DMDDMD Becker (dilutions)Becker (dilutions) Control (diluted)Control (diluted)LongLong

ShortShort

Page 15: Understanding Gene and Cell Therapy Approaches for DMD November 6 2015

Therapy development

Annemieke Aartsma-Rus

• Dystrophin is missing• Trying to replace dystrophin

• Also many other therapies aiming at improving muscle quality/slowing down disease processes

Page 16: Understanding Gene and Cell Therapy Approaches for DMD November 6 2015

What are cell models

Annemieke Aartsma-Rus

• Cells derived from patients • Muscle biopsies• Skin biopsies converted into muscle cells (lab)

• Expanded in the lab (limited!!)• “Immortalized” cells

• Muscle stem cells treated with viruses• Keep expanding, but have been modified

• Cell cultures are model systems• Valuable tool for early stages of research

Page 17: Understanding Gene and Cell Therapy Approaches for DMD November 6 2015

What are mdx mice?

Annemieke Aartsma-Rus

Mdx mouse• Mutation in mouse dystrophin gene• No dystrophin protein• But….disease not very severe

• Very efficient muscle regeneration• Turns up volume switch utrophin gene in muscle

• No dsytrophin & utrophin: severe disease• (Double knockout mouse)

Page 18: Understanding Gene and Cell Therapy Approaches for DMD November 6 2015

Other animal models

Annemieke Aartsma-Rus

Golden retriever muscular dystrophy (GRMD)• Mutation in dog dystrophin gene• No dystrophin protein• Mutation beginning gene• Severe disease (muscle & heart)• Muscle weakness, remain ambulant• Most dogs do not live > year • Severity is variable

• Rare mild individuals

Page 19: Understanding Gene and Cell Therapy Approaches for DMD November 6 2015

Other animal models

Annemieke Aartsma-Rus

Pig model• Mutation in pig dystrophin gene• No dystrophin protein• Deletion exon 52• Severe disease (muscle & heart)

Page 20: Understanding Gene and Cell Therapy Approaches for DMD November 6 2015

Drug testing in patients

Annemieke Aartsma-Rus

• Test compound properties• Taken up by tissues efficiently?• How quickly cleared from the body?

• Test compound for efficacy• Does it work?• At which dose?

• Test compound for safety• Are there side effects?• At which dose?• Are they tolerable?

Page 21: Understanding Gene and Cell Therapy Approaches for DMD November 6 2015

Development of therapies

Annemieke Aartsma-Rus

• Tests from cell and animal models to clinical trials

• All steps are important to show proof-of-concept (does it work in a model system ?)

• Next steps are always more complicated

• Success in one step is no guarantee for success in subsequent steps

• Clinical trials are experiments in humans

• May not work, may not be safe

Page 22: Understanding Gene and Cell Therapy Approaches for DMD November 6 2015

Cell therapy

Annemieke Aartsma-Rus

Muscle stem cells• Isolate muscle stem cells from healthy donor

• Expand outside the body (culture in lab)

• Transplant into patients

• Transplanted cells repair muscle

• Transplanted cells make dystrophin

Page 23: Understanding Gene and Cell Therapy Approaches for DMD November 6 2015

Muscle stem cells (myoblasts)

Annemieke Aartsma-Rus

• Immune response (suppress)• Do not exit circulation after injection• Local injection: stay close to injection site• Tremblay (Canada): multiple local injections

• Local dystrophin restoration• Not feasible for larger muscles

Page 24: Understanding Gene and Cell Therapy Approaches for DMD November 6 2015

Stem cell therapy

Annemieke Aartsma-Rus

Stem cells from fat, bone and bloodvessel walls • Can exit bloodstream and migrate into muscle• Very low efficiency

Mesangioblasts most promising• Encouraging results in dog model• Safety trial ongoing in Italy (Giulio Cossu) • 3 patients received stem cells• Some side effects• Preparing for injection 2 more patients

Page 25: Understanding Gene and Cell Therapy Approaches for DMD November 6 2015

Niche

Annemieke Aartsma-Rus

InflammationRepair

Muscle damage

Fibrosis

• Dystrophic muscle is damaged (scar tissue/fibrosis)• The few transplanted stem cells that reach muscle

• Do not receive proper signals to become muscle• Receive signals from scar tissue: more fibrosis

Page 26: Understanding Gene and Cell Therapy Approaches for DMD November 6 2015

Immunity

Annemieke Aartsma-Rus

• Transplanting cells from one person to another will elicit an immune response

• Need chronic immune suppression

• Side effects

• Isolate patient stem cells, expand in the lab, correct mutation with gene therapy & transplant

• No immune response

• Gene therapy more efficient in cultured cells than in muscles

Page 27: Understanding Gene and Cell Therapy Approaches for DMD November 6 2015

Cell therapy summary

Annemieke Aartsma-Rus

• Opportunities

• Applicable to all patients

• Deliver dystrophin gene and repair muscle

• Currently in very early stage clinical development

• Challenges

• Efficiency very low

• Damaged muscle gives wrong signals to cells

• Immunity (only with allogenic transplantation

Page 28: Understanding Gene and Cell Therapy Approaches for DMD November 6 2015

Gene Therapy

Annemieke Aartsma-Rus

• Add functional gene to muscle cells patients

• Dystrophin protein made from new gene

• Applicable to ALL patients

• Genes located in nucleus cells

• How to get gene into (majority) nuclei of muscle cells?

Page 29: Understanding Gene and Cell Therapy Approaches for DMD November 6 2015

Gene Therapy

Annemieke Aartsma-Rus

Maaike van Putten

Page 30: Understanding Gene and Cell Therapy Approaches for DMD November 6 2015

Gene Therapy

Annemieke Aartsma-Rus

Virus

• Small organism that injects genetic information into cells

• Use to deliver dystrophin gene

• Adapt

• Remove virus genes (pathogenic)

• Add new gene (dystrophin)

Page 31: Understanding Gene and Cell Therapy Approaches for DMD November 6 2015

Gene Therapy

Annemieke Aartsma-Rus

Which virus?

• Most viruses do not infect muscle tissue

• Muscle cells do not divide often

• Lot of connective tissue (filters out viruses)

• Exception: adeno-associated virus (AAV)

• Preference for muscle

• Not pathogenic in man

Page 32: Understanding Gene and Cell Therapy Approaches for DMD November 6 2015

Gene Therapy

Annemieke Aartsma-Rus

• Very small (20 nm, 0.00002 mm)

• Capacity: 4.500 DNA subunits

• Dystrophin gene: 2.200.000 DNA subunits

• Genetic code gene: 14.000 subunits

• Remove part from genetic code

• Only essential parts remain

Page 33: Understanding Gene and Cell Therapy Approaches for DMD November 6 2015

Gene Therapy

Annemieke Aartsma-Rus

MicrodystrophinOnly crucial domainsFits in AAV particle

Page 34: Understanding Gene and Cell Therapy Approaches for DMD November 6 2015

Gene Therapy

Annemieke Aartsma-Rus

Clinical trials

• Safety study in 6 Duchenne patients

• 2006/7, USA: local injection biceps (Mendell,Samulski, Xiao Xiao)

• Immune response!

• Dystrophin in 2/6 patients (very low levels)

• Prepare for bigger trial (whole muscle treatment)

Page 35: Understanding Gene and Cell Therapy Approaches for DMD November 6 2015

Upscaling

Annemieke Aartsma-Rus

• Mouse 12 gram muscle

• Monkey 4 kg muscle

• Human boy 10-25 kg muscle

• Monkeys and humans much larger than mice

• Need much more viruses

• Manufacturing systems optimized to allow production of sufficient amounts for treating human limbs at clinical grade

333x

2-6x

Page 36: Understanding Gene and Cell Therapy Approaches for DMD November 6 2015

Delivery

Annemieke Aartsma-Rus

• Whole animal delivery possible for mouse

• Not feasible (yet) for large animals

• Limited by amount of virus

• Produced

• Injected

• Whole limb delivery in development for human

• Hydrodynamic limb perfusion (most efficient)

• Regional limb perfusion (less damage)

Page 37: Understanding Gene and Cell Therapy Approaches for DMD November 6 2015

Limb perfusion

Annemieke Aartsma-Rus

• Tested in monkeys and dogs with ‘color gene’

• Delivery to multiple muscles feasible

• Tested in adult MD patients with saline

• Possible for lower leg or arm (less efficient)

• Not yet tested in humans to deliver gene

Page 38: Understanding Gene and Cell Therapy Approaches for DMD November 6 2015

Gene Therapy Summary

Annemieke Aartsma-Rus

• Opportunities

• Applicable to all patients

• Currently in early clincial development (safety/tolerability tests)

• Challenges

• Microdystrophin only partially functional

• Delivery

• Immunity

Page 39: Understanding Gene and Cell Therapy Approaches for DMD November 6 2015

Gene/cell therapy: DNA editing

Annemieke Aartsma-Rus

• DNA has a repair system

• Activated upon DNA damage

• Use this system to correct for DNA mistakes?

Mutation

Template with correct DNA information

DNA repair system

Mistake corrected (in one cell)

Page 40: Understanding Gene and Cell Therapy Approaches for DMD November 6 2015

DNA editing

Annemieke Aartsma-Rus

• Challenge: DNA repair system very inefficient (1 in 1,000,000 – 1,000,000,000 cells)

• Much more efficient when DNA is ‘broken’ (1 in 10-1000 cells)

Have to generate DNA breaks at/close to mutation

Page 41: Understanding Gene and Cell Therapy Approaches for DMD November 6 2015

DNA scissor system

Annemieke Aartsma-Rus

• DNA scissors can cut DNA at specific location

Scissor cuts at/near mutation

Repair break with template(Correct small mutations)

Repair break without templateSmall mutations will be introduced (can correct genetic code like exon skipping)

Page 42: Understanding Gene and Cell Therapy Approaches for DMD November 6 2015

DNA scissor system

Annemieke Aartsma-Rus

Combination of DNA scissors to restore genetic code

Scissors cut around exon break is repaired

Exon is deleted Genetic code restored (like exon skipping)

Page 43: Understanding Gene and Cell Therapy Approaches for DMD November 6 2015

DNA scissor system

Annemieke Aartsma-Rus

• DNA scissors can make breaks in DNA

• Different types of scissors in development

• Zinc Fingers, TALENs and RGNs

• Challenge: deliver scissors and templates to muscles

Page 44: Understanding Gene and Cell Therapy Approaches for DMD November 6 2015

Exon skipping

Annemieke Aartsma-Rus

NormalNormal DuchenneDuchenne

Page 45: Understanding Gene and Cell Therapy Approaches for DMD November 6 2015

Dystrophin gene

Annemieke Aartsma-Rus

Page 46: Understanding Gene and Cell Therapy Approaches for DMD November 6 2015

Splicing

Annemieke Aartsma-Rus

ExonsExons IntronsIntrons1

3

5

6

7 Gene (DNA)Gene (DNA)

RNA copy (pre mRNA)RNA copy (pre mRNA)

messenger RNAmessenger RNA

1 - - - - - - - - - 79

dystrophin proteindystrophin protein

SplicingSplicing

2

4

3 4 56 7

1 21 2 3 4 5 6 7 8

Page 47: Understanding Gene and Cell Therapy Approaches for DMD November 6 2015

Duchenne: genetic code disrupted

Annemieke Aartsma-Rus

Page 48: Understanding Gene and Cell Therapy Approaches for DMD November 6 2015

Duchenne: genetic code disrupted

Annemieke Aartsma-Rus

Protein translation stops prematurelyProtein translation stops prematurely

Dystrophin not functionalDystrophin not functional

Exon 46 Exon 47 Exon 51 Exon 52?

Page 49: Understanding Gene and Cell Therapy Approaches for DMD November 6 2015

Becker: genetic code maintained

Annemieke Aartsma-Rus

Page 50: Understanding Gene and Cell Therapy Approaches for DMD November 6 2015

Becker: genetic code maintained

Annemieke Aartsma-Rus

Protein translation continuesProtein translation continues

Dystrophin partly functionalDystrophin partly functionalLess damageLess damage

Exon 46 Exon 47 Exon 52 Exon 53

Page 51: Understanding Gene and Cell Therapy Approaches for DMD November 6 2015

Exon skipping: restore genetic code

Annemieke Aartsma-Rus

Page 52: Understanding Gene and Cell Therapy Approaches for DMD November 6 2015

Applicability

Annemieke Aartsma-Rus Aartsma-Rus Hum Mutat 2009, 30:293-9

hotspot

Page 53: Understanding Gene and Cell Therapy Approaches for DMD November 6 2015

Exon skip chemistries

Annemieke Aartsma-Rus

• Two chemistries in clinical development

• GSK/Prosensa: 2’-O-methyl phosphorothioate (drisapirsen)

• AVI-Biopharma/Sarepta: phosphorodiamidate morpholino oligomers (eteplirsen)

• Exon 51

Page 54: Understanding Gene and Cell Therapy Approaches for DMD November 6 2015

Exon skipping summary

Annemieke Aartsma-Rus

• Opportunities

• AON delivery easier than genes/cells

• Clinical trial results encouraging

• Challenges

• Mutation specific approach

• Need to develop many AONs to treat majority of patients

• Repeated treatment needed (also opportunity)

Page 55: Understanding Gene and Cell Therapy Approaches for DMD November 6 2015

Stop codon readthrough

Annemieke Aartsma-Rus

1 79

Page 56: Understanding Gene and Cell Therapy Approaches for DMD November 6 2015

PTC124/ataluren

Annemieke Aartsma-Rus

1 79

PTC

Cell ignores new stop signalCell ignores new stop signalComplete protein is madeComplete protein is made

Page 57: Understanding Gene and Cell Therapy Approaches for DMD November 6 2015

Stop codon readthrough summary

Annemieke Aartsma-Rus

• Opportunities

• Oral delivery

• Applicable to multiple diseases

• Challenges

• Mutation specific approach (15%)