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Clinical Phenotyping and Genotyping of HIV-Associated Neuropathy

  • Research type

    Research Study

  • Full title

    Clinical Phenotyping and Genotyping of HIV-Associated Sensory Neuropathy : The HIV-POGO study

  • IRAS ID

    155485

  • Contact name

    Andrew Rice

  • Contact email

    a.rice@imperial.ac.uk

  • Sponsor organisation

    Imperial College

  • Research summary

    Clinical Phenotyping and Genotyping of HIV-Associated Sensory Neuropathy : The HIV-POGO study

    HIV associated sensory neuropathy (HIV-SN) is a frequent complication of HIV infection, affecting between 20 and 57% of infected individuals. The advent of better antiretroviral treatment for HIV has meant that mortality from HIV has decreased dramatically in the UK. This means however, that chronic, age-related conditions associated with HIV, such as HIV-SN and cognitive impairment, are increasing in prevalence and becoming a significant disease burden.

    The classification, diagnosis and treatment of HIV-SN remains poor. Currently, little is known about the genetic basis of the disorder and what risk factors mean that some patients with HIV develop neuropathy and pain, whilst others do not. It is hoped that by further characterising or ‘phenotyping’ the disorder, it will be easier to identify which patients are at risk of developing neuropathy and chronic pain. It may also mean that treatment can be more individualised as currently patients often undergo a frustrating 'trial and error' protocol of treatment, as clinicians can not yet predict who will respond to which treatment.

    It has also been suggested that there is a link between HIV-SN and HIV associated neurocognitive disorder (HAND), which is another common, age-related complication of HIV infection. It may be that the existence of one pathology could predict the development of the other, or that the presence of HAND may impair the diagnosis or treatment of chronic pain associated with HIV-SN.

    This study aims to recruit a cohort of HIV patients with and without HIV-SN and to identify genetic risk factors for the development of HIV-SN and neuropathic pain. It also aims to more deeply phenotype the condition, using well validated questionnaires, and to identify any influence that early neurocognitive dysfunction may have on the reporting, diagnosis and treatment of neuropathic pain in the HIV population.

  • REC name

    London - Chelsea Research Ethics Committee

  • REC reference

    14/LO/1574

  • Date of REC Opinion

    3 Oct 2014

  • REC opinion

    Further Information Favourable Opinion

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