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Graf, Johannes ; Kretz, Markus

From structure to function: route to understanding lncRNA mechanism

Graf, Johannes und Kretz, Markus (2020) From structure to function: route to understanding lncRNA mechanism. BioEssays 42, S. 2000027.

Veröffentlichungsdatum dieses Volltextes: 27 Jan 2021 13:44
Artikel
DOI zum Zitieren dieses Dokuments: 10.5283/epub.44635


Zusammenfassung

RNAs have emerged as a major target for diagnostics and therapeutics approaches. Regulatory nonprotein-coding RNAs (ncRNAs) in particular display remarkable versatility. They can fold into complex structures and interact with proteins, DNA, and other RNAs, thus modulating activity, localization, or interactome of multi-protein complexes. Thus, ncRNAs confer regulatory plasticity and represent a ...

RNAs have emerged as a major target for diagnostics and therapeutics approaches. Regulatory nonprotein-coding RNAs (ncRNAs) in particular display remarkable versatility. They can fold into complex structures and interact with proteins, DNA, and other RNAs, thus modulating activity, localization, or interactome of multi-protein complexes. Thus, ncRNAs confer regulatory plasticity and represent a new layer of regulatory control. Interestingly, long noncoding RNAs (lncRNAs) tend to acquire complex secondary and tertiary structures and their function-in many cases-is dependent on structural conservation rather than primary sequence conservation. Whereas for many proteins, structure and its associated function are closely connected, for lncRNAs, the structural domains that determine functionality and its interactome are still not well understood. Numerous approaches for analyzing the structural configuration of lncRNAs have been developed recently. Here, will provide an overview of major experimental approaches used in the field, and discuss the potential benefit of using combinatorial strategies to analyze lncRNA modes of action based on structural information.



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Details

DokumentenartArtikel
Titel eines Journals oder einer ZeitschriftBioEssays
Verlag:Wiley
Ort der Veröffentlichung:HOBOKEN
Band:42
Seitenbereich:S. 2000027
Datum2020
InstitutionenBiologie und Vorklinische Medizin > Institut für Biochemie, Genetik und Mikrobiologie
Biologie und Vorklinische Medizin > Institut für Biochemie, Genetik und Mikrobiologie > Lehrstuhl für Biochemie I
Identifikationsnummer
WertTyp
10.1002/bies.202000027DOI
Stichwörter / KeywordsRNA SECONDARY STRUCTURE; LONG NONCODING RNA; X-CHROMOSOME INACTIVATION; STRUCTURE PREDICTION; PRIMER EXTENSION; SHAPE; REVEALS; PROTEIN; TRANSCRIPTOME; PURIFICATION; lncRNA; long noncoding RNA
Dewey-Dezimal-Klassifikation500 Naturwissenschaften und Mathematik > 570 Biowissenschaften, Biologie
StatusVeröffentlicht
BegutachtetJa, diese Version wurde begutachtet
An der Universität Regensburg entstandenJa
URN der UB Regensburgurn:nbn:de:bvb:355-epub-446350
Dokumenten-ID44635

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