CLN1, CLN2, CLN3, CLN5, CLN6, CLN7

Pediatric Storage Disorders Lab (Jon Cooper)New lessons from our work on Batten disease

Jon Cooper (PI), Hemanth Nelvagal, Marta Tarczyluk, Yewande Pearce, Jenny Lange, Charlott Repschlager, Tytus Murphy, Laurent, van Trigt, Ana AssisBasic & Clinical Neuroscience, Institute of Psychiatry, Psychology & Neuroscience, King’s College London, jon.cooper@kcl.ac.uk

Los Angeles Biomedical Research Institute, Department of Pediatrics, Harbor-UCLA Medical Center

David Geffen School of Medicine, University of California, Los Angeles

From 1st August 2016…

The lab is moving to Los Angeles!!

Sorry I can’t be at the BDSRA Family Conference this year,but I’ll look forward to seeing everyone next year…

This is an exciting opportunity to move the lab’s Batten disease research forwards more quickly!!

What goes wrong?

ProteinDNA

Function?X

Mutation

X

No Protein Disease

Mistakes or mutations in DNA passed on from one generation to the next means that proteins that have crucial jobs inside cells don’t get made

There is a failed breakdown & recycling of waste = build up of‘STUFF’

X X X

Where do things happen in the brain? The body is affected too!

It’s not just nerve cells that are important!

Do problemsstart in

heart itself?

OR: due tochanges

in the brain?

OR: a faulty connection

betweenthem?

PERHAPS a combination of these events?

Studying this inmice & human BDHow does this

impact walking?

We normallythink of Batten

disease as mostlyaffecting the brain

BUT we now know(surprisingly)

that the spinal cordhas BIG problems too!

Spinal cord problems start earlybefore they do in the brain

We see this in ALL sorts of Batten disease(CLN1, CLN2, CLN3, CLN7 so far…)

We are now looking what happens in the peripheral nervous system

This happens in peopletoo (not just mice)…

If we treat the cord directlywe can improve pathology

There are alsoproblems elsewhere

in the body

+

Brain Body

NOT just a disease of the brain…

Heart problemsCLN1, CLN3

If we know where and how theseproblems occur then we

can try to treat them

How does this happen?

??

CLN3, CLN6, CLN7

Even in the brain not all parts

are affected the same!

Nerve Cells

Glial Support CellsBillions…

Up to 50 times more!!

Nerve cells are outnumbered by glial cells that help them

Astrocytes

Microglia

Nerve cells(neurons)

Grow cells in a dish from Cln1, Cln2 and Cln3 mice

We previously onlythought about nerve cells

BUT all may be affectedby Batten disease

Three way relationship crucial for brain function

What is ‘missing’ is different in each type of BD

How to ‘fix’ this is likelyto be different too..

How things go wrong is likelyto be different…

Infantile BD (CLN1)Late infantile BD (CLN2)

Enzyme Deficiency

Also: CLN10/CTSD, CLN5?

CAN move from cell to cell

Juvenile BD (CLN3)

Transmembrane Protein

Also: CLN6, CLN7, CLN8

CAN’T move from cell to cell(stuck inside cells)

Can they still do their normal jobs?

If glia are sick then treating them may help

nerve cells too..

?Some drug combinations

appear to slow the disease in Cln3 mice?

CLN1 disease

LOTS of early glial activation, BUTGlia are sick & harm neurons

CLN3 disease

Glial activation early, but ‘get’s stuck’Glia are sick (in a different way)

& harm neurons

CLN2 disease

Problems are with nerve cellsand glia are relatively ‘OK’?

What effects do glia have upon neurons?

Glia are more (or less) important, depending on the sort of Batten disease

We now have new funding to testmore drugs and find more

effective combinations

How these cells are affected is

surprisingly different!!