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Bishop, Douglas K.

One or more keywords matched the following properties of Bishop, Douglas K.

Property	Value
keywords	meiosis, homologous recombination, homology-directed DNA repair, gene targeting, Rad51, Dmc1, RecA
overview	Homologous recombination repairs DNA damage, facilitates DNA replication, and creates the physical connections between chromosomes needed for reductional chromosome segregation during meiosis. We study two key recombination proteins, Dmc1 and Rad51 that are related to the central bacterial recombination protein, RecA. The mechanisms of recombinational repair of damage induced double strand breaks in DNA (DSBs) and the mechanism of meiotic recombination are very closely related in terms of the DNA intermediates that form; DSBs are normal intermediates in most or all meiotic recombination. There are, however critical differences in how meiotic recombination is regulated as compared to mitotic recombinational repair. Our research is directed at understanding how Dmc1's function is specialized for meiosis, how the functions of Rad51 and Dmc1 differ, how the two proteins interact with one another during meiosis, and how the two proteins interact with components of the synaptonemal complex, a meiosis-specific chromosome scaffold. Our studies show that Rad51, which serves as the central “recombinase” in mitotic cells, is converted to a Dmc1 accessory protein in meiosis. Our current approaches to understanding Rad51 and Dmc1 function include biochemical reconstitution of Dmc1 activity. This work currently involves 7 meiotic recombination proteins. We were first to show that recombination proteins can be detected at multiple subnuclear sites during recombination using immunostaining techniques. We have used cytological methods in the past to identify proteins required for recruitment of recombinase to double strand break sites in mitotic and meiotic cells. These regulators include the breast cancer susceptibility genes BRCA1 and BRCA2, which promote the assembly of recombination complexes, and RAD54 family translocases, which promote disassembly. We recently began to focus our cytological efforts on super-resolution light microscopy methods including STORM and STED. These methods are shedding new light on the architecture of the recombinosome. Finally we use molecular genetic techniques that allow detection of DNA recombination intermediates to study the mechanism that regulate meiotic recombination in living cells.

Property

Value

keywords

meiosis, homologous recombination, homology-directed DNA repair, gene targeting, Rad51, Dmc1, RecA

overview

Homologous recombination repairs DNA damage, facilitates DNA replication, and creates the physical connections between chromosomes needed for reductional chromosome segregation during meiosis. We study two key recombination proteins, Dmc1 and Rad51 that are related to the central bacterial recombination protein, RecA. The mechanisms of recombinational repair of damage induced double strand breaks in DNA (DSBs) and the mechanism of meiotic recombination are very closely related in terms of the DNA intermediates that form; DSBs are normal intermediates in most or all meiotic recombination. There are, however critical differences in how meiotic recombination is regulated as compared to mitotic recombinational repair. Our research is directed at understanding how Dmc1's function is specialized for meiosis, how the functions of Rad51 and Dmc1 differ, how the two proteins interact with one another during meiosis, and how the two proteins interact with components of the synaptonemal complex, a meiosis-specific chromosome scaffold. Our studies show that Rad51, which serves as the central “recombinase” in mitotic cells, is converted to a Dmc1 accessory protein in meiosis. Our current approaches to understanding Rad51 and Dmc1 function include biochemical reconstitution of Dmc1 activity. This work currently involves 7 meiotic recombination proteins. We were first to show that recombination proteins can be detected at multiple subnuclear sites during recombination using immunostaining techniques. We have used cytological methods in the past to identify proteins required for recruitment of recombinase to double strand break sites in mitotic and meiotic cells. These regulators include the breast cancer susceptibility genes BRCA1 and BRCA2, which promote the assembly of recombination complexes, and RAD54 family translocases, which promote disassembly. We recently began to focus our cytological efforts on super-resolution light microscopy methods including STORM and STED. These methods are shedding new light on the architecture of the recombinosome. Finally we use molecular genetic techniques that allow detection of DNA recombination intermediates to study the mechanism that regulate meiotic recombination in living cells.

One or more keywords matched the following items that are connected to Bishop, Douglas K.

Item Type	Name
Concept	DNA Damage
Concept	DNA-Binding Proteins
Concept	DNA Repair
Concept	DNA, Fungal
Concept	DNA, Neoplasm
Concept	DNA
Concept	DNA-Directed DNA Polymerase
Concept	DNA, Superhelical
Concept	DNA Replication
Concept	DNA, Circular
Concept	DNA, Viral
Concept	DNA, Complementary
Concept	Rad52 DNA Repair and Recombination Protein
Concept	DNA Repair Enzymes
Concept	DNA Breaks, Double-Stranded
Concept	DNA, Cruciform
Concept	DNA Helicases
Concept	DNA, Single-Stranded
Concept	DNA Primers
Concept	DNA Topoisomerases
Concept	Recombinational DNA Repair
Academic Article	Xrcc3 is required for assembly of Rad51 complexes in vivo.
Academic Article	BRCA2 and homologous recombination.
Academic Article	Saccharomyces cerevisiae checkpoint genes MEC1, RAD17 and RAD24 are required for normal meiotic recombination partner choice.
Academic Article	The breast cancer susceptibility gene BRCA1 is required for subnuclear assembly of Rad51 and survival following treatment with the DNA cross-linking agent cisplatin.
Academic Article	Crossover interference in Saccharomyces cerevisiae requires a TID1/RDH54- and DMC1-dependent pathway.
Academic Article	Early decision; meiotic crossover interference prior to stable strand exchange and synapsis.
Academic Article	Saccharomyces cerevisiae Dmc1 protein promotes renaturation of single-strand DNA (ssDNA) and assimilation of ssDNA into homologous super-coiled duplex DNA.
Academic Article	Calcium ion promotes yeast Dmc1 activity via formation of long and fine helical filaments with single-stranded DNA.
Academic Article	Multiple repair pathways mediate tolerance to chemotherapeutic cross-linking agents in vertebrate cells.
Academic Article	Red-Hed regulation: recombinase Rad51, though capable of playing the leading role, may be relegated to supporting Dmc1 in budding yeast meiosis.
Academic Article	The Yin and Yang of treating BRCA-deficient tumors.
Academic Article	A hot spot for RAD51C interactions revealed by a peptide that sensitizes cells to cisplatin.
Academic Article	RAD51 up-regulation bypasses BRCA1 function and is a common feature of BRCA1-deficient breast tumors.
Academic Article	A comparative analysis of Dmc1 and Rad51 nucleoprotein filaments.
Academic Article	The Mei5-Sae3 protein complex mediates Dmc1 activity in Saccharomyces cerevisiae.
Academic Article	Tid1/Rdh54 promotes dissociation of Dmc1 from nonrecombinogenic sites on meiotic chromatin.
Academic Article	Swi2/Snf2-related translocases prevent accumulation of toxic Rad51 complexes during mitotic growth.
Academic Article	Brca1 in immunoglobulin gene conversion and somatic hypermutation.
Academic Article	Cells deficient in the FANC/BRCA pathway are hypersensitive to plasma levels of formaldehyde.
Academic Article	The epistatic relationship between BRCA2 and the other RAD51 mediators in homologous recombination.
Academic Article	Rad51, the lead in mitotic recombinational DNA repair, plays a supporting role in budding yeast meiosis.
Academic Article	A chemical compound that stimulates the human homologous recombination protein RAD51.
Academic Article	Rad51 is an accessory factor for Dmc1-mediated joint molecule formation during meiosis.
Academic Article	RI-1: a chemical inhibitor of RAD51 that disrupts homologous recombination in human cells.
Academic Article	Multiple mechanisms of meiotic recombination.
Academic Article	RecA homologs Dmc1 and Rad51 interact to form multiple nuclear complexes prior to meiotic chromosome synapsis.
Academic Article	Rad52 associates with RPA and functions with rad55 and rad57 to assemble meiotic recombination complexes.
Academic Article	High copy number suppression of the meiotic arrest caused by a dmc1 mutation: REC114 imposes an early recombination block and RAD54 promotes a DMC1-independent DSB repair pathway.
Academic Article	Assembly of RecA-like recombinases: distinct roles for mediator proteins in mitosis and meiosis.
Academic Article	Heterodimeric complexes of Hop2 and Mnd1 function with Dmc1 to promote meiotic homolog juxtaposition and strand assimilation.
Academic Article	Synthesis-dependent strand annealing in meiosis.
Academic Article	RecA homology search is promoted by mechanical stress along the scanned duplex DNA.
Academic Article	Gradual implementation of the meiotic recombination program via checkpoint pathways controlled by global DSB levels.
Academic Article	DNA strand exchange and RecA homologs in meiosis.
Academic Article	RAD54 family translocases counter genotoxic effects of RAD51 in human tumor cells.
Academic Article	DNA damage response clamp 9-1-1 promotes assembly of ZMM proteins for formation of crossovers and synaptonemal complex.
Academic Article	Meiotic crossover control by concerted action of Rad51-Dmc1 in homolog template bias and robust homeostatic regulation.
Academic Article	The third exon of the budding yeast meiotic recombination gene HOP2 is required for calcium-dependent and recombinase Dmc1-specific stimulation of homologous strand assimilation.
Academic Article	The RAD51-stimulatory compound RS-1 can exploit the RAD51 overexpression that exists in cancer cells and tumors.
Academic Article	Caffeine impairs resection during DNA break repair by reducing the levels of nucleases Sae2 and Dna2.
Academic Article	Caffeine inhibits gene conversion by displacing Rad51 from ssDNA.
Academic Article	Small Rad51 and Dmc1 Complexes Often Co-occupy Both Ends of a Meiotic DNA Double Strand Break.
Academic Article	The ATPase activity of E. coli RecA prevents accumulation of toxic complexes formed by erroneous binding to undamaged double stranded DNA.
Academic Article	Purification of Saccharomyces cerevisiae Homologous Recombination Proteins Dmc1 and Rdh54/Tid1 and a Fluorescent D-Loop Assay.
Academic Article	RPA resolves conflicting activities of accessory proteins during reconstitution of Dmc1-mediated meiotic recombination.
Academic Article	Non-enzymatic roles of human RAD51 at stalled replication forks.
Academic Article	Distinct Functions in Regulation of Meiotic Crossovers for DNA Damage Response Clamp Loader Rad24(Rad17) and Mec1(ATR) Kinase.
Academic Article	A mutant form of Dmc1 that bypasses the requirement for accessory protein Mei5-Sae3 reveals independent activities of Mei5-Sae3 and Rad51 in Dmc1 filament stability.
Academic Article	Distinct Functions in Regulation of Meiotic Crossovers for DNA Damage Response Clamp Loader Rad24(Rad17) and Mec1(ATR) Kinase.
Academic Article	How strand exchange protein function benefits from ATP hydrolysis.

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