Study offers a new mindset in the search for stroke therapies
UNSW Australia Health News Sep 13, 2017
UNSW researchers have identified a promising new avenue to explore in the search for stroke treatments, after translating findings from AlzheimerÂs disease.
The study published in the journal Nature Communications finds that mice deficient in tau, a protein within neurons, are significantly protected from excitotoxic brain damage after experimental stroke.
Stroke is a major cause of death and disability, and there is only a short window for therapeutic intervention, aimed at restoring blood flow to the brain before neurons are irreversibly damaged.
Professor Lars Ittner and Dr Yazi Ke at UNSW and NeuRA had already established that in AlzheimerÂs disease, memory deficits and early deaths were tau-dependent.
The researchers suspected a reduction of tau would also reduce acute brain damage in stroke.
ÂTau as a drug target is intensively explored in AlzheimerÂs disease, but as a drug target in stroke is completely new thinking, Professor Ittner said.
ÂThatÂs where our paper has implications beyond mouse model molecular work. Drug development in this space should consider stroke as a disease that you can treat by targeting tau, Dr Ke added.
The paper, with first author Dr Mian Bi and co-senior author Dr Ke, is the first to show a direct role of tau in brain damage after stroke. It demonstrates profound protection from brain damage, of more than 90 per cent, in the absence of tau.
Tau has been eyed as a therapeutic target in AlzheimerÂs disease for several years, and Professor Ittner is hopeful that work in that area can also advance research on stroke.
But he cautions these findings were made in mouse models only, and that pathways to therapies take decades.
ÂThis cannot yet be directly translated to therapy, but what it opens up is a new kind of thinking about the mechanisms that lead to brain damage after stroke, and as such, opens new avenues to develop therapies in the future, he said.
Dr Bi said it will be important that other studies validate the work, and he is sure the findings will encourage more research in this direction.
ÂAround 10 years ago the drug development field in stroke was very hot, but most therapeutic stroke trials came to an end in failure, he said.
ÂAvenues to therapy are very long, but this might re-start interest in the field with a new direction that hasnÂt been tried before. ItÂs a bit of light after all the past failure.Â
Professor Ittner agrees: ÂItÂs a new insight into a disease that is at the molecular level, still poorly understood, and it needs such new insights or rethinking to make a step forward towards therapy.Â
Go to Original
The study published in the journal Nature Communications finds that mice deficient in tau, a protein within neurons, are significantly protected from excitotoxic brain damage after experimental stroke.
Stroke is a major cause of death and disability, and there is only a short window for therapeutic intervention, aimed at restoring blood flow to the brain before neurons are irreversibly damaged.
Professor Lars Ittner and Dr Yazi Ke at UNSW and NeuRA had already established that in AlzheimerÂs disease, memory deficits and early deaths were tau-dependent.
The researchers suspected a reduction of tau would also reduce acute brain damage in stroke.
ÂTau as a drug target is intensively explored in AlzheimerÂs disease, but as a drug target in stroke is completely new thinking, Professor Ittner said.
ÂThatÂs where our paper has implications beyond mouse model molecular work. Drug development in this space should consider stroke as a disease that you can treat by targeting tau, Dr Ke added.
The paper, with first author Dr Mian Bi and co-senior author Dr Ke, is the first to show a direct role of tau in brain damage after stroke. It demonstrates profound protection from brain damage, of more than 90 per cent, in the absence of tau.
Tau has been eyed as a therapeutic target in AlzheimerÂs disease for several years, and Professor Ittner is hopeful that work in that area can also advance research on stroke.
But he cautions these findings were made in mouse models only, and that pathways to therapies take decades.
ÂThis cannot yet be directly translated to therapy, but what it opens up is a new kind of thinking about the mechanisms that lead to brain damage after stroke, and as such, opens new avenues to develop therapies in the future, he said.
Dr Bi said it will be important that other studies validate the work, and he is sure the findings will encourage more research in this direction.
ÂAround 10 years ago the drug development field in stroke was very hot, but most therapeutic stroke trials came to an end in failure, he said.
ÂAvenues to therapy are very long, but this might re-start interest in the field with a new direction that hasnÂt been tried before. ItÂs a bit of light after all the past failure.Â
Professor Ittner agrees: ÂItÂs a new insight into a disease that is at the molecular level, still poorly understood, and it needs such new insights or rethinking to make a step forward towards therapy.Â
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