Hepatitis a vaccine immunogenicity and boostability in adults receiving immunosuppressive therapy and adults living with HIV: a prospective single-Centre cohort study.

IF 9.1 2区 医学 Q1 INFECTIOUS DISEASES
Jenny L Schnyder,Hannah M Garcia Garrido,Michael W Tanck,Irma Maurer,Agnes M Harskamp,Neeltje Kootstra,Martin P Grobusch,Abraham Goorhuis
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Abstract

INTRODUCTION Hepatitis A (hepA) vaccination is highly immunogenic in healthy individuals, however there is uncertainty about the immunogenicity in immunocompromised populations (ICPs). METHODS In this prospective cohort study, people living with HIV (PLWH), patients on immunosuppressive mono- and combination therapy, and controls received two hepA vaccine doses at months 0 and 6-12, or three combined hepA/B vaccine doses at months 0, 1 and 6-12. Antibody levels were measured before and at different time-points post-vaccination (T2, 6, 8, 12 months). The primary endpoint was the seroconversion rate (SCR) at T8, defined as hepA antibodies ≥20 mIU/ml. To assess boostability, an additional vaccine dose was administered 1-5 years after T12 in those with antibodies < 50 mIU/ml, with antibody measurements before and seven days after the booster dose. RESULTS We included 150 participants. At T2 SCRs ranged between 35-58% in ICPs versus 94% in controls. Among PLWH, patients on monotherapy, combination therapy and controls SCRs at T8 were 33/34 (97%), 32/34 (94%), 25/30 (83%) and 28/28 (100%) respectively. The booster dose resulted in 71% additional seroconversion (17/24), with only patients using combination therapy not responding. CONCLUSIONS HepA vaccination is highly immunogenic in virologically suppressed PLWH and patients on immunosuppressive monotherapy, with SCRs after the complete hepA vaccination schedule similar to controls and adequate booster responses in case of waning immunity. However, patients using immunosuppressive combination therapy as well as all ICPs who did not receive the complete hepA vaccination schedule, are at risk of non-response to vaccination and post-vaccination antibody measurements are recommended.
接受免疫抑制治疗的成人和感染艾滋病毒的成人接种甲型肝炎疫苗的免疫原性和增强性:一项前瞻性单中心队列研究。
在这项前瞻性队列研究中,艾滋病病毒感染者(PLWH)、接受免疫抑制单一疗法和联合疗法的患者以及对照组分别在第 0 个月和第 6-12 个月接种了两剂甲肝疫苗,或在第 0 个月、第 1 个月和第 6-12 个月接种了三剂甲肝/乙肝联合疫苗。在接种前和接种后的不同时间点(T2、6、8、12 个月)测量抗体水平。主要终点是T8时的血清转换率(SCR),定义为hepA抗体≥20 mIU/ml。为了评估增强性,在抗体<50 mIU/ml的人群中,在T12后1-5年再接种一剂疫苗,并在接种前和接种后7天测量抗体。在 T2 阶段,ICP 的 SCR 为 35% 至 58%,而对照组的 SCR 为 94%。在 PLWH 中,接受单一疗法、联合疗法和对照疗法的患者在 T8 的 SCR 分别为 33/34 (97%)、32/34 (94%)、25/30 (83%) 和 28/28 (100%)。结论在病毒学抑制的 PLWH 和接受免疫抑制单药治疗的患者中,接种 HepA 疫苗具有很高的免疫原性,完整的 HepA 疫苗接种程序后的 SCR 与对照组相似,并且在免疫力下降时有足够的加强应答。但是,使用免疫抑制剂联合疗法的患者以及所有未按计划接种完整乙肝疫苗的 ICPs 都有可能对疫苗接种无反应,因此建议进行接种后抗体测定。
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来源期刊
Journal of travel medicine
Journal of travel medicine 医学-医学:内科
CiteScore
20.90
自引率
5.10%
发文量
143
审稿时长
6-12 weeks
期刊介绍: The Journal of Travel Medicine is a publication that focuses on travel medicine and its intersection with other disciplines. It publishes cutting-edge research, consensus papers, policy papers, and expert reviews. The journal is affiliated with the Asia Pacific Travel Health Society. The journal's main areas of interest include the prevention and management of travel-associated infections, non-communicable diseases, vaccines, malaria prevention and treatment, multi-drug resistant pathogens, and surveillance on all individuals crossing international borders. The Journal of Travel Medicine is indexed in multiple major indexing services, including Adis International Ltd., CABI, EBSCOhost, Elsevier BV, Gale, Journal Watch Infectious Diseases (Online), MetaPress, National Library of Medicine, OCLC, Ovid, ProQuest, Thomson Reuters, and the U.S. National Library of Medicine.
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