Your search keyword '"Klein, Isaac A."' showing total 2 results

1. DNA damage defines sites of recurrent chromosomal translocations in B lymphocytes

Author

Hakim, Ofir, Resch, Wolfgang, Yamane, Arito, Klein, Isaac, Kieffer-Kwon, Kyong-Rim, Jankovic, Mila, Oliveira, Thiago, Bothmer, Anne, Voss, Ty C., Ansarah-Sobrinho, Camilo, Mathe, Ewy, Liang, Genqing, Cobell, Jesse, Nakahashi, Hirotaka, Robbiani, Davide F., Nussenzweig, Andre, Hager, Gordon L., Nussenzweig, Michel C., and Casellas, Rafael

Subjects

Translocation (Genetics) -- Physiological aspects -- Health aspects, B cells -- Genetic aspects -- Health aspects, DNA damage -- Physiological aspects -- Health aspects, Cancer -- Development and progression -- Genetic aspects, Environmental issues, Science and technology, Zoology and wildlife conservation

Abstract

Recurrent chromosomal translocations underlie both haematopoietic and solid tumours. Their origin has been ascribed to selection of random rearrangements, targeted DNA damage, or frequent nuclear interactions between translocation partners; however, the relative contribution of each of these elements has not been measured directly or on a large scale. Here we examine the role of nuclear architecture and frequency of DNA damage in the genesis of chromosomal translocations by measuring these parameters simultaneously in cultured mouse B lymphocytes. In the absence of recurrent DNA damage, translocations between Igh or Myc and all other genes are directly related to their contact frequency. Conversely, translocations associated with recurrent site-directed DNA damage are proportional to the rate of DNA break formation, as measured by replication protein A accumulation at the site of damage. Thus, non-targeted rearrangements reflect nuclear organization whereas DNA break formation governs the location and frequency of recurrent translocations, including those driving B-cell malignancies., Most cancers bear cytogenetic abnormalities including chromosomal translocations and rearrangements (1). Although translocations and rearrangements are central to the development of cancer, their origins are poorly understood. One possibility is [...]

Published

2012

2. Rag mutations reveal robust alternative end joining

Author

Corneo, Barbara, Wendland, Rebecca L., Deriano, Ludovic, Cui, Xiaoping, Klein, Isaac A., Wong, Serre-Yu, Arnal, Suzzette, Holub, Abigail J., Weller, Geoffrey R., Pancake, Bette A., Shah, Sundeep, Brandt, Vicky L., Meek, Katheryn, and Roth, David B.

Subjects

Gene mutations -- Research, DNA repair -- Research, Environmental issues, Science and technology, Zoology and wildlife conservation, Research

Abstract

Mammalian cells repair DNA double-strand breaks (DSBs) through either homologous recombination or non-homologous end joining (NHEJ). V(D)J recombination, a cut-and-paste mechanism for generating diversity in antigen receptors, relies on NHEJ [...]

Published

2007