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, especially in resource-poor settings. Here patients (n = 96) attending Pokdisus AIDS Clinic at the Cipto Mangunkusumo Hospital, Jakarta who had been treated with d4T were screened for symptomatic neuropathy. Clinical, demographic, and genetic factors were considered as possible neuropathy risk factors. DNA from saliva was used to examine alleles of TNFA-308, BAT1 (intron 10), TNFA-1031, IL1A+4845, and IL12B (3' UTR). The prevalence of neuropathy (symptoms and signs) was 34%. On multivariate analysis, neuropathy following d4T exposure was associated with increasing age, increasing height, and TNFA-1031*2 (model p = 0.0009). Isoniazid exposure (present in 56% of patients) was not associated with neuropathy in this cohort, where all patients had received pyridoxine coadministration. These data suggest that a simple algorithm based on patient age, height, and TNF genotype could be used to predict the individual's risk of symptomatic neuropathy prior to prescription of d4T.

译文

:与廉价的核苷类似物逆转录酶抑制剂(NRTIs)[特别是司他夫定(d4T)]暴露有关的毒性感觉神经病会导致艾滋病毒患者的管理陷入困境,尤其是在资源贫乏地区。在这里,对接受过d4T治疗的雅加达Cipto Mangunkusumo医院的Pokdisus艾滋病诊所的患者(n = 96)进行了筛查,以检查是否患有症状性神经病。临床,人口和遗传因素被认为是可能的神经病危险因素。来自唾液的DNA用于检查TNFA-308,BAT1(内含子10),TNFA-1031,IL1A 4845和IL12B(3'UTR)的等位基因。神经病(症状和体征)的患病率为34%。在多变量分析中,d4T暴露后的神经病变与年龄增加,身高增加和TNFA-1031 * 2相关(模型p = 0.0009)。在这个队列中,所有患者均接受吡ido醇联合给药,异烟肼暴露(占56%的患者)与神经病变无关。这些数据表明,基于患者年龄,身高和TNF基因型的简单算法可用于在开处方d4T之前预测个体出现症状性神经病的风险。

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