New genes involved in cancer identified by retroviral tagging

T Suzuki, H Shen, K Akagi, HC Morse, JD Malley… - Nature …, 2002 - nature.com
T Suzuki, H Shen, K Akagi, HC Morse, JD Malley, DQ Naiman, NA Jenkins, NG Copeland
Nature genetics, 2002nature.com
Retroviral insertional mutagenesis in BXH2 and AKXD mice induces a high incidence of
myeloid leukemia and B-and T-cell lymphoma, respectively. The retroviral integration sites
(RISs) in these tumors thus provide powerful genetic tags for the discovery of genes involved
in cancer 1, 2. Here we report the first large-scale use of retroviral tagging for cancer gene
discovery in the post-genome era. Using high throughput inverse PCR 1, we cloned and
analyzed the sequences of 884 RISs from a tumor panel composed primarily of B-cell …
Abstract
Retroviral insertional mutagenesis in BXH2 and AKXD mice induces a high incidence of myeloid leukemia and B-and T-cell lymphoma, respectively. The retroviral integration sites (RISs) in these tumors thus provide powerful genetic tags for the discovery of genes involved in cancer 1, 2. Here we report the first large-scale use of retroviral tagging for cancer gene discovery in the post-genome era. Using high throughput inverse PCR 1, we cloned and analyzed the sequences of 884 RISs from a tumor panel composed primarily of B-cell lymphomas. We then compared these sequences, and another 415 RIS sequences previously cloned from BXH2 myeloid leukemias and from a few AKXD lymphomas, against the recently assembled mouse genome sequence. These studies identified 152 loci that are targets of retroviral integration in more than one tumor (common retroviral integration sites, CISs) and therefore likely to encode a cancer gene. Thirty-six CISs encode genes that are known or predicted to be genes involved in human cancer or their homologs, whereas others encode candidate genes that have not yet been examined for a role in human cancer. Our studies demonstrate the power of retroviral tagging for cancer gene discovery in the post-genome era and indicate a largely unrecognized complexity in mouse and presumably human cancer.
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