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接种 Duffy 结合蛋白可抑制人体疟疾感染期间寄生虫的生长。

Vaccination with Duffy-binding protein inhibits parasite growth during controlled human malaria infection.

机构信息

Department of Biochemistry, University of Oxford, Oxford OX1 3QU, UK.

Jenner Institute, University of Oxford, Oxford OX3 7DQ, UK.

出版信息

Sci Transl Med. 2023 Jul 12;15(704):eadf1782. doi: 10.1126/scitranslmed.adf1782.

Abstract

There are no licensed vaccines against . We conducted two phase 1/2a clinical trials to assess two vaccines targeting Duffy-binding protein region II (PvDBPII). Recombinant viral vaccines using chimpanzee adenovirus 63 (ChAd63) and modified vaccinia virus Ankara (MVA) vectors as well as a protein and adjuvant formulation (PvDBPII/Matrix-M) were tested in both a standard and a delayed dosing regimen. Volunteers underwent controlled human malaria infection (CHMI) after their last vaccination, alongside unvaccinated controls. Efficacy was assessed by comparisons of parasite multiplication rates in the blood. PvDBPII/Matrix-M, given in a delayed dosing regimen, elicited the highest antibody responses and reduced the mean parasite multiplication rate after CHMI by 51% ( = 6) compared with unvaccinated controls ( = 13), whereas no other vaccine or regimen affected parasite growth. Both viral-vectored and protein vaccines were well tolerated and elicited expected, short-lived adverse events. Together, these results support further clinical evaluation of the PvDBPII/Matrix-M vaccine.

摘要

目前尚无针对 的许可疫苗。我们开展了两项 1/2a 期临床试验,以评估两种针对 结合蛋白区域 II (PvDBPII) 的疫苗。使用黑猩猩腺病毒 63 (ChAd63) 和改良安卡拉痘苗病毒 (MVA) 载体的重组病毒疫苗以及一种蛋白和佐剂制剂 (PvDBPII/Matrix-M) 在标准和延迟给药方案中进行了测试。志愿者在最后一次接种疫苗后接受了受控的人体疟疾感染 (CHMI),同时还有未接种疫苗的对照组。通过比较血液中的寄生虫繁殖率来评估疫苗的疗效。与未接种疫苗的对照组相比( = 13),在延迟给药方案中使用的 PvDBPII/Matrix-M 疫苗产生了最高的抗体反应,并将 CHMI 后寄生虫繁殖率的平均降低了 51%( = 6),而其他疫苗或方案则没有影响寄生虫的生长。两种病毒载体疫苗和蛋白疫苗均耐受良好,并产生了预期的、短暂的不良反应。总之,这些结果支持进一步评估 PvDBPII/Matrix-M 疫苗的临床效果。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3c8e/7615121/16d6633ad70e/EMS188109-f001.jpg

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