Microsporidia: invasion apparatus
微孢子虫:入侵装置
基本信息
- 批准号:10434963
- 负责人:
- 金额:$ 42万
- 依托单位:
- 依托单位国家:美国
- 项目类别:
- 财政年份:2016
- 资助国家:美国
- 起止时间:2016-05-16 至 2026-05-31
- 项目状态:未结题
- 来源:
- 关键词:Acquired Immunodeficiency SyndromeAgricultureAnimal FeedAnimalsAntibodiesAquacultureBenignBioinformaticsBiologicalBirdsCategory B pathogenCell membraneCellsCellular biologyCessation of lifeChronic diarrheaCollaborationsComparative StudyComplementComplexConjunctivitisCryoelectron MicroscopyDataDevelopmentDiarrheaEconomicsEncephalitisEncephalitozoon hellemEnterocytozoon bieneusiEpitopesEtiologyFishesFoodGeneticGenomeGerminationGrantHIVHIV InfectionsHumanImmuneImmune SeraImmunizationImmunocompetentImmunocompromised HostImmunoelectron MicroscopyImmunologicsIn VitroInfectionInsectaInvadedInvertebratesInvestigationKeratoconjunctivitisLaboratoriesLaboratory ResearchMammalsMethodsMicrobeMicroscopicMicroscopyMicrosporidiaMicrosporidiosisMolecularMorphologyMusMyositisNematodaNervous system structureNosemaNosema corneumOrgan TransplantationOrganellesOrganismPathogenesisPathogenicityPatientsPenetrationPhylogenetic AnalysisPost-Translational Protein ProcessingProcessProteinsProteomeProteomicsPublishingRecombinantsReproduction sporesResearchResearch Project GrantsResolutionRespiratory MusclesRoleScanningSeptata intestinalisSisterSiteSoilSourceStructureSynapsesSystemTFRC geneTechniquesTransfectionTubeUnited States National Institutes of HealthValidationVero CellsWatereconomic impactemerging pathogenexperimental studyfungusgastrointestinalgene functiongenome resourcehuman pathogenimmunomodulatory therapiesinfection managementinsightinterestnovel therapeutic interventionopportunistic pathogenparasite invasionpathogenpathogen genomepreservationprogramspublic health relevancereproductivesample fixationstructural biologysugarthree dimensional structuretoolwasting
项目摘要
ABSTRACT Microsporidia are intracellular pathogens related to the Fungi that have been studied for more
than 150 years. They are opportunistic pathogens in patients with AIDS, most commonly causing diarrhea,
encephalitis, myositis, or conjunctivitis. In patients with advanced AIDS they have been etiologic in up to 30%
of cases of chronic diarrhea with wasting. Microsporidia have also been found to cause infections in other
immunocompromised hosts, such as patients who have undergone organ transplantation or those on immune
modulating therapies. Infections are now also being recognized in immune competent hosts causing either
keratoconjunctivitis or diarrhea. Microsporidia are classified as NIH category B priority pathogens and EPA
pathogens of interest as they are transmitted by both food and water sources. In addition to being human
pathogens, these pathogenic organisms have major economic impacts on agriculture (via effects on insects
and sericulture), aquaculture and animals (food, domestic and wildlife). Infections in animals range from
cryptic, benign infections to spectacular, massive infections that cause extensive damage and often death of
the host. Microsporidia produce spores containing a unique invasion organelle, the polar tube, which is one
of the most complex single celled forms known in the biological world. The mechanism by which the polar
tube interacts with its host cell during invasion is still unknown. A long standing research program in my
laboratory group is focused on understanding the mechanism of invasion and the structural biology and
composition of the polar tube. We have developed techniques for the purification of this structure, identified
polar tube proteins (PTPs) and their post translational modifications, and defined methods to study how these
proteins interact. Furthermore, our investigations have defined the invasion synapse and the functional role(s)
of several PTPs in the process of invasion. However, the full complement of proteins in this structure and the
interactions of these components during invasion remain to be determined. This research grant will employ
a combination of proteomic, immunologic and ultrastructural studies to characterize the polar tube and its
protein interactome to better define and understand the mechanism of invasion. Furthermore, advanced
microscopic techniques (i.e. cryo-EM and super resolution microscopy) will be employed to provide insight
into the three dimensional structure of the polar tube and arrangement of PTPs providing critical information
on fundamental questions concerning the organization of this invasion organelle that have not been able to
be resolved by traditional microscopy. In other microbes studies on invasion have provided critical data for
understanding pathogenesis and for new therapeutic approaches to the management of infections. We have
already demonstrated that antisera to various PTPs can inhibit invasion and infection. We believe that studies
of the composition, formation and function of this organelle during germination and invasion should provide a
basis for the development of new strategies for control of these important HIV-associated pathogens.
摘要微孢子虫是一种与真菌有关的胞内病原体,
超过150年。它们是艾滋病患者的机会致病菌,最常见的是引起腹泻,
脑炎、肌炎或结膜炎。在晚期艾滋病患者中,高达30%的患者为病因
慢性腹泻伴消瘦的病例。微孢子虫也被发现引起其他
免疫功能低下的宿主,如经历过器官移植的患者或免疫功能低下的患者。
调节疗法。感染现在也在免疫能力强的宿主中被识别,
角膜结膜炎或腹泻。微孢子虫被归类为NIH B类优先病原体,EPA
病原体的利益,因为他们通过食物和水源传播。除了作为人类
病原体,这些病原体生物对农业具有重大的经济影响(通过对昆虫的影响
养殖业和畜牧业(食用、家养和野生动物)。动物感染的范围从
从神秘的良性感染到壮观的大规模感染,这些感染会造成广泛的损害,甚至通常导致死亡
主持人微孢子虫产生的孢子含有一种独特的入侵细胞器,极管,这是一个
最复杂的单细胞形式的一部分。极地的机制
tube在入侵过程中与宿主细胞的相互作用仍然是未知的。一个长期的研究项目在我的
实验组的重点是了解入侵机制和结构生物学,
Polar Tube的组成。我们已经开发了纯化这种结构的技术,
极性管蛋白(PTP)及其翻译后修饰,并确定了研究这些修饰的方法。
蛋白质相互作用。此外,我们的研究已经确定了入侵突触和功能作用(S)
在入侵过程中的几个PTP。然而,这种结构中的全部蛋白质和
这些成分在入侵期间的相互作用仍有待确定。这项研究经费将用于
结合蛋白质组学、免疫学和超微结构研究来表征极管及其
蛋白质相互作用组,以更好地定义和理解入侵的机制。此外,先进
将采用显微镜技术(即冷冻电镜和超分辨率显微镜)来提供洞察力
进入到三维结构的极管和安排的PTP提供关键信息
关于这种入侵细胞器的组织的基本问题,
用传统的显微镜就能分辨出来。在其他微生物中,关于入侵的研究为
了解发病机制和新的治疗方法来管理感染。我们有
已经证明了各种PTP的抗血清可以抑制侵袭和感染。我们相信研究
对这种细胞器在萌发和入侵过程中的组成、形成和功能的研究,
为制定控制这些重要的艾滋病毒相关病原体的新战略奠定了基础。
项目成果
期刊论文数量(0)
专著数量(0)
科研奖励数量(0)
会议论文数量(0)
专利数量(0)
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Louis M. Weiss其他文献
Opportunistic pulmonary aspergillosis with chest wall invasion: plain film and computed tomographic findings
机会性肺曲霉菌病伴胸壁侵犯:平片和计算机断层扫描结果
- DOI:
- 发表时间:
1983 - 期刊:
- 影响因子:0
- 作者:
P. Caligiuri;Heber MacMahon;John Courtney;Louis M. Weiss - 通讯作者:
Louis M. Weiss
A Toxoplasma gondii O-glycosyltransferase that modulates bradyzoite cyst wall rigidity is structurally and functionally distinct from host homologues
调节缓殖子包囊壁刚性的弓形虫 O-糖基转移酶在结构和功能上与宿主同源物不同
- DOI:
- 发表时间:
2023 - 期刊:
- 影响因子:0
- 作者:
Pranav Kumar;T. Tomita;Thomas A. Gerken;Collin J. Ballard;Y. Lee;Louis M. Weiss;Nadine L. Samara - 通讯作者:
Nadine L. Samara
emPlasmodium/em microtubule-binding protein EB1 is critical for partitioning of nuclei in male gametogenesis
疟原虫/红细胞内期疟原虫微管结合蛋白 EB1 对于雄性配子发生过程中的核分裂至关重要
- DOI:
10.1128/mbio.00822-23 - 发表时间:
2023-06-13 - 期刊:
- 影响因子:4.700
- 作者:
Sydney Mauer;Nelly Camargo;Biley A. Abatiyow;Olivia R. Gargaro;Stefan H. I. Kappe;Sudhir Kumar;Louis M. Weiss - 通讯作者:
Louis M. Weiss
Microsporidiosis in Humans
- DOI:
10.1128/cmr.00010-20 - 发表时间:
2021 - 期刊:
- 影响因子:
- 作者:
Bing Han;Guoqing Pan;Louis M. Weiss - 通讯作者:
Louis M. Weiss
Microsporidian spores contain hibernating dimeric ribosomes
微孢子虫孢子含有处于冬眠状态的二聚体核糖体。
- DOI:
10.1038/s41564-023-01481-0 - 发表时间:
2023-09-14 - 期刊:
- 影响因子:19.400
- 作者:
Elizabeth Weyer;Louis M. Weiss - 通讯作者:
Louis M. Weiss
Louis M. Weiss的其他文献
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{{ truncateString('Louis M. Weiss', 18)}}的其他基金
International Workshop on Opportunistic Protists (IWOP-12, 13 and 14)
机会原生生物国际研讨会(IWOP-12、13和14)
- 批准号:
8408859 - 财政年份:2012
- 资助金额:
$ 42万 - 项目类别:
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