4.2 Article

Understanding the Etiology and Management of HIV-Associated Peripheral Neuropathy

Journal

CURRENT HIV/AIDS REPORTS
Volume 11, Issue 3, Pages 195-201

Publisher

SPRINGER
DOI: 10.1007/s11904-014-0211-2

Keywords

HIV; Peripheral neuropathy; Distal symmetric polyneuropathy; DSP; Anti-retroviral; Pain

Funding

  1. Astellas
  2. Acorda
  3. Pfizer
  4. Depomed

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HIV may cause several forms of peripheral neuropathy, the most common of which is distal symmetric polyneuropathy (DSP) characterized by pain and sensory deficits in a stocking-glove distribution. The pathophysiology of DSP remains largely unknown but is thought to be related both to the neurotoxicity of HIV-through indirect immunomodulatory mechanisms-and to the neurotoxic effects of anti-retroviral therapies, most notably the dideoxynucleoside reverse transcription inhibitors or so-called d-drugs. Determining whether symptoms arise from the virus or the treatment poses a challenge to the clinician who must decide if a patient's HAART regimen should be altered. Treatment of symptoms related to HIV-DSP is a difficult task and there is no evidence that the traditional agents used in chronic neuropathic pain are efficacious in the HIV-DSP population. Indeed few pharmacologic agents have proven efficacy in HIV-DSP - these include cannabis and the capsaicin 8 % dermal patch. As such, alternative, non-pharmacologic therapies are being investigated. More research is needed to further elucidate the complex pathophysiology of HIV-DSP which may yield additional therapies for these patients.

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