Identifying and targeting key driver genes for collagen production within the 11q13/14 breast cancer amplicon

Author:

Araiza-Olivera Daniela,Prudnikova Tatiana Y.,Uribe-Alvarez Cristina,Cai Kathy Q.,Franco-Barraza Janusz,Dones Jesús M.,Raines Ronald T.,Chernoff JonathanORCID

Abstract

AbstractGenetic studies indicate that breast cancer can be divided into several basic molecular groups. One of these groups, termed IntClust-2, is characterized by amplification of a small portion of chromosome 11 and has a median survival of only five years. Several cancer-relevant genes occupy this portion of chromosome 11, and it is thought that overexpression of a combination of driver genes in this region is responsible for the poor outcome of women in this group. In this study we used a gene editing method to knock out, one by one, each of 198 genes that are located within the amplified region of chromosome 11 and determined how much each of these genes contributed to the survival of breast cancer cells. In addition to well-known drivers such asCCND1andPAK1, we identified two different genes (SERPINH1andP4HA3), that encode proteins involved in collagen synthesis and organization. Using bothin vitroandin vivofunctional analyses, we determined thatP4HA3and/orSERPINH1provide a critical driver function on IntClust-2 basic processes, such as viability, proliferation, and migration. Inhibiting these enzymes via genetic or pharmacologic means reduced collagen synthesis and impeded oncogenic signaling transduction in cell culture models, and a small-molecule inhibitor of P4HA3 was effective in treating 11q13 tumor growth in an animal model. As collagen has a well-known association with tissue stiffness and aggressive forms of breast cancer, we believe that the two genes we identified provide an opportunity for a new therapeutic strategy in IntClust-2 breast cancers.

Publisher

Cold Spring Harbor Laboratory

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