The DNA damage checkpoint is a series of complex mechanisms that monitor cell cycle progression in response to genotoxic insults. Once activated it leads to a cell cycle slowdown and the instauration of a complex protein network involving physical and functional interaction with various DNA metabolism reactions (replication, repair, recombination). Moreover a series of tolerance systems have been developed in case the damage would arrive to S phase. One of those systems is the DNA translesion synthesis that using specialized DNApolymerases is able to replicate over the lesion allowing replication fork progression. Using a variety of different genetic and biochemical approaches such as yeast 2-hybrid, coimmunoprecipitations, in vitro pulldown and coimmunolocalization we characterized the complex formed by the Ddc1, Rad17 and Mec3 proteins (also called 9-1-1 complex) and we were able to detect a possible interaction between the 9-1-1, involved in the first step of the checkpoint signaling cascade, and Rev7 a regulatory subunit of PolZ one of the most important translesion polymerase in yeast. Altogether these interactions strongly support an internal crosstalk between different repair system and cell cycle control.

Caratterizzazione biochimica e funzionale del complesso 9-1-1 in S. cerevisiae, crocevia tra checkpoint e sistemi di tolleranza al danno

SABBIONEDA, SIMONE
2005

Abstract

The DNA damage checkpoint is a series of complex mechanisms that monitor cell cycle progression in response to genotoxic insults. Once activated it leads to a cell cycle slowdown and the instauration of a complex protein network involving physical and functional interaction with various DNA metabolism reactions (replication, repair, recombination). Moreover a series of tolerance systems have been developed in case the damage would arrive to S phase. One of those systems is the DNA translesion synthesis that using specialized DNApolymerases is able to replicate over the lesion allowing replication fork progression. Using a variety of different genetic and biochemical approaches such as yeast 2-hybrid, coimmunoprecipitations, in vitro pulldown and coimmunolocalization we characterized the complex formed by the Ddc1, Rad17 and Mec3 proteins (also called 9-1-1 complex) and we were able to detect a possible interaction between the 9-1-1, involved in the first step of the checkpoint signaling cascade, and Rev7 a regulatory subunit of PolZ one of the most important translesion polymerase in yeast. Altogether these interactions strongly support an internal crosstalk between different repair system and cell cycle control.
2005
Italiano
PLEVANI, PAOLO
MUZI FALCONI, MARCO
Università degli Studi di Milano
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/20.500.14242/74664
Il codice NBN di questa tesi è URN:NBN:IT:UNIMI-74664