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Zofiówka sanatorium

机译:Zofiówka疗养院

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Objectives: To characterize HIV/hepatitis B virus (HBV) coinfection in the AIDS Clinical Trials Group Longitudinal Linked Randomized Trials cohort and compare long-term HBV outcomes between regimens with 1 (MONO) or 2 (DUAL) anti-HBV agents. Design: A retrospective study of coinfected AIDS Clinical Trials Group Longitudinal Linked Randomized Trials subjects who received regimens containing anti-HBV agent(s). Methods: Stored samples at baseline and weeks 16, 32, 48, 144, and 240 were tested for HBV DNA, HBV e antigen (HBeAg), HBV e antibody (HBeAb), and hepatitis D virus (HDV) antibody. Resistance and genotype were tested in samples with HBV DNA >600 IU/mL. MONO versus DUAL analyses were limited to HBV treatment-naive subjects (Naive-MONO, Naive-DUAL). Results: Of 150 study subjects, median age was 40 years, 96% were male; 57% white, 26% black, 13% Hispanic. Baseline median CD4 was 224 cells per cubic millimeter, HIV RNA 4.48 log10 copies/mL, HBV DNA 6.30 log10 IU/mL; 59% HBeAg positive and 65% HBeAb negative; HBV genotypes A = 69%, G = 18%, D = 7%, <2% for A/G, B, C, F, H. Coinfection with HDV was 2%. There were 49 Naive-MONO (lamivudine) and 22 Naive-DUAL (11 lamivudine + tenofovir, 11 emtricitabine + tenofovir) with detectable HBV DNA. In the 240-week follow-up, HBV DNA suppression was not significantly higher in Naive-DUAL (P = 0.14); lower baseline HBV DNA (P < 0.01) was associated with suppression. Among 32 Naive-MONO subjects with detectable HBV DNA at baseline and results at week 48, 41% suppressed; among such 15 Naive-DUAL subjects, 53% suppressed. HBeAg and HBeAb analyses showed similar trends. Conclusions: While consistent trends toward increased HBV DNA suppression, HBeAg loss and HBeAb seroconversion were observed in Naive-DUAL compared with Naive-MONO, they were not statistically significant. Overall, HDV coinfection was low.
机译:目的:在艾滋病临床试验组纵向关联随机试验队列中表征HIV /乙型肝炎病毒(HBV)合并感染的特征,并比较使用1种(MONO)或2种(DUAL)抗HBV药物治疗的长期HBV结果。设计:一项回顾性研究,涉及接受抗乙肝病毒药物治疗的合并感染艾滋病临床试验组纵向相关性随机试验受试者。方法:在基线和第16、32、48、144和240周时对存储的样品进行HBV DNA,HBV e抗原(HBeAg),HBV e抗体(HBeAb)和D型肝炎病毒(HDV)抗体测试。在HBV DNA> 600 IU / mL的样品中测试了耐药性和基因型。 MONO与DUAL分析仅限于未经HBV治疗的受试者(Naive-MONO,Naive-DUAL)。结果:在150名研究对象中,中位年龄为40岁,其中96%为男性; 57%白色,26%黑色,13%西班牙裔。基线中值CD4为224个细胞/立方毫米,HIV RNA 4.48 log10拷贝/ mL,HBV DNA 6.30 log10 IU / mL; HBeAg阳性59%,HBeAb阴性65%; HBV基因型A = 69%,G = 18%,D = 7%,A / G,B,C,F,H <2%。HDV的合并感染率为2%。有49份可检测到的HBV DNA的Naive-MONO(拉米夫定)和22份Naive-DUAL(11个拉米夫定+替诺福韦,11个恩曲他滨+替诺福韦)。在为期240周的随访中,朴素-DUAL对HBV DNA的抑制作用没有显着提高(P = 0.14)。较低的基线HBV DNA(P <0.01)与抑制相关。在基线时具有可检测的HBV DNA的32位天真-MONO受试者中,在第48周的结果中,有41%被抑制;在这15位天真的DUAL受试者中,有53%被抑制。 HBeAg和HBeAb分析显示出相似的趋势。结论:与Naive-MONO相比,在Naive-DUAL中观察到了一致的趋势,即HBV DNA抑制增加,HBeAg丢失和HBeAb血清转化的趋势一致,但在统计学上无统计学意义。总体而言,HDV合并感染率较低。

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