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HIV 阳性患者对 D 亚属腺病毒感染的体液免疫反应受损。

Impaired humoral responses to subgenus D adenovirusenovirus infections in HIV-positive patients.

作者信息

Lord A, Bailey A S, Klapper P E, Snowden N, Khoo S H

机构信息

Clinical Virology, Manchester Royal Infirmary, Manchester, United Kingdom.

出版信息

J Med Virol. 2000 Dec;62(4):405-9.

Abstract

HIV-positive patients are at increased risk of developing adenovirus infection, particularly of the gastrointestinal tract and with unusual subgenus D strains. To investigate humoral immunity to these strains of adenoviruses, the humoral immune response was examined in longitudinal samples of serum against isolates collected from a prospective study of HIV-positive patients with subgenus D adenovirus infection. Of 10 HIV-positive patients developing adenovirus infection, 3 had chronic infection (8->27 months) with one serotype, 3 had chronic infection (>/=10 months) with changing serotypes and 4 had acute and self-limiting adenovirus infection (<1 month). Fifty-one sera were tested, and samples collected before adenovirus infection were available in 8 patients. Neutralising assays were performed against the patient's own isolate (adenoviruses 9, 17, 19, 19/23, 19/37, 23, 26, 23/26, 43 and 46) and common circulating strains of adenovirus 1-5. Indirect immunofluorescence tests were carried out against the autologous isolate and complement-fixation tests were undertaken using a standard assay. Immunofluorescence test antibodies were detected (titre >/=160) in all patients, and present to high titre (>/=320) in 8/10 patients. Complement-fixing antibodies were not detected in significant titre. Of particular note, there was no significant neutralising antibody response to the patient's own isolate after acute infection. Neutralising antibody to adenovirus 3 (titre 20) was transiently detected in two patients. In the remaining patients neutralising antibody directed against adenoviruses 1-5 was not detected. Persistent carriage of subgenus D adenoviruses in HIV-positive patients is probably the result of failure of cell-mediated immune responses to clear primary infection. Nevertheless, there is marked impairment of B cell responses resulting in poor neutralising and complement-fixing antibody production even though immunofluorescence test determined antibodies are produced in high titre. These possibly reflect impairment of effective B cell priming mechanisms within the germinal centres of lymph nodes, or the polyclonal activation of B cells driven by HIV infection.

摘要

HIV阳性患者发生腺病毒感染的风险增加,尤其是胃肠道感染,且感染的多为不常见的D亚属毒株。为研究针对这些腺病毒毒株的体液免疫,我们在一项针对感染D亚属腺病毒的HIV阳性患者的前瞻性研究中,检测了血清纵向样本中针对所分离毒株的体液免疫反应。在10例发生腺病毒感染的HIV阳性患者中,3例为单一血清型的慢性感染(8至27个月),3例为血清型变化的慢性感染(≥10个月),4例为急性自限性腺病毒感染(<1个月)。共检测了51份血清,8例患者有腺病毒感染前采集的样本。针对患者自身分离株(腺病毒9型、17型、19型、19/23型、19/37型、23型、26型、23/26型、43型和46型)以及腺病毒1至5型的常见流行毒株进行了中和试验。针对自体分离株进行了间接免疫荧光试验,并采用标准方法进行补体结合试验。所有患者均检测到免疫荧光试验抗体(滴度≥160),8/10的患者抗体滴度较高(≥320)。未检测到显著滴度的补体结合抗体。特别值得注意的是,急性感染后,患者对自身分离株未产生显著的中和抗体反应。两名患者短暂检测到针对腺病毒3型的中和抗体(滴度为20)。其余患者未检测到针对腺病毒1至5型的中和抗体。HIV阳性患者持续携带D亚属腺病毒可能是细胞介导的免疫反应无法清除原发感染的结果。然而,B细胞反应明显受损,导致中和抗体和补体结合抗体产生不佳,尽管免疫荧光试验确定抗体产生的滴度较高。这些可能反映了淋巴结生发中心内有效的B细胞启动机制受损,或者是HIV感染驱动的B细胞多克隆激活。

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