‘Plasma viral detection’ and ‘past CNS HIV-related diseases’ were

‘Plasma viral detection’ and ‘past CNS HIV-related diseases’ were categorical variables taking a value of 1 when the response was positive. We were not able to test the effect of nadir CD4 cell count because the range of this variable was restricted

in our cohort as advancement of the disease was a criterion of inclusion. For the SVM calculations, the data were first normalized (mean 0 and SD 1), so that the weights with the largest magnitude indicate predictors with the greatest impact on NP prediction. The factors with the greatest impact on prediction of NP impairment were age (weighting 0.33) and current CART duration (weighting −0.16) (Table 2). A positive value indicates that find more a larger value of the component is associated with NP impairment, while a negative value indicates that a lower value is associated with NP impairment. Hence older age and past CNS disease are likely indicators of NP impairment, with positive weightings, while shorter CART duration, lower CD4 cell count and, for this group, shorter HIV duration and lower viral load

are more likely to indicate NP impairment. In terms of the nonnormalized original data, and based on this set of possible components, NP impairment is predicted to occur when the following expression holds: We next assessed NP impairment based on the same set of predictors Sirolimus molecular weight but with log10 HIV RNA replaced by whether current HIV RNA (copies/mL) was above (1) or below (0) the 50 copies/mL detection limit for each individual. Once again, age (weighting 0.36) and current CART duration (weighting −0.28) were the dominant components (Table 2). Also consistent in indicating NP impairment between the two scenarios were past occurrence

of CNS disease and lower current CD4 cell count. The predictor of NP impairment under this scenario, and using the original nonnormalized data values, was given by Both SVM models yielded medium-to-large negative correlations (Spearman r=0.50; P<0.0001) (-)-p-Bromotetramisole Oxalate between the model’s predicted values and the average Z-score, meaning that better predictions of NP-impaired status were associated with greater severity of cognitive deficits. The same models were also tested including self-reported depressive symptoms and CART CPE. Including data on self-reported depressive symptoms for the scenario where log10 HIV RNA was included only yielded an accuracy of 75% for the prediction of impairment and an accuracy of 72% for the prediction of NP nonimpairment. For the scenario where detectable vs. undetectable HIV RNA was included, along with depressive symptoms, the best model achieved an accuracy of 72% for NP impairment and an accuracy of 70% for NP nonimpairment.

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