Three amino acid residues in the envelope of human immunodeficiency virus type 1 CRF07_BC regulate viral neutralization susceptibility to the human monoclonal neutralizing antibody IgG1b12

The CD4 binding site(CD4bs) of envelope glycoprotein(Env) is an important conserved target for anti-human immunodeficiency virus type 1(HIV-1) neutralizing antibodies. Neutralizing monoclonal antibodies IgG1 b12(b12) could recognize conformational epitopes that overlap the CD4 bs of Env. Different virus strains, even derived from the same individual, showed distinct neutralization susceptibility to b12. We examined the key amino acid residues affecting b12 neutralization susceptibility using single genome amplification and pseudovirus neutralization assay. Eleven amino acid residues were identified that affect the sensitivity of Env to b12. Through site-directed mutagenesis, an amino acid substitution at position 182 in the V2 region of Env was confirmed to play a key role in regulating the b12 neutralization susceptibility. The introduction of V182 L to a resistant strain enhanced its sensitivity to b12 more than twofold. Correspondingly, the introduction of L182 V to a sensitive strain reduced its sensitivity to b12 more than tenfold. Amino acid substitution at positions 267 and 346 could both enhance the sensitivity to b12 more than twofold. However, no additive effect was observed when the three site mutageneses were introduced into the same strain, and the sensitivity was equivalent to the single V182 L mutation. CRF07_BC is a major circulating recombinant form of HIV-1 prevalent in China. Our data may provide important information for understanding the molecular mechanism regulating the neutralization susceptibility of CRF07_BC viruses to b12 and may be helpful for a vaccine design targeting the CD4 bs epitopes.

Human T-lymphotropic virus type 1-associated myelopathy/tropical spastic paraparesis: Clinical presentation and pathophysiology

Human T-cell lymphotropic virus type 1(HTLV-1)-associated myelopathy/tropical spastic paraparesis(HAM/TSP) is a slowly progressive neurodegenerative disorder in which lesions of the central nervous system cause progressive weakness, stiffness, and a lower limb spastic paraparesis. In some cases, polymyositis, inclusion bodymyositis, or amyotrophic lateral sclerosis-like syndromes are associated with HTLV-1. TSP was first described in Jamaica in 1888 and known as Jamaican peripheral neuritis before TSP was related to HTLV-1 virus, the first retrovirus being identified, and the disease is since named HAM/TSP. There is no established treatment program for HAM/TSP. Prevention is difficult in lowincome patients(i.e., HTLV-1 infected breast feeding mothers in rural areas, sex workers). Thus, there is a need for new therapeutic avenues. Therapeutic approaches must be based on a better understanding, not only of clinical and clinicopathological data, but also of the pathophysiology of the affection. Consequently, a better understanding of existing or newly developed animal models of HAM/TSP is a prerequisite step in the development of new treatments.

Preliminary study on Herpes simplex virus type 1 infection of human oral epithelial cell in vitro

Objective： To explore the functions and mechanisms of herpes simplex virus type I（HSV-1） while infecting human oral epithelial cells in vitro（being similar to the infection in vivo）. Methods：An abundance of HSV-1 strains amplified in Vero cells were used to infect human oral epithelial cells. The culture supernatant was collected to infect Vero cells again. Morphology of HSV-1 was identified by inverted microscope and transmission electron microscope. Nucleic acid of the virus was detected by PCR. Results：The infected human oral epithelial cells didn＇ t display an obvious cytopathic effect（CPE） under inverted microscope（while Vero cells which were infected by the culture supernatant showed typical（CPE）. The virus particles were not observed in the cytoplasm nor in nucleus of human oral epithelial cells, however under transmission electron microscope in the cytoplasm of Vero cells, the nucleic acid of HSV-1 could be detected in infected human oral epithelial cells, by PCR. Conclusion-HSV-1 can successfully infect human oral epithelial cells. This model may provide a useful approach for studying the pathogenesis of herpes virus-associated periodontal disease.

INTRACELLULAR EXPRESSION OF MULTIMERIZED ANTISENSE TAR-CORE RNAS INHIBIT THE REPLICATION OF HUMAN IMMUNODEFICIENCY VIRUS TYPE 1 IN HUMAN CD_4+T LYMPHOCYTES

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A Human T Lymphotropic Virus Type 1 Carrier Coinfected with <i>Mycobacterium intracellulare</i>and <i>Pneumocystis jirovecii</i>with a Characteristic Compositional Change of Bone Marrow Cells

Human T lymphotropic virus type 1 (HTLV-1) is endemic in the southern part of Japan. Infection of the virus can cause adult T cell leukemia/lymphoma (ATL), while most infected individuals remain in a carrier state for a long period of time. Although rare cases of carriers, like ATL patients, who developed opportunistic infections, have been reported, hematological changes of carriers who are prone to opportunistic infections have not been well defined. Here, we present a case of an HTLV-1 carrier who developed Mycobacterium intracellulare infection and Pneumocystis jirovecii pneumonia (PcP) simultaneously. Flow cytometric analysis of bone marrow cells revealed an aberrant compositional change similar to that in ATL patients. This suggests the presence of a pre-ATL state prior to the development of ATL, which is notable in terms of underlying cellular immunodeficiency.

水芹总酚酸体外抗HIV-1的作用

目的探讨水芹总酚酸体外抑制人类免疫缺陷病毒1型的作用。方法用不同稀释度的水芹总酚酸与TZM-bl细胞共同培养,使用MTT法检测活细胞的数量,观察水芹总酚酸对TZM-bl细胞的毒性作用;用人类免疫缺陷病毒1型实验室适应株SF33、BAL分别感染TZM-bl细胞,基于TZM-bl细胞的荧光素酶检测体系,采用荧光素酶活性检测方法检测水芹总酚酸抗人类免疫缺陷病毒1型的活性。结果水芹总酚酸对TZM-bl细胞表现出较低的细胞毒性,半数细胞毒浓度>1600μg·ml^(-1)。水芹总酚酸对TZM-bl细胞HIV-1 SF33、HIV-1 BAL病毒的半抑制浓度平均值分别为38.93和24.25μg·ml^(-1),治疗指数分别为>41和>66。结论水芹总酚酸在体外具有抑制人类免疫缺陷病毒1型复制活性的作用。

The role of monocyte-lineage cells in human immunodeficiency virus persistence: mechanisms and progress

Human immunodeficiency virus type 1(HIV-1) persistence is a major barrier to the successful treatment and eradication of acquired immunodeficiency syndrome(AIDS).In addition to resting CD4+ T cells,a significant long-lived compartment of HIV-1 infection in vivo includes blood monocytes and tissue macrophages.Studying HIV-1 persistence in monocyte-lineage cells is critical because these cells are important HIV-1 target cells in vivo.Monocyte-lineage cells,including monocytes,dendritic cells(DCs) and macrophages,play a significant role in HIV-1 infection and transmission.These cells have been implicated as viral reservoirs that facilitate HIV-1 latency and persistence.A better understanding of HIV-1 interactions with monocyte-lineage cells can potentially aid in the development of new approaches for intervention.This minireview highlights the latest advances in understanding the role of monocyte-lineage cells in HIV-1 persistence and emphasizes new insights into the mechanisms underlying viral persistence.

Adult T-cell leukemia/lymphoma presenting multiple lymphomatous polyposis

Multiple lymphomatous polyposis (MLP) is an unusual form of non-Hodgkin's lymphoma characterized by polyps throughout the gastrointestinal tract. It has been reported that most MLP are observed in cases with mantle cell lymphoma of B-cell type. We herein present a case of a 66-year-old man with adult T-cell leukemia/lymphoma (ATLL). Colonoscopy revealed MLP throughout the colon and histopathological findings of ATLL cell infiltration. The patient died despite combination of chemotherapy. The literature of manifestations of colonic involvement of ATLL isreviewed and the importance of endoscopic evaluation to differentiate ATLL intestinal lesions from opportunistic infectious enterocolitis is discussed.

A novel mouse model of adult T-cell leukemia cell invasion into the spinal cord

Adult T-cell leukemia( ATL) is a mature T-cell malignancy caused by human T-cell leukemia virus type I infection, and 10%-25% of patients show central nervous system( CNS) involvement. CNS involvement significantly reduces survival and there are no effective treatments for CNS involvement. Therefore, an appropriate animal model is required to evaluate the inhibitory effects of novel drugs on the progression of ATL with CNS involvement. Here, we established a mouse model of ATL with CNS involvement using NOD.Cg-Prkdc~ (scid) Il2 rg ^(tm1Wjl)/SzJ mice inoculated with ATL cells intramuscularly in the postauricular region, and these mice showed paraparesis. Of the 10 mice inoculated with ATL cells intramuscularly(I.M.) at 5 weeks of age, 8(80%) showed paraparesis, whereas none of the 10 mice inoculated with ATL cells subcutaneously(S.C.) showed paraparesis. In the I.M. group, PCR detected HTLV-1-specific genes in the thoracic and lumbar vertebrae; however, in the S.C. group, the vertebrae were negative for HTLV-1 genes. Histological analysis revealed a particularly high incidence of tumors, characterized by accumulation of the injected cells, in the thoracic vertebrae of mice in the I.M. group. Tumor cell infiltration was relatively high in the bone marrow. Spinal cord compression caused by invasion of the tumor mass outside the pia mater was observed in the thoracic vertebrae of the spinal cord. In conclusion, we have reported a mouse model of tumor growth with paraparesis that may be used to assess novel therapeutic agents for ATL with CNS involvement.

BMI-1抑制剂PTC-596对人乳腺癌MCF-7细胞增殖、周期和凋亡的影响

目的 分析BMI-1抑制剂PTC-596对人乳腺癌MCF-7细胞增殖、周期和凋亡的影响。方法以人乳腺癌MCF-7细胞为肿瘤细胞模型,正常培养为阴性对照组,25、50 nmol/L PTC-596处理SGC-7901细胞48 h为低、高药物浓度实验组。利用CCK8法分析细胞增殖能力;流式细胞术分别结合PI单染、DCFHDA探针、JC-1探针以及PI/FITC-Annexin V双染分析细胞周期、活性氧(reactive oxygen species, ROS)累积、线粒体膜电位和凋亡细胞比例;Western blot法检测细胞BIM-1蛋白和周期相关蛋白CyclinD1、CyclinB1、P21以及凋亡相关蛋白Bax、Bcl-2、c-PARP蛋白相对表达水平。结果 与对照组相比,PTC-596高效抑制人乳腺癌MCF-7细胞的增殖,处理48 h后IC_(50)为(49.33±7.02)nmol/L。低、高药物浓度实验组细胞中BMI-1表达显著减少(P <0.01)。实验组细胞中CyclinB1和P21相对表达增加,CyclinD1表达减少,细胞有丝分裂被抑制,出现G_2/M期周期阻滞;同时活性氧累积增多,线粒体膜电位下降,Bax表达上调,Bcl-2表达下调,c-PARP增加,凋亡细胞比例从2.04%显著上升为10.56%、26.74%。与对照组相比较,以上结果差异均有统计学意义(P <0.05)。结论 PTC-596高效杀伤人乳腺癌MCF-7细胞,其机制可能与抑制BMI-1、诱导细胞周期阻滞和内源性线粒体途径细胞凋亡密切相关。

湖南省HIV-1感染者原发性耐药现况调查

目的了解湖南省1型人类免疫缺陷病毒(HIV-1)感染者其基因亚型分布和原发性耐药(PDR)情况,为艾滋病防控及抗病毒治疗(ART)提供参考依据。方法收集湖南省2021年1月—2022年8月某院HIV门诊新确诊并且未接受ART的HIV-1感染者的人口学及流行病学相关数据,采集患者血清,提取核糖核酸,利用In-house的方法采取2轮聚合酶链式反应进行基因扩增,Sanger法对产物进行测序,分析患者临床资料及HIV-1亚型及耐药情况。结果共纳入患者667例,基因型耐药检测失败20例,647例检测成功的新确诊HIV-1感染者纳入研究。53例患者感染的HIV-1株发生PDR,发生率为8.19%,主要集中于男性(88.68%)、未婚(71.70%)、男男性行为(MSM,60.38%)、21~40岁的群体(58.49%),且多为湖南省本地籍居民(98.11%)。共检测出15种HIV-1毒株亚型,主要亚型为CRF_01AE(35.70%)、CRF07_BC(25.19%)、B/C(18.86%)以及CRF55_01B(7.88%)。不同HIV-1亚型患者的PDR发生率比较,差异有统计学意义(χ^(2)=18.62,P=0.017)。蛋白酶抑制剂(PIs)耐药率为0.15%,核苷酸类逆转录酶抑制剂(NRTIs)耐药率为2.78%,非核苷酸类逆转录酶抑制剂(NNRTIs)耐药率为6.65%,整合酶抑制剂(INSTIs)耐药率为0.31%。结论湖南省HIV-1毒株亚型分布复杂,PDR发生率已超过世界卫生组织制定的低水平耐药预警线(<5%),应加大感染预防与控制力度,阻断耐药毒株传播。

Full-length clone and characterization of a human immunodeficiency virus type 1 subtype B' isolated from Hubei Province,China

There are two types of Human Immunodeficiency Virus （HIV）： HIV-1 and HIV-2. HIV-1 dominates epidemics in many different parts of the world, and HIV-2 is principally responsible for the epidemic in westem Africa. In China, Zeng et al have reported the first individual infected with HIV-1 in 1985. And in the 1990s, there was a severe epidemic involving the HIV-1 B＇ strain among people who sold blood and plasma in Henan, Hubei and adjacent provinces. To further study in HIV/AIDS vaccines and HIV-1 drug resistance for people in these regions, we need to construct an infectious HIV-1 B＇ molecular clone which is representative of the virus in these areas. To this end, we have isolated a HIV-1 B＇ virus from a child who was infected with HIV-1 from his mother in Hubei province, and have constructed a full-length clone from this genome.

Scores of amino acid 0D-3D information as applied in cleavage site prediction and better specificity elucidation for human immunodeficiency virus type 1 protease

A new set of descriptors,namely score vectors of the zero dimension,one dimension,two dimensions and three dimensions(SZOTT),was derived from principle component analysis of a matrix of 1369 structural variables including 0D,1D,2D and 3D information for the 20 coded amino acids. SZOTT scales were then used in cleavage site prediction of human immunodeficiency virus type 1 protease. Linear discriminant analysis(LDA) and support vector machines(SVM) were applied to developing models to predict the cleavage sites. The results obtained by linear discriminant analysis(LDA) and support vector machines(SVM) are as follows. The Matthews correlation coefficients(MCC) by the resubstitution test,leave-one-out cross validation(LOOCV) and external validation are 0.879 and 0.911,0.849 and 0.901,0.822 and 0.846,respectively. The receiver operating characteristic(ROC) analysis showed that the SVM model possesses better simulative and predictive ability in comparison with the LDA model. Satisfactory results show that SZOTT descriptors can be further used to predict cleavage sites of human immunodeficiency virus type 1 protease.

福建省HIV-1流行毒株基因分型与流行特征分析

目的了解HIV-1流行株在福建省感染人群中的基因亚型分布及流行特征。方法随机抽取福建省2003-2005年发现的70例HIV感染者血样,提取前病毒DNA进行体外扩增,获得核心蛋白(gag)、包膜蛋白(env)及pol区基因的核酸片段,并对各基因区核苷酸序列进行测定和序列分析。结果选取46份流行病学资料以及不同基因区域序列资料完整的样本进入亚型分析,结果显示目标人群中存在B、C2种亚型以及CRF07-BC、CRF08-BC、CRF01-AE3种流行重组型,以及国内未见报道的B/F重组毒株、A1/D重组毒株等,其中以CRF01-AE重组毒株为主,占69.56%。基因亚型的流行特征分析显示,本省感染的HIV患者中以CRF01-AE重组型占多数,可能的新型重组型全部分布于境外感染者中;在性接触传播的感染者(71.74%)中呈现多种亚型分布的特征;随着时间变化福建省HIV感染者的亚型分布发生变化。结论福建省HIV-1亚型分布众多,各亚型在不同感染地分布不平衡,性乱人群中的亚型分布较为复杂,从总的亚型流行特征来看,HIV-1在我省有流行加快的趋势。

Identification of Aristolactam Derivatives That Act as Inhibitors of Human Immunodeficiency Virus Type 1 Infection and Replication by Targeting Tat-Mediated Viral Transcription

Despite the success of antiretroviral therapy(ART),efforts to develop new classes of antiviral agents have been hampered by the emergence of drug resistance.Dibenzo-indole-bearing aristolactams are compounds that have been isolated from various plants species and which show several clinically relevant effects,including anti-inflammatory,antiplatelet,and antimycobacterial actions.However,the effect of these compounds on human immunodeficiency virus type 1(HIV-1)infection has not yet been studied.In this study,we discovered an aristolactam derivative bearing dibenzo[cd,f]indol-4(5 H)-one that had a potent anti-HIV-1 effect.A structure-activity relationship(SAR)study using nine synthetic derivatives of aristolactam identified the differing effects of residue substitutions on the inhibition of HIV-1 infection and cell viability.Among the compounds tested,1,2,8,9-tetramethoxy-5-(2-(piperidin-1-yl)ethyl)-dibenzo[cd,f]indol-4(5 H)-one(Compound 2)exhibited the most potent activity by inhibiting HIV-1 infection with a half-maximal inhibitory concentration(IC50)of 1.03 lmol/L and a half-maximal cytotoxic concentration(CC50)of 16.91 lmol/L(selectivity index,16.45).The inhibitory effect of the compounds on HIV-1 infection was linked to inhibition of the viral replication cycle.Mode-of-action studies showed that the aristolactam derivatives did not affect reverse transcription or integration;instead,they specifically inhibited Tat-mediated viral transcription.Taken together,these findings show that several aristolactam derivatives impaired HIV-1 infection by inhibiting the activity of Tat-mediated viral transcription,and suggest that these derivatives could be antiviral drug candidates.

人参皂苷Rg3体外抗HSV-1活性与免疫调节效应

目的：研究人参皂苷Rg3体外对单纯疱疹病毒1型（HSV-1）的抑制作用与免疫调节效应。方法：采用结晶紫染色法观察Rg3对HSV-1致细胞病变效应的抑制作用。用MTT比色法检测Rg3对Vero细胞和小鼠脾细胞增殖的影响。以Rg3诱导小鼠脾细胞，用鼠脾T淋巴母细胞增殖分析法测定上清中IL-2活性，细胞病变抑制法测定IFN-γ活性。结果：浓度在1．56～25mg·L^-1的Rg3对HSV-1致细胞病变效应抑制作用显著高于病毒对照组（P〈0．05）；浓度小于25mg·L^-1的Rg3对传代Vero细胞及小鼠脾细胞的增殖作用与细胞对照组比较差异无显著性（P〉0．05）；3．13～6．25mg·L^-1的Rg3体外诱生IL-2和IFN-γ分泌水平显著高于对照组（P〈0．05）。结论：一定浓度的Rg3具有体外抗HSV-1活性，对传代Vero细胞及小鼠脾细胞无毒性，可显著促进IL-2和IFN-γ分泌，参与免疫调节效应。

深圳市HIV-1毒株的流行状况

目的了解深圳地区人类免疫缺陷病毒1型(HIV-1)毒株亚型及流行情况,分析其传染来源和传播规律。方法应用巢式聚合酶链反应技术,对122例在深圳市发现的HIV-1感染者外周血单个核细胞中的env基因和gag基因进行扩增,并对各基因区核苷酸序列进行测定和分析。结果122份样本中共存在CRF01_AE、CRF08_BC、CRF07_BC3种重组毒株以及B'、B、C3种亚型,其在所有分析样本中的比例分别为45.1%(55/122)、31.1%(38/122)、6.6%(8/122)、14.8%(18/122)、1.6%(2/122)和0.8%(1/122)。CRF01_AE、CRF08_BC、CRF07_BC、B和B'亚型间的组内离散率分别为(4.455±1.478)%、(2.997±1.345)%、(4.380±2.024)%、(5.186±2.487)%和(4.869±2.638)%,与部分国内和国际参考株01AE.TH.90.CM240、97CNGX-9F、CN.97.C54A、B.US.83.JRFL、RL42核苷酸序列间的离散率分别为(5.228±0.823)%、(3.634±1.073)%、(4.233±1.119)%、(4.950±2.564)%、(5.795±2.198)%。CRF07_BC和CRF08_BC亚型以吸毒人群为主,CRF01_AE重组亚型以性途径和吸毒人群为主,B和B'亚型主要分布在静脉吸毒、性传播和献/输血人群。结论深圳地区有3种亚型和3种重组亚型HIV-1毒株流行,CRF01_AE、CRF08_BC重组亚型和B'亚型为主要流行毒株,CRF01_AE是性传播人群中的主要流行毒株,CRF08_BC和CRF01_AE是静脉吸毒人群中的主要流行毒株。

128例经血感染HIV患者合并HCV和HBV感染状况

目的了解经血感染人类免疫缺陷病毒1型(HIV-1)患者合并感染乙型肝炎病毒(HBV)及丙型肝炎病毒(HCV)的情况及发病特点。方法回顾性分析128例经血感染HIV患者合并感染HBV和HCV的感染率、肝脏表现及部分免疫学特征。结果128例患者中,单纯合并HCV感染者107例(83.6%),其中40例(31.3%)出现肝功能异常或肝损害,15例(11.7%)合并肝炎症状;单纯合并HBV感染3例(2.3%),均出现肝功能异常和肝炎症状;HIV、HBV、HCV三重感染7例(5.5%),无1例存在肝功能异常和肝炎症状;11例(8.6%)患者未合并HBV或HCV。结论经血感染HIV的患者与HCV的合并感染率高于与HBV的合并感染率,HIV合并HCV感染与HBV感染的临床转归也存在差异。

应用异源双链泳动分析法快速确定(HIV-1)基因亚型

应用异源双链泳动分析法（Ｈｅｔｅｒｏｕｄｕｐｌｅｘ ｍｏｂｉｌｉｔｙ ａｓｓａｙ，ＨＭＡ） ，对来自我国云南、四川、新疆、浙江、广东、福建、天津７ 省市７３ 份ＨＩＶ 感染者样品，进行了ＨＩＶ－ １ 膜蛋白（ｅｎｖ） 基因片段亚型分析。通过ＨＭＡ 能确定亚型的有７０ 份，占样品总数的９５－８９ ％ （７０／７３） 。其中Ａ 亚型２－８６ ％ （２／７０） ，Ｆ亚型２ ．８６ ％ （２／７０） ，泰国Ｂ 亚型１８ ．５８ ％ （１３／７０） ，欧美Ｂ 亚型８ ．５６ ％ （６／７０） ，Ｃ亚型３８ ．５７ ％ （２７／７０） ，Ｅ亚型２８－５７ ％ （２０／７０） 。为了检验结果的准确性和探讨３ 份样品不能用ＨＭＡ分型的原因，进一步对样品进行序列测定和系统树分析，并将两者结果的相互比较，两者对ＨＩＶ－ １ 分型显示出高度的一致性，其亚型一致率达９５－８９ ％ （７０／７３） 。而３ 份样品不能确定亚型的原因主要是，其ｅｎｖ 基因区段与相应的参考亚型质粒毒株相比变异太大。这提示，为了提高ＨＭＡ分型的敏感性，应不断地选择代表性好的毒株构建参考亚型质粒。

我国HIV-1 B'/C重组流行株Tat蛋白的表达、纯化及功能分析

根据全国HIV分子流行病学研究发现,B'和C亚型HIV-1在我国发生了重组,并以优势株形式在我国广泛流行。为了探讨这种HIV-1B'/C重组毒株tat基因的变异与其表型之间的关系,利用pET表达系统在大肠杆菌中高效表达了三种不同基因变异类型的Tat蛋白,重组蛋白占菌体总蛋白的26%,Westernblot显示较好的反应原性,并通过金属鏊合层析纯化了目的蛋白。荧光素酶活性检测表明:体外表达的Tat蛋白具有明显的生物学活性,可以反式激活HIVLTR引导的报告基因的表达;三种Tat蛋白在激活活性上的差异与流行现场检测的病毒载量的高低存在明显的对应关系,说明tat基因的变异可以引起病毒生物学特性的改变,进而影响病毒的流行特征。此结果为进一步研究我国HIV重组毒株的基因变异特征及变异规律奠定了基础。