Immunomics-Guided Antigen Discovery for Praziquantel-Induced Vaccination in Urogenital Human Schistosomiasis

Pearson, Mark S; Tedla, Bemnet A; Becker, Luke; Nakajima, Rie; Jasinskas, Al; Mduluza, Takafira; Mutapi, Francisca; Oeuvray, Claude; Greco, Beatrice; Sotillo, Javier; Felgner, Philip L; Loukas, Alex

Publication:
Immunomics-Guided Antigen Discovery for Praziquantel-Induced Vaccination in Urogenital Human Schistosomiasis

dc.contributor.author	Pearson, Mark S
dc.contributor.author	Tedla, Bemnet A
dc.contributor.author	Becker, Luke
dc.contributor.author	Nakajima, Rie
dc.contributor.author	Jasinskas, Al
dc.contributor.author	Mduluza, Takafira
dc.contributor.author	Mutapi, Francisca
dc.contributor.author	Oeuvray, Claude
dc.contributor.author	Greco, Beatrice
dc.contributor.author	Sotillo, Javier
dc.contributor.author	Felgner, Philip L
dc.contributor.author	Loukas, Alex
dc.contributor.funder	Merck KGaA	es_ES
dc.contributor.funder	Australian Trade and Investment Commission	es_ES
dc.contributor.funder	National Health and Medical Research Council (Australia)	es_ES
dc.contributor.funder	Thrasher Research Fund	es_ES
dc.contributor.funder	Wellcome Trust	es_ES
dc.contributor.funder	NIH - National Institute of Allergy and Infectious Diseases (NIAID) (Estados Unidos)	es_ES
dc.date.accessioned	2022-03-29T10:12:27Z
dc.date.available	2022-03-29T10:12:27Z
dc.date.issued	2021-05-25
dc.description.abstract	Despite the enormous morbidity attributed to schistosomiasis, there is still no vaccine to combat the disease for the hundreds of millions of infected people. The anthelmintic drug, praziquantel, is the mainstay treatment option, although its molecular mechanism of action remains poorly defined. Praziquantel treatment damages the outermost surface of the parasite, the tegument, liberating surface antigens from dying worms that invoke a robust immune response which in some subjects results in immunologic resistance to reinfection. Herein we term this phenomenon Drug-Induced Vaccination (DIV). To identify the antigenic targets of DIV antibodies in urogenital schistosomiasis, we constructed a recombinant proteome array consisting of approximately 1,000 proteins informed by various secretome datasets including validated proteomes and bioinformatic predictions. Arrays were screened with sera from human subjects treated with praziquantel and shown 18 months later to be either reinfected (chronically infected subjects, CI) or resistant to reinfection (DIV). IgG responses to numerous antigens were significantly elevated in DIV compared to CI subjects, and indeed IgG responses to some antigens were completely undetectable in CI subjects but robustly recognized by DIV subjects. One antigen in particular, a cystatin cysteine protease inhibitor stood out as a unique target of DIV IgG, so recombinant cystatin was produced, and its vaccine efficacy assessed in a heterologous Schistosoma mansoni mouse challenge model. While there was no significant impact of vaccination with adjuvanted cystatin on adult worm numbers, highly significant reductions in liver egg burdens (45-55%, P<0.0001) and intestinal egg burdens (50-54%, P<0.0003) were achieved in mice vaccinated with cystatin in two independent trials. This study has revealed numerous antigens that are targets of DIV antibodies in urogenital schistosomiasis and offer promise as subunit vaccine targets for a drug-linked vaccination approach to controlling schistosomiasis.	es_ES
dc.description.peerreviewed	Sí	es_ES
dc.description.sponsorship	This study received financial support from Merck KGaA, Darmstadt, Germany, and the Australian Trade and Investment Commission (Australian Tropical Medicine Commercialisation grants program ATMC50322). The funder was not involved in the study design, collection, analysis, interpretation of data, the writing of this article or the decision to submit it for publication. AL was funded by an NHMRC Senior Principal Research Fellowship (APP1117504). FM was funded by the Thrasher Research Fund (12440) and the Wellcome Trust (108061/Z/15/Z). The authors thank Atik Susianto for maintenance of the parasites and laboratory animals. They also gratefully acknowledge the NIAID Schistosomiasis Research Center of the Biomedical Research Institute, Rockville, MD, USA for the provision of S. mansoni-infected B. glabrata snails for this work through NIH-NIAID contract HHSN2722017000141 for distribution through BEI resources.	es_ES
dc.format.page	663041	es_ES
dc.format.volume	12	es_ES
dc.identifier.citation	Front Immunol. 2021 May 25;12:663041.	es_ES
dc.identifier.doi	10.3389/fimmu.2021.663041	es_ES
dc.identifier.e-issn	1664-3224	es_ES
dc.identifier.journal	Frontiers In Immunology	es_ES
dc.identifier.pubmedID	34113343	es_ES
dc.identifier.uri	http://hdl.handle.net/20.500.12105/13878
dc.language.iso	eng	es_ES
dc.publisher	Frontiers Media	es_ES
dc.relation.publisherversion	https://doi.org/10.3389/fimmu.2021.663041	es_ES
dc.repisalud.centro	ISCIII::Centro Nacional de Microbiología	es_ES
dc.repisalud.institucion	ISCIII	es_ES
dc.rights.accessRights	open access	es_ES
dc.rights.license	Atribución 4.0 Internacional	*
dc.rights.uri	http://creativecommons.org/licenses/by/4.0/	*
dc.subject	Cystatin	es_ES
dc.subject	Immunomics	es_ES
dc.subject	Praziquantel	es_ES
dc.subject	Proteome microarray	es_ES
dc.subject	Urogenital schistosomiasis	es_ES
dc.subject	Vaccine	es_ES
dc.title	Immunomics-Guided Antigen Discovery for Praziquantel-Induced Vaccination in Urogenital Human Schistosomiasis	es_ES
dc.type	journal article	es_ES
dc.type.hasVersion	VoR	es_ES
dspace.entity.type	Publication
relation.isAuthorOfPublication	40eca1bb-9f01-4912-99c8-1fc7f0246d5b
relation.isAuthorOfPublication.latestForDiscovery	40eca1bb-9f01-4912-99c8-1fc7f0246d5b