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Huntington's Disease Therapeutics Conference 2016 – day 2

Strategies for getting rid of mutant huntingtin & clinical trial updates: day 2 of the HD therapeutics conference

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After an exciting day of science yesterday, day 2 saw updates on strategies to rid cells of the harmful mutant huntingtin proteinhuntingtin protein The protein produced by the HD gene. and exciting reports on current and planned clinical trials.

Wednesday morning – huntingtin lowering strategies

Huntingtin lowering or “gene silencinggene silencing An approach to treating HD that uses targeted molecules to tell cells not to produce the harmful huntingtin protein” may be the most exciting potential HD treatment strategy. Since every case of HD is due to inheriting a mutant HD gene, getting rid of the effects of that gene is a very attractive idea! We’ve talked a lot about gene silencinggene silencing An approach to treating HD that uses targeted molecules to tell cells not to produce the harmful huntingtin protein at HDBuzz – catch up here if the topic is new to you.

Eric Reitz used home-drawn chicken cartoons to explain his work on cellular garbage clearance in HD
Eric Reitz used home-drawn chicken cartoons to explain his work on cellular garbage clearance in HD

Ignacio Munoz-Sanjuan is giving an update about efforts at the CHDI foundation to develop “biomarkers” to improve silencing studies. A “biomarkerbiomarker a test of any kind – including blood tests, thinking tests and brain scans – that can measure or predict the progression of a disease like HD. Biomarkers may make clinical trials of new drugs quicker and more reliable.” is some kind of lab test that can be done, in this case, to see if your expeimental drug is doing what you’d like it to. With HD gene silencinggene silencing An approach to treating HD that uses targeted molecules to tell cells not to produce the harmful huntingtin protein studies, the goal is to reduce levels of the protein made from the HD gene.

In the lab, we can easily measure how much mutant huntingtin proteinhuntingtin protein The protein produced by the HD gene. is being made to see if silencing drugs work. But once we start treating human HD patients, we can’t easily get access to the most important tissue we need to treat – the brain. The techniques that Munoz-Sanjuan is describing include imaging techniques that let researchers check on brain health non-invasively. In mice treated with HD gene silencinggene silencing An approach to treating HD that uses targeted molecules to tell cells not to produce the harmful huntingtin protein drugs, several of these imaging techniques show improvements, no brain surgery required!

These lab results are now being examined in HD patients – hopefully they will empower future silencing studies. Beyond imaging, we can try to sample brain levels of the huntingtin proteinhuntingtin protein The protein produced by the HD gene. more directly. Recently, multiple groups have developed ways to measure huntingtin in brain fluid. These tools are already being incorporated into ongoing gene silencinggene silencing An approach to treating HD that uses targeted molecules to tell cells not to produce the harmful huntingtin protein studies!

Pavlina Konstantinova is the director of emerging technologies at uniQure, who have an interest in developing gene silencinggene silencing An approach to treating HD that uses targeted molecules to tell cells not to produce the harmful huntingtin protein for HD. uniQure uses tiny viruses to deliver a small piece of DNA to cells, which instructs them to reduce levels of the huntingtin proteinhuntingtin protein The protein produced by the HD gene.. We’ve recently covered similar viral delivery techniques on HDBuzz. uniQure is testing their gene silencinggene silencing An approach to treating HD that uses targeted molecules to tell cells not to produce the harmful huntingtin protein viruses in HD mice in collaboration with the help of HD researchers. uniQure is also working to better understand whether it’s safe to reduce levels of the HD gene in long-term mouse studies.

The final presentation of the morning is from Jodi McBride, who studies HD gene silencinggene silencing An approach to treating HD that uses targeted molecules to tell cells not to produce the harmful huntingtin protein in both mice and monkeys. Larger animals, like monkeys, are important to study because they have large, complex, brains like humans. Fixing mice is easy! McBride raises a critical issue for gene silencinggene silencing An approach to treating HD that uses targeted molecules to tell cells not to produce the harmful huntingtin protein studies – how safe is it to reduce levels of the huntingtin proteinhuntingtin protein The protein produced by the HD gene.? McBride’s lab is silencing the HD gene in the brains of monkeys to see if this treatment has any toxic side effects. McBride’s team is experimenting with a new brain scanner that lets surgeons infuse gene therapy virus much more accurately. McBride is also working to develop a monkey model of HD by delivering mutant HD genes to their brains using viruses.

Via videoconference, Feng Zhang addresses the meeting on the incredibly hot topic of ‘genome editingGenome Editing The use of zinc-finger nucleases to make changes in DNA. 'Genome' is a word for all the DNA we each have.’. Scientists once believed that we were stuck with the DNA we were born with, but new technologies make it possible to edit DNA. Zhang has conducted pioneering research with the most widely-used genome editingGenome Editing The use of zinc-finger nucleases to make changes in DNA. 'Genome' is a word for all the DNA we each have. tool called CRISPR/Cas9CRISPR A system for editing DNA in precise ways. We’ve covered this technology on HDBuzz before. The CRISPR/Cas9CRISPR A system for editing DNA in precise ways system originates from bacteria, who use it as a defense mechanism against viruses. Researchers have taken advantage of the CRISPRCRISPR A system for editing DNA in precise ways system to make specific changes to DNA in other types of cells, including human ones. Zhang describes the huge zoo of CRISPR/Cas9CRISPR A system for editing DNA in precise ways modifications that scientists have devised to make specific types of genetic changes. Zhang’s lab is working to refine and improve the CRISPR/Cas9CRISPR A system for editing DNA in precise ways system to make sure that it only makes desired changes to DNA. If you’re going to engineer a system that can modify DNA, you want to make sure it follows your instructions!

“The safety board has allowed us to move to the higher dose of gene-silencing drug. This means there were no safety concerns in the first group of patients.”

David Rubinsztein from Cambridge University studies autophagy – one of the garbage-disposal mechanisms in cells. Cellular gunk builds up in HD and increasing garbage removal might help. Drugs to increase autophagy have been tested in HD mice and shown some benefits but the drugs have bad side effects. The search is on for ‘cleaner’ drugs to increase autophagy. Rubinsztein’s team have identified and are studying new ways of activating autophagy. He’s also looking at the relationship between autophagy garbage disposal, and trafficking – the movement of substances round cells. Genetic mutations that affect trafficking may be involved in some caes of Alzheimer’s and Parkinson’s disease.

Eric Reits from University of Amsterdam is interested in another garbage removal system – the proteosome. The proteosome is like a woodchipper in our cells – unwanted stuff is fed into it and broken into little pieces. Reits has developed a new way of looking at which proteins are flagged for woodchipping by the proteosome. The proteosome might help get rid of mutant huntingtin proteinhuntingtin protein The protein produced by the HD gene.. But the proteosome seems to be less efficient in parts of the brain affected most by HD. Can we activate these proteosomes to help get rid of mutant huntingtin? He’s working on it!

Wednesday afternoon: clinical trialclinical trial Very carefully planned experiments designed to answer specific questions about how a drug affects human beings updates

This afternoon we’re getting a blitz of updates from drug companies currently running HD clinical trials. Neal Simon (Azevan Pharmacuticals), describes their STAIR trial with a drug targeting irritability in HD patients. Their first study, designed to see whether the drug is safe, will begin enrolling patients in late March/early April. While establishing the drug is safe, Azevan will also explore whether their drug improves irritability in HD patients.

Marielle Delnomdedieu (Pfizer) updates the conference on the 4 studies they’re currently doing to establish if their drug helps HD. This drug blocks the activity of a brain enzyme called “PDE10PDE10 a brain protein that may be a good drug target and biomarker in Huntington's disease. PDE10 is found almost exclusively in parts of the brain where brain cells die in HD.” – we’ve covered this topic on Buzz. Pfizer has determined that the drug is safe and well-tolerated in HD patients. They’re completed 91% of the recruitment for the Amaryllis trial, which is investigating whether the drug improves HD symptoms. In parallel, they’re also running studies to understand if the drug improves the function of important brain circuits in HD patients.

John Leonard (Vaccinex) updates the crowd about the progress of their SIGNAL trial. The SIGNAL trial is divided into two groups, ‘cohortcohort a group of participants in a clinical research study A’ and ‘cohortcohort a group of participants in a clinical research study B’, the first group of 36 patients is completely recruited. The second group is recruiting now, with a goal of having the final patient visit occur in September 2017.

Sarah Tabrizi presented an update on the current gene silencing trial - this is the trial design
Sarah Tabrizi presented an update on the current gene silencing trial – this is the trial design

The final clinical trialclinical trial Very carefully planned experiments designed to answer specific questions about how a drug affects human beings blitz is from Sarah Tabrizi (University College London) about the HTTRx-CS1 ‘gene silencinggene silencing An approach to treating HD that uses targeted molecules to tell cells not to produce the harmful huntingtin protein’ study she’s leading with Roche and Ionis. This trial is investigating whether “antisense oligonucleotidesASOs A type of gene silencing treatment in which specially designed DNA molecules are used to switch off a gene” (ASOsASOs A type of gene silencing treatment in which specially designed DNA molecules are used to switch off a gene) that reduce levels of the huntingtin proteinhuntingtin protein The protein produced by the HD gene. are safe. Because ASOsASOs A type of gene silencing treatment in which specially designed DNA molecules are used to switch off a gene can’t get into the brain on their own, they have to be delivered by infusion into the spinal fluid around the brain. This is done by infusing the drug into the spinal fluid using a thin needle every four weeks.

Tabrizi shows data from monkeys treated in the same way as the humans patients. ASOASOs A type of gene silencing treatment in which specially designed DNA molecules are used to switch off a gene treatment leads to robust reductions of huntingtin proteinhuntingtin protein The protein produced by the HD gene. across the brain.

Tabrizi: “The safety board has allowed us to move to the higher dose”. This means there were no safety concerns in the first group of patients. Things are moving quickly! Tabrizi: “Estimated study completion date September 2017”

Tabrizi concludes: “the real research heroes in the HD community are the patients an their families that give all their time”.

In the today’s final talk, Marcus Munafo (University of Bristol) suggests some ways in which science can be made more reliable with fewer false starts.

A very exciting afternoon! A huge amount of work happening in clinics around the world to put to use all the basic science we’ve seen.

The authors have no conflicts of interest to declare.

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Glossary

ASOs
A type of gene silencing treatment in which specially designed DNA molecules are used to switch off a gene
biomarker
a test of any kind – including blood tests, thinking tests and brain scans – that can measure or predict the progression of a disease like HD. Biomarkers may make clinical trials of new drugs quicker and more reliable.
clinical trial
Very carefully planned experiments designed to answer specific questions about how a drug affects human beings
cohort
a group of participants in a clinical research study
CRISPR
A system for editing DNA in precise ways
gene silencing
An approach to treating HD that uses targeted molecules to tell cells not to produce the harmful huntingtin protein
Genome Editing
The use of zinc-finger nucleases to make changes in DNA. 'Genome' is a word for all the DNA we each have.
huntingtin protein
The protein produced by the HD gene.
PDE10
a brain protein that may be a good drug target and biomarker in Huntington's disease. PDE10 is found almost exclusively in parts of the brain where brain cells die in HD.

More glossary terms…

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