02%). Both gender
and height were strongly correlated with ENFD; however, when both were included in the model, height remained significant whereas gender was not significant at an alpha level of 0.10. A partial F-test on the additional effect of gender confirmed that gender could be dropped from the model. To examine the incremental effect of OXPHOS CI and CIV enzyme activity as well as of mt 8-oxo-dG levels, each was introduced individually into the previously constructed model. The association between distal leg ENFD and log PBMC CIV activity was significant (P = 0.04; incremental adjusted R 2 = 2%); that between distal leg ENFD and log PBMC CI activity was on the border of significance (P = 0.06; incremental adjusted R 2 = 1.58%). No significant NVP-BEZ235 in vivo association was observed
between distal leg ENFD and PBMC mt 8-oxo-dG. BMI was included in the adjusted model for distal leg ENFD because of its confounding effect on the relationship between ENFD and HIV RNA. The final model revealed that age, CD4 cell count, height, BMI, and log10 PBMCCIV activity were significant predictors of distal leg ENFD (adjusted R 2 = 27.33%; Table 3). Similar analyses were performed to construct a final regression model for proximal thigh ENFD. Although Pearson correlation showed potential associations of proximal thigh ENFD with height and CD4 cell count, a model with all
effects of interests (age, height, CD4 cell count, and log10HIV RNA) showed that only CD4 cell count was a significant predictor, explaining Talazoparib supplier approximately 4.6% of the variability in proximal thigh ENFD. Our study found that older age, larger BMI, taller stature, lower CD4 cell count and higher PBMC OXPHOS CIV levels were risk factors for lower distal leg ENFD in ARV-naïve Thai subjects free of neuropathy. ENFD documents the extent of damage present in unmyelinated nerve fibres per mm length of epidermis. A distal ENFD of 10 fibres/mm or less in US HIV-infected individuals with either no neuropathy or asymptomatic disease has been reported to confer a 14-fold greater risk of Amine dehydrogenase developing symptomatic disease than ENFD > 10 fibres/mm [8]. Early data obtained from hospitalized patients in the US before ARV medications were available indicated that approximately one-third of HIV-infected patients had both clinical and electrophysiological evidence of neuropathy [9]. Neuropathy was primarily noted to be a complication of late-stage HIV disease associated with advanced immunosuppression [10]. However, while neuropathic symptoms frequently did not occur until the development of AIDS, electrophysiological evidence of peripheral nerve involvement was found in many patients with normal or near-normal CD4 cell counts [11].
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