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Completed RESEARCH GRANT UKRI Gateway to Research

Unravelling dorsal root ganglion as an intrinsic filtering device

£4.54M GBP

Funder Medical Research Council
Recipient Organization University of Leeds
Country United Kingdom
Start Date Aug 31, 2021
End Date Dec 31, 2024
Duration 1,218 days
Number of Grantees 3
Roles Co-Investigator; Principal Investigator; Award Holder
Data Source UKRI Gateway to Research
Grant ID MR/V012738/1
Grant Description

Pathological pain continues to constitute an enormous yet unresolved health problem. Despite centuries of research and investment, the precise mechanistic understanding of numerous pathological pain conditions remains incomplete and opioids (such as morphine) are still a 'gold standard' in analgesia. Accordingly, many types of pain (such as chronic arthritis pain, migraine, neuropathic and cancer pains) are particularly difficult to treat since most of the conventional pain-killers either do not relieve such pain or have serious side-effects.

In order to perceive and evaluate our environment, humans are equipped with peripheral nerves (peripheral somatosensory system). These nerves run through our body and collect information about rigidity, warmth and chemical composition of the surrounding milieu and also about our own body's integrity. Specific 'damage-sensing' nerves (nociceptors) are responsible for generating pain sensation.

In order to understand and treat pain we need a better understanding of the mechanisms of how nociceptive nerve fibers conduct signals from the periphery to the central nervous system (CNS) where the perception of pain is formed. We have discovered that there is a structure within each nerve that can limit how much of 'pain' signal is delivered to CNS.

These microscopic 'filters' may hold a key to our ability to block these signals off so that they do not reach the brain. This project is focused on deciphering how these 'signal filters' work, with an ultimate goal to leveraging these to provide new ways to relieve pain in a range of debilitating conditions. Our preliminary work established that such filtering is robust in nerves that deal with pain specifically but less so in other sensory nerves.

However, hardly anything is known about the overall principles of how these filters work, why they work differently in nerves of different type or how this filtering changes in chronic pain conditions. Our project attempts to answer these intriguing questions through three specific aims: i) Obtain detailed information on the design of these filters in sensory nerves of different types.

ii) Create biologically realistic computer models for the filtering process in different nerves. iii) Test how such filtering is altered in preclinical models of chronic pain due to nerve injury.

To achieve the above aims we have developed a comprehensive and multidisciplinary approach which combines cutting-edge biology approaches, such as what is called light-sheet microscopy allowing to look deep into animal tissue, in vivo studies and extensive computer modelling. We are confident that this research will bring new understanding of human sensory systems and, particularly, of chronic pain mechanisms.

Importantly, our findings may shape new approaches for analgesic drug development and effective pain management, thus having significant benefit for individuals who suffer from chronic pain conditions

All Grantees

University of Texas At San Antonio; University of Leeds

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