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AuthorHeck, Astrid Johannadc.contributor.author
AuthorOstertag, Theresadc.contributor.author
AuthorSchnell, Leoniedc.contributor.author
AuthorFischer, Stephandc.contributor.author
AuthorAgrawalla, Bikram Kesharidc.contributor.author
AuthorWinterwerber, Piadc.contributor.author
AuthorWirsching, Evadc.contributor.author
AuthorFouler, Michaeldc.contributor.author
AuthorFrick, Manfreddc.contributor.author
AuthorKuan, Seah Lingdc.contributor.author
AuthorWeil, Tanjadc.contributor.author
AuthorBarth, Holgerdc.contributor.author
Date of accession2023-05-31T15:06:50Zdc.date.accessioned
Available in OPARU since2023-05-31T15:06:50Zdc.date.available
Date of first publication2019-07-18dc.date.issued
AbstractThe targeted pharmacological modulation of polymorphonuclear leukocytes (PMNs) is of major medical interest. These innate immune cells play a central role in the defense against pathogenic microorganisms. However, their excessive chemotactic recruitment into tissues after traumatic injury is detrimental due to local and systemic inflammation. Rho-GTPases, being the master regulators of the actin cytoskeleton, regulate migration and chemotaxis of PMNs, are attractive pharmacological targets. Herein, supramolecular protein complexes are assembled in a “mix-and-match” approach containing the specific Rho-inhibiting clostridial C3 enzyme and three PMN-binding peptides using an avidin platform. Selective delivery of the C3 Rho-inhibitor with these complexes into the cytosol of human neutrophil-like NB-4 cells and primary human PMNs ex vivo is demonstrated, where they catalyze the adenosine diphosphate (ADP) ribosylation of Rho and induce a characteristic change in cell morphology. Notably, the complexes do not deliver C3 enzyme into human lung epithelial cells, A549 lung cancer cells, and immortalized human alveolar epithelial cells (hAELVi), demonstrating their cell type-selectivity. The supramolecular complexes represent attractive molecular tools to decipher the role of PMNs in infection and inflammation or for the development of novel therapeutic approaches for diseases that are associated with hyperactivity and reactivity of PMNs such as post-traumatic injury.dc.description.abstract
Languageendc.language.iso
PublisherUniversität Ulmdc.publisher
LicenseCC BY 4.0 Internationaldc.rights
Link to license texthttps://creativecommons.org/licenses/by/4.0/dc.rights.uri
KeywordC3 Rho inhibitordc.subject
Keywordpolymorphonuclear leukocytes (PMNs)dc.subject
Keywordsupramolecular toxin complexdc.subject
Keywordtargeted protein deliverydc.subject
Dewey Decimal GroupDDC 610 / Medicine & healthdc.subject.ddc
LCSHLeucocytesdc.subject.lcsh
TitleSupramolecular toxin complexes for targeted pharmacological modulation of polymorphonuclear leukocyte functionsdc.title
Resource typeWissenschaftlicher Artikeldc.type
VersionpublishedVersiondc.description.version
DOIhttp://dx.doi.org/10.18725/OPARU-48909dc.identifier.doi
URNhttp://nbn-resolving.de/urn:nbn:de:bsz:289-oparu-48985-5dc.identifier.urn
GNDSupramolekulare Chemiedc.subject.gnd
FacultyMedizinische Fakultätuulm.affiliationGeneral
FacultyFakultät für Naturwissenschaftenuulm.affiliationGeneral
InstitutionUKU. Institut für Pharmakologie und Toxikologieuulm.affiliationSpecific
InstitutionInstitut für Anorganische Chemie I (Materialien und Katalyse)uulm.affiliationSpecific
InstitutionInstitut für Allgemeine Physiologieuulm.affiliationSpecific
Peer reviewjauulm.peerReview
DCMI TypeTextuulm.typeDCMI
CategoryPublikationenuulm.category
DOI of original publication10.1002/adhm.201900665dc.relation1.doi
Source - Title of sourceAdvanced Healthcare Materialssource.title
Source - Place of publicationWileysource.publisher
Source - Volume8source.volume
Source - Issue17source.issue
Source - Year2019source.year
Source - From page1source.fromPage
Source - To page12source.toPage
Source - Article number1900665source.articleNumber
Source - ISSN2192-2640source.identifier.issn
Source - eISSN2192-2659source.identifier.eissn
EU project uulmBIOQ / Diamond Quantum Devices and Biology / EC / FP7 / 319130uulm.projectEU
Open AccessEarly Accessuulm.OA
CommunityUniversitätsklinikum Ulmuulm.community
CommunityFakultät für Naturwissenschaftenuulm.community
CommunityMedizinische Fakultätuulm.community
WoS000476382500001uulm.identifier.wos
Bibliographyuulmuulm.bibliographie
Is Supplemented Byhttps://onlinelibrary.wiley.com/action/downloadSupplement?doi=10.1002%2Fadhm.201900665&file=adhm201900665-sup-0001-S1.pdfdc.relation.isSupplementedBy
DFG project uulmSFB 1149 Teilprojekt A04 / Zelltypspezifische Trägerproteine für die gezielte pharmakologische Hemmung der Rho-/Aktin-abhängigen Leukozyten-Rekrutierung in den Alveolarraum nach stumpfem Thoraxtrauma / DFG / 251293561uulm.projectDFG
DFG project uulmSFB 1149 Teilprojekt A05 / Zelluläre und molekulare Effekte der Trauma-induzierten Schädigung des distalen respiratorischen Epithels / DFG / 251293561uulm.projectDFG
DFG project uulmSFB 1279 Teilprojekt C01 / Entwicklung und Synthese optimierter Peptid-Biohybride / DFG / 316249678uulm.projectDFG
DFG project uulmSFB 1279 Teilprojekt C02 / Biohybridtransporter zum zellspezifischen Transport und der kontrollierten Freisetzung von pharmakologisch aktiven Peptiden / DFG / 316249678uulm.projectDFG


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