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    Cytokine genotype suggests a role for inflammation in nucleoside analog-associated sensory neuropathy (NRTI-SN) and predicts an individual's NRTI-SN risk

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    Authors
    Cherry, C.
    Rosenow, A.
    Affandi, J.
    McArthur, J.
    Wesselingh, S.
    Price, Patricia
    Date
    2008
    Type
    Journal Article
    
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    Citation
    Cherry, C. and Rosenow, A. and Affandi, J. and McArthur, J. and Wesselingh, S. and Price, P. 2008. Cytokine genotype suggests a role for inflammation in nucleoside analog-associated sensory neuropathy (NRTI-SN) and predicts an individual's NRTI-SN risk. AIDS Research and Human Retroviruses. 24 (2): pp. 117-123.
    Source Title
    AIDS Research and Human Retroviruses
    DOI
    10.1089/aid.2007.0168
    ISSN
    0889-2229
    School
    School of Biomedical Sciences
    URI
    http://hdl.handle.net/20.500.11937/35531
    Collection
    • Curtin Research Publications
    Abstract

    Nucleoside analog-associated sensory neuropathy (NRTI-SN) attributed to stavudine, didanosine, or zalcitabine (the dNRTIs) and distal sensory polyneuropathy (DSP) attributed to HIV are clinically indistinguishable. As inflammatory cytokines are involved in DSP, we addressed a role for inflammation in NRTI-SN by determining the alleles of immune-related genes carried by patients with and without NRTI-SN. Demographic details associated with risk of various neuropathies were included in the analysis. Alleles of 14 polymorphisms in 10 genes were determined in Australian HIV patients with definite NRTI-SN (symptom onset <6 months after first dNRTI exposure, n = 16), NRTI-SN-resistant patients (no neuropathy despite >6 months on dNRTIs, n = 20), patients with late onset NRTI-SN (neuropathy onset after >6 months of dNRTIs, n = 19), and HIV-negative controls. Carriage of TNFA-1031*2 was highest in NRTI-SN patients, suggesting potentiation of NRTI-SN. Carriage of IL12B (3' UTR)*2 was higher in NRTI-SN-resistant patients than controls or NRTI-SN patients, suggesting a protective role. BAT1 (intron 10)*2 was more common in NRTI-SN than resistant patients, but neither group differed from controls. This marks the conserved HLA-A1, B8, DR3 haplotype. Of the demographic details considered, increasing height was associated with NRTI-SN risk. A model including cytokine genotype and height predicted NRTI-SN status (p < 0.0001, R2 = 0.54). Late onset NRTI-SN patients clustered genetically with NRTI-SN-resistant patients, so these patients may be genetically "protected." In addition to patient height, cytokine genotype influenced NRTI-SN risk following dNRTI exposure, suggesting inflammation contributes to NRTI-SN. © 2008 Mary Ann Liebert, Inc.

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    • Age and height predict neuropathy risk in patients with HIV prescribed stavudine
      Cherry, C.; Affandi, J.; Imran, D.; Yunihastuti, E.; Smyth, K.; Vanar, S.; Kamarulzaman, A.; Price, Patricia (2009)
      OBJECTIVE: Sensory neuropathy is a common problem in HIV-infected patients and is the dose-limiting toxicity of stavudine. Affordable methods of predicting neuropathy risk are needed to guide prescribing in countries where ...
    • Can we predict neuropathy risk before stavudine prescription in a resource-limited setting?
      Affandi, J.; Price, Patricia; Imran, D.; Yunihastuti, E.; Djauzi, S.; Cherry, C. (2008)
      A toxic sensory neuropathy associated with exposure to inexpensive nucleoside analogue reverse transcriptase inhibitors (NRTIs) [particularly stavudine (d4T)] causes dilemmas in the management of patients with HIV, ...
    • A polymorphism in IL4 may associate with sensory neuropathy in African HIV patients
      Wadley, A.; Kamerman, P.; Chew, C.; Lombard, Z.; Cherry, C.; Price, Patricia (2013)
      Introduction Animal and in vitro models of HIV-associated sensory neuropathy suggest an inflammatory etiology. Previous genetic association studies of HIV-SN have been in small Caucasian or Asian cohorts. We assessed ...
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