Podrobný výpis o publikaci

KREJČÍ, Lumír, Jiří DAMBORSKÝ, B. THOMSEN, M. DUNO a C. BENDIXEN. Molecular dissection of interactions between Rad51 and members of the recombination-repair group. Online. Molecular and Cellular Biology. 2001, roč. 21, č. 3, s. 966-976. ISSN 0270-7306. [citováno 2024-04-24]

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Základní údaje
Originální název	Molecular dissection of interactions between Rad51 and members of the recombination-repair group
Autoři	KREJČÍ, Lumír, Jiří DAMBORSKÝ, B. THOMSEN, M. DUNO a C. BENDIXEN
Vydání	Molecular and Cellular Biology, 2001, 0270-7306.

Další údaje
Originální jazyk	angličtina
Typ výsledku	Článek v odborném periodiku
Obor	Genetika a molekulární biologie
Stát vydavatele	Spojené státy
Utajení	není předmětem státního či obchodního tajemství
Impakt faktor	Impact factor: 9.836
Kód RIV	RIV/00216224:14310/01:00002738
Organizační jednotka	Přírodovědecká fakulta
UT WoS	000166353700026
Změnil	Změnil: prof. Mgr. Jiří Damborský, Dr., učo 1441. Změněno: 13. 2. 2002 06:02.

Anotace
Recombination is important for the repair of DNA damage and for chromosome segregation during meiosis; it has also been shown to participate in the regulation of cell proliferation. In the yeast Saccharomyces cerevisiae, recombination requires products of the RAD52 epistasis group. The Rad51 protein associates with the Rad51, Rad52, Rad54, and Rad55 proteins to form a dynamic complex. We describe a new strategy to screen for mutations which cause specific disruption of the interaction between certain proteins in the complex, leaving other interactions intact. This approach defines distinct protein interaction domains and protein relationships within the Rad51 complex. Alignment of the mutations onto the constructed three-dimensional model of the Rad51 protein reveal possible partially overlapping interfaces for the Rad51-Rad52 and the Rad51-Rad54 interactions. Rad51-Rad55 and Rad51-Rad51 interactions are affected by the same spectrum of mutations, indicating similarity between the two modes of binding. Finally, the detection of a subset of mutations within Rad51 which disrupt the interaction with mutant Rad52 protein but activate the interaction with Rad54 suggests that dynamic changes within the Rad51 protein may contribute to an ordered reaction process.

Anotace

Recombination is important for the repair of DNA damage and for chromosome segregation during meiosis; it has also been shown to participate in the regulation of cell proliferation. In the yeast Saccharomyces cerevisiae, recombination requires products of the RAD52 epistasis group. The Rad51 protein associates with the Rad51, Rad52, Rad54, and Rad55 proteins to form a dynamic complex. We describe a new strategy to screen for mutations which cause specific disruption of the interaction between certain proteins in the complex, leaving other interactions intact. This approach defines distinct protein interaction domains and protein relationships within the Rad51 complex. Alignment of the mutations onto the constructed three-dimensional model of the Rad51 protein reveal possible partially overlapping interfaces for the Rad51-Rad52 and the Rad51-Rad54 interactions. Rad51-Rad55 and Rad51-Rad51 interactions are affected by the same spectrum of mutations, indicating similarity between the two modes of binding. Finally, the detection of a subset of mutations within Rad51 which disrupt the interaction with mutant Rad52 protein but activate the interaction with Rad54 suggests that dynamic changes within the Rad51 protein may contribute to an ordered reaction process.

Návaznosti
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MSM 143100005, záměr	Investor: Ministerstvo školství, mládeže a tělovýchovy ČR, Strukturně-funkční vztahy biomolekul a jejich role v metabolismu