Your search keyword '"Jing H. Wang"' showing total 2 results

1. Alternative end-joining catalyzes robust IgH locus deletions and translocations in the combined absence of ligase. 4 and Ku70.

Author

BoboiIa, Cristian, Jankovic, Mila, Yan, Catherine T., Jing H. Wang, Wesemann, Duane R., Tingting Zhang, Fazeli, Alex, Feldman, Lauren, Nussenzweig, Andre, Nussenzweig, Michel, and Alt, Frederick W.

Subjects

GENETIC recombination, CHROMOSOMAL translocation, LIGASES, IMMUNOGLOBULINS, ONCOGENES, CHROMOSOMES

Abstract

Class switch recombination (CSR) in B lymphocytes is initiated by introduction of multiple DNA double-strand breaks (DSB5) into switch(S) regions that flank immunoglobulin heavy chain (IgH) constant region exons. CSR is completed by joining a DSB in the donor Sp to a DSB in a downstream acceptor S region (e.g., Sγ1) by endjoining. In normal cells, many CSR junctions are mediated by classical nonhomologous end-joining (C-NHEJ), which employs the Ku70/80 complex for DSB recognition and XRCC4/DNA ligase 4 for ligation. Alternative end-joining (A-EJ) mediates CSR, at reduced levels, in the absence of C-NHEJ, even in combined absence of Ku70 and ligase 4. demonstrating an A-EJ pathway totally distinct from C-NHEJ. Multiple DSBs are introduced into Sp during CSR, with some being rejoined or joined to each other to generate internal switch deletions (ISDs). In addition, S-region DSB5 can be joined to other chromosomes to generate translocations. the level of which is increased by absence of a single C-NHEJ component (e.g., XRCC4). We asked whether ISD and S-region translocations occur in the complete absence of C-NHEJ (e.g., in Ku70/ligase 4 double-deficient B cells). We found, unexpectedly, that B-cell activation for CSR generates substantial ISD in both Sγ1 and Syl and that ISD in both is greatly increased by the absence of C-NHEJ. IgH chromosomal translocations to the c-myc oncogene also are augmented in the combined absence of Ku70 and ligase 4. We discuss the implications of these findings for A-EJ in normal and abnormal DSB repair. [ABSTRACT FROM AUTHOR]

Published

2010

2. Homozygous DNA ligase IV R278H mutation in mice leads to leaky SCID and represents a model for human LIG4 syndrome.

Author

Rucci, Francesca, Notarangelo, Luigi D., Fazeli, Alex, Patrizi, Laura, Hickernell, Thomas, Paganini, Tiziana, Coakley, Kristen M., Detre, Cynthia, Keszei, Marton, Walter, Jolan E., Feldman, Lauren, Hwei-Ling Cheng, PoIiani, Pietro Luigi, Jing H. Wang, Balter, Barbara B., Recher, Mike, Andersson, Emma-Maria, Zha, Shan, Giliani, Silvia, and Terhorst, Cox

Subjects

GENETIC mutation, SEVERE combined immunodeficiency, LYMPHOCYTES, DNA ligases, MICE physiology, IONIZING radiation, PHYSIOLOGY, THERAPEUTICS

Abstract

DNA ligase IV (LIG4) is an essential component of the nonhomologous end-joining (NHEJ) repair pathway and plays a key role in V(D)J recombination. Hypomorphic LIG4 mutations in humans are associated with increased cellular radiosensitivity, microcephaly, facial dysmorphisms, growth retardation, developmental delay, and a variable degree of immunodeficiency. We have generated a knock-in mouse model with a homozygous Lig4 R278H mutation that corresponds to the first LIG4 mutation reported in humans. The phenotype of homozygous mutant mice Lig4R278H/R278H (Lig4R/R) includes growth retardation, a decreased life span, a severe cellular sensitivity to ionizing radiation, and a very severe, but incomplete block in I and B cell development. Peripheral T lymphocytes show an activated and anergic phenotype, reduced viability, and a restricted repertoire, reminiscent of human leaky SCID. Genomic instability is associated with a high rate of thymic tumor development. Finally, Lig4R/R mice spontaneously produce low-affinity antibodies that include autoreactive specificities, but are unable to mount high-affinity antibody responses. These findings highlight the importance of LIG4 in lymphocyte development and function, and in genomic stability maintenance, and provide a model for the complex phenotype of LIG4 syndrome in humans. [ABSTRACT FROM AUTHOR]

Published

2010