印度首例报道HIV-1C亚型相关的“肌萎缩侧索硬化症(ALS)”样疾病

A patient of ALS like disorder in an HIV 1 clade C infected heterosexual m ale is being reported. A 37 year old gentleman presented with subacute, progre ssive asymmetrical onset of weakness and wasting of upper limbs associated with brisk muscle stretch reflexes and without any sensory or sphincter involvement. While nerve conduction tests were normal, the EMG of proximal and distal limb mu scles on both sides revealed evidence of denervation and reinnervation. Routine blood and urine tests and investigations for underlying causes of motor neuron d isease were noncontributory. He was HIV 1, subtype clade C seropositive. A diag nosis of HIV related anterior horn cell disease was considered and zidovudine, lamivudine and nevirapine were started. After 1 month, there was a subjective im provement of 10%and objective improvement in strength of muscles of proximal up per limb on both sides by one grade power on MRC scale. Reports of amyotrophic l ateral sclerosis (ALS) like illness in HIV are sparse. The reversibility of “A LS” like features in this subgroup of patients might offer an insight into the pathogenesis of amyotrophic lateral sclerosis. This is a first report of ALS l ike illness caused by subtype C of HIV 1 strain.

HIV-1C亚型DNA疫苗诱导小鼠免疫反应的研究

构建含中国流行株HIV-1 C亚型核心蛋白gag基因的重组质粒pVAX-gag,并在体外进行了表达与鉴定.同时构建了含此gag基因的原核表达质粒pGEX-gag,表达纯化并鉴定重组蛋白Gag.以质粒pVAX-gag免疫Balb/C小鼠后,用ELISpot和流式细胞仪检测其细胞免疫反应.再以纯化后的重组蛋白Gag作为包被抗原,用ELISA检测其体液免疫反应.结果显示重组质粒pVAX-gag免疫小鼠后可有效地诱导机体产生细胞免疫和体液免疫反应,且免疫剂量和免疫效果存在一定的正相关性.重组原核表达质粒pGEX-gag的表达产物能与抗p24单克隆抗体发生特异性反应,可用于抗HIV抗体检测.

HIV-1C亚型nef基因构建的DNA质粒诱导小鼠免疫反应的研究

目的构建表达中国流行株HIV-1C亚型调控nef基因的重组质粒pVAX-nef,并免疫BALB/c小鼠,观察其免疫效果,为探索新型HIV DNA疫苗提供数据。方法利用分子生物学技术,将nef基因克隆到pVAX,并在体外进行表达与鉴定。以纯化的Nef蛋白作为包被抗原,用ELISA检测其体液免疫反应,用ELISPOT检测其细胞免疫反应。结果重组质粒pVAX-nef成功构建。接种小鼠后2周,ELISPOT结果显示产生了针对HIV特异的CD4和CD8细胞抗原表位的免疫应答,且与免疫剂量存在一定的正相关性。ELISA实验诱导产生了抗HIV-1特异性抗体,其中40μg免疫组诱导的抗体水平最高。结论重组质粒pVAX-nef免疫小鼠后可有效地诱导机体产生细胞免疫和体液免疫反应。

Global Transmission of Human Immunodeficiency Virus 1 Subtype C and Its Impact on the Circulation of B/C Recombination Strains in China

This study aimed to reconstruct the origin and worldwide epidemic history of human immunodeficiency virus(HIV)1 subtype C and comprehend how HIV-1 subtype C was introduced into and spread throughout China in the formof B/C recombinant strains.Envelope sequences ofHIV-1 subtype C and some other subtypes deposited before December 31,2020 were downloaded from the Los Alamos HIV Database and the Chinese National Center for AIDS/STD Control and Prevention Database.The available sequences were screened for quality,and Bayesian analysis was used to build the maximum clade credibility evolutionary tree to analyze and judge the origin and spread of HIV-1 subtype C.HIV-1 subtype C originated in central Africa around 1952,then spread to southern Africa around 1969 and to eastern Africa around 1973.HIV-1 subtype C fromsouthern Africa was introduced into India in 1977.HIV-1 subtype C of eastern Africa was introduced into Brazil in 1987.Indian HIV-1 subtype C was exported to China in three migration events during the period from 1986 to 1989.The two predominant recombinants in China(CRF07_BC and CRF08_BC)emerged in 1988 and 1990,respectively.Other B/C recombinants,namely,CRF64_BC,CRF61_BC and CRF62_BC,originated in 1993,2002 and 2000,respectively.Our study has reconstructed the global origin and evolutionary history of HIV-1 subtype C.In addition,our study demonstrated that the Chinese HIV-1 subtype C originated from three related Indian lineages around the mid to late 1980s and,since then,has formed some B/C recombinants with subtype B that caused a widespread epidemic in China.