Page 73

Notes:

conferenceseries

.com

Volume 8

Journal of Biotechnology & Biomaterials

ISSN: 2155-952X

Adv.Biotech 2018

November 15-17, 2018

November 15-17, 2018 | Berlin, Germany

4

th

International Conference on

Advances in Biotechnology and Bioscience

Investigating the nexus between DNA repair pathways and genomic instability in cancer

Sonali Bhattacharjee

Cold Spring Harbor Laboratory, USA

D

NA double-strand breaks are one of the most lethal lesions to a cell that can be repaired by one of the two cellular pathways;

non-homologous end joining or homologous recombination. Homologous recombination genes are particularly attractive

targets for precision cancer therapy because these genes have altered expression patterns in cancer cells when compared with

normal cells and these genetic abnormalities can be targeted for selectively killing cancer cells while leaving normal cells

unscathed. Synthetic lethality is thought to be the new frontier of cancer therapeutics because it overcomes the limitation of

chemotherapy, which is unable to discriminate between cancer cells and normal cells. Two genes are synthetically lethal when

simultaneous disruptions of both genes gives rise to a lethal phenotype, while the disruption of either gene alone is viable.

Many homologous recombination genes have synthetic lethal relationships with oncogenes and tumor suppressor genes, which

can be targeted for the development of cancer therapy- an approach referred to as combination therapy. In the presentation,

author will summarize recent progress in understanding both the functioning and the regulation of the DNA repair machinery

and elaborate on the clinical applications of these proteins in cancer therapy

.

bhattacharjee@cshl.edu

J Biotechnol Biomater 2018, Volume 8

DOI: 10.4172/2155-952X-C6-104