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对疟原虫红细胞内期的免疫

Immunity to erythrocytic stages of malarial parasites.

作者信息

Long C A, Daly T M, Kima P, Srivastava I

机构信息

Department of Microbiology and Immunology, Hahnemann University, Philadelphia, Pennsylvania.

出版信息

Am J Trop Med Hyg. 1994;50(4 Suppl):27-32. doi: 10.4269/ajtmh.1994.50.27.

DOI:10.4269/ajtmh.1994.50.27
PMID:7909653
Abstract

In those individuals who live in endemic areas, immunity to malaria is slow to develop and stage-specific. The nature and antigenic specificity of this response, which may involve components of both cell-mediated and humoral immunity, is not well understood. Rodent models provide useful systems to explore the spectrum of host responses that may contribute to resolution of erythrocytic-stage infection or possibly to pathogenesis. Moreover, these models allow identification of plasmodial molecules that can induce different types of host responses. Two different mouse model systems, Plasmodium yoelii yoelii and P. chabaudi adami are presented. These have been selected because resolution of infection by P. yoelii yoelii has been shown to require B cell-dependent mechanisms, while control of acute P. chabaudi adami infection can be achieved by T cell-dependent mechanisms. A monoclonal antibody that provides passive protection to P. yoelii challenge infection has been shown to recognize the cysteine-rich, carboxyl-terminal region of the merozoite surface protein-1. This region, obtained in an appropriate configuration from recombinant Escherichia coli, can induce significant protective immune responses in naive mice. In contrast, cell-mediated immune mechanisms make a major contribution to resolution of asexual-stage P. chabaudi adami infection. An empirical approach using continuous flow electrophoresis has identified several low molecular weight plasmodial proteins that can induce partial protective responses in susceptible hosts. These observations are briefly discussed with respect to human malaria.

摘要

在生活在疟疾流行地区的人群中,对疟疾的免疫力发展缓慢且具有阶段特异性。这种反应的性质和抗原特异性,可能涉及细胞介导免疫和体液免疫的成分,目前还不太清楚。啮齿动物模型为探索可能有助于解决红细胞期感染或可能导致发病机制的宿主反应谱提供了有用的系统。此外,这些模型还能识别可诱导不同类型宿主反应的疟原虫分子。本文介绍了两种不同的小鼠模型系统,约氏疟原虫约氏亚种和查巴迪疟原虫。之所以选择它们,是因为已证明约氏疟原虫约氏亚种感染的解决需要B细胞依赖机制,而查巴迪疟原虫急性感染的控制可通过T细胞依赖机制实现。一种对约氏疟原虫攻击感染提供被动保护的单克隆抗体已被证明能识别裂殖子表面蛋白-1富含半胱氨酸的羧基末端区域。从重组大肠杆菌中以适当构型获得的该区域,可在未感染的小鼠中诱导显著的保护性免疫反应。相比之下,细胞介导的免疫机制对查巴迪疟原虫无性期感染的解决起主要作用。一种使用连续流动电泳的经验方法已鉴定出几种低分子量的疟原虫蛋白,它们可在易感宿主中诱导部分保护性反应。本文就这些观察结果与人类疟疾相关问题进行了简要讨论。

相似文献

1
Immunity to erythrocytic stages of malarial parasites.对疟原虫红细胞内期的免疫
Am J Trop Med Hyg. 1994;50(4 Suppl):27-32. doi: 10.4269/ajtmh.1994.50.27.
2
CD4+ T cells acting independently of antibody contribute to protective immunity to Plasmodium chabaudi infection after apical membrane antigen 1 immunization.在顶膜抗原1免疫后,独立于抗体发挥作用的CD4 + T细胞有助于对查巴迪疟原虫感染产生保护性免疫。
J Immunol. 2000 Jul 1;165(1):389-96. doi: 10.4049/jimmunol.165.1.389.
3
Humoral response to a carboxyl-terminal region of the merozoite surface protein-1 plays a predominant role in controlling blood-stage infection in rodent malaria.对裂殖子表面蛋白-1羧基末端区域的体液反应在控制啮齿类动物疟疾的血液阶段感染中起主要作用。
J Immunol. 1995 Jul 1;155(1):236-43.
4
Plasmodium: immunization with carboxyl-terminal regions of MSP-1 protects against homologous but not heterologous blood-stage parasite challenge.疟原虫:用裂殖子表面蛋白-1(MSP-1)的羧基末端区域进行免疫可抵御同源但不能抵御异源血期寄生虫攻击。
Exp Parasitol. 1999 Jan;91(1):78-85. doi: 10.1006/expr.1999.4357.
5
Merozoite surface protein 4/5 provides protection against lethal challenge with a heterologous malaria parasite strain.裂殖子表面蛋白4/5可提供针对异源疟原虫菌株致死性攻击的保护作用。
Infect Immun. 2004 Oct;72(10):5840-9. doi: 10.1128/IAI.72.10.5840-5849.2004.
6
Complete protective immunity induced in mice by immunization with the 19-kilodalton carboxyl-terminal fragment of the merozoite surface protein-1 (MSP1[19]) of Plasmodium yoelii expressed in Saccharomyces cerevisiae: correlation of protection with antigen-specific antibody titer, but not with effector CD4+ T cells.用在酿酒酵母中表达的约氏疟原虫裂殖子表面蛋白-1(MSP1[19])的19千道尔顿羧基末端片段免疫小鼠诱导产生的完全保护性免疫:保护作用与抗原特异性抗体滴度相关,但与效应性CD4+T细胞无关。
J Immunol. 1997 Oct 1;159(7):3400-11.
7
A bicistronic DNA vaccine containing apical membrane antigen 1 and merozoite surface protein 4/5 can prime humoral and cellular immune responses and partially protect mice against virulent Plasmodium chabaudi adami DS malaria.一种包含顶端膜抗原1和裂殖子表面蛋白4/5的双顺反子DNA疫苗可引发体液免疫和细胞免疫反应,并部分保护小鼠免受恶性疟原虫DS株的致命感染。
Infect Immun. 2004 Oct;72(10):5565-73. doi: 10.1128/IAI.72.10.5565-5573.2004.
8
Protection against Plasmodium chabaudi malaria induced by immunization with apical membrane antigen 1 and merozoite surface protein 1 in the absence of gamma interferon or interleukin-4.在缺乏γ干扰素或白细胞介素-4的情况下,用顶膜抗原1和裂殖子表面蛋白1免疫诱导对查巴迪疟原虫疟疾的保护作用。
Infect Immun. 2004 Oct;72(10):5605-12. doi: 10.1128/IAI.72.10.5605-5612.2004.
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Recombinant Mycobacterium bovis bacillus Calmette-Guérin secreting merozoite surface protein 1 (MSP1) induces protection against rodent malaria parasite infection depending on MSP1-stimulated interferon gamma and parasite-specific antibodies.分泌裂殖子表面蛋白1(MSP1)的重组牛分枝杆菌卡介苗,依赖于MSP1刺激的γ干扰素和寄生虫特异性抗体,诱导对啮齿动物疟原虫感染的保护作用。
J Exp Med. 1998 Sep 7;188(5):845-54. doi: 10.1084/jem.188.5.845.
10
A recombinant 15-kilodalton carboxyl-terminal fragment of Plasmodium yoelii yoelii 17XL merozoite surface protein 1 induces a protective immune response in mice.约氏疟原虫17XL裂殖子表面蛋白1的重组15千道尔顿羧基末端片段可在小鼠中诱导保护性免疫反应。
Infect Immun. 1993 Jun;61(6):2462-7. doi: 10.1128/iai.61.6.2462-2467.1993.

引用本文的文献

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Parasitol Int. 2022 Dec;91:102637. doi: 10.1016/j.parint.2022.102637. Epub 2022 Aug 1.
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A Novel Model of Asymptomatic Plasmodium Parasitemia That Recapitulates Elements of the Human Immune Response to Chronic Infection.一种新型无症状疟原虫血症模型,该模型概括了人类对慢性感染的免疫反应要素。
PLoS One. 2016 Sep 1;11(9):e0162132. doi: 10.1371/journal.pone.0162132. eCollection 2016.
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Impact of pre-existing MSP1(42)-allele specific immunity on potency of an erythrocytic Plasmodium falciparum vaccine.
预先存在的 MSP1(42)-等位基因特异性免疫对红内期疟原虫疫苗效力的影响。
Malar J. 2012 Sep 7;11:315. doi: 10.1186/1475-2875-11-315.
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Immunogenicity and in vitro protective efficacy of recombinant Mycobacterium bovis bacille Calmette Guerin (rBCG) expressing the 19 kDa merozoite surface protein-1 (MSP-1(19)) antigen of Plasmodium falciparum.表达恶性疟原虫裂殖子表面蛋白-1(MSP-1(19))抗原的重组牛型结核分枝杆菌(rBCG)的免疫原性和体外保护效力。
Parasitol Res. 2011 Apr;108(4):887-97. doi: 10.1007/s00436-010-2130-5. Epub 2010 Nov 6.
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Growth-inhibitory antibodies are not necessary for protective immunity to malaria infection.生长抑制抗体对于疟疾感染的保护性免疫并非必需。
Infect Immun. 2010 Feb;78(2):680-7. doi: 10.1128/IAI.00939-09. Epub 2009 Nov 16.
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MSP-1p42-specific antibodies affect growth and development of intra-erythrocytic parasites of Plasmodium falciparum.疟原虫裂殖子表面蛋白1的42 kDa片段特异性抗体影响恶性疟原虫红细胞内期寄生虫的生长和发育。
Malar J. 2009 Aug 3;8:183. doi: 10.1186/1475-2875-8-183.
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Secreted antibody is required for immunity to Plasmodium berghei.分泌型抗体是对伯氏疟原虫免疫所必需的。
Infect Immun. 2009 Jan;77(1):414-8. doi: 10.1128/IAI.00982-08. Epub 2008 Nov 10.
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Induction of strain-transcending immunity against Plasmodium chabaudi adami malaria with a multiepitope DNA vaccine.用多表位DNA疫苗诱导针对恰氏疟原虫疟疾的跨株免疫。
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Infect Immun. 2001 Sep;69(9):5464-70. doi: 10.1128/IAI.69.9.5464-5470.2001.