Comparative Genomic Analysis of Primary Versus Metastatic Colorectal Carcinomas

Overview

Journal J Clin Oncol

Specialty Oncology

Date 2012 Jun 6

PMID 22665543

Citations 137

Authors

Efsevia Vakiani

Manickam Janakiraman

Ronglai Shen

Rileen Sinha

Zhaoshi Zeng

Jinru Shia

Andrea Cercek

Nancy Kemeny

Michael DAngelica

Agnes Viale

Adriana Heguy

Philip Paty

Timothy A Chan

Leonard B Saltz

Martin Weiser

David B Solit

Affiliations

Soon will be listed here.

Abstract

Purpose: To compare the mutational and copy number profiles of primary and metastatic colorectal carcinomas (CRCs) using both unpaired and paired samples derived from primary and metastatic disease sites.

Patients And Methods: We performed a multiplatform genomic analysis of 736 fresh frozen CRC tumors from 613 patients. The cohort included 84 patients in whom tumor tissue from both primary and metastatic sites was available and 31 patients with pairs of metastases. Tumors were analyzed for mutations in the KRAS, NRAS, BRAF, PIK3CA, and TP53 genes, with discordant results between paired samples further investigated by analyzing formalin-fixed, paraffin-embedded tissue and/or by 454 sequencing. Copy number aberrations in primary tumors and matched metastases were analyzed by comparative genomic hybridization (CGH).

Results: TP53 mutations were more frequent in metastatic versus primary tumors (53.1% v 30.3%, respectively; P < .001), whereas BRAF mutations were significantly less frequent (1.9% v 7.7%, respectively; P = .01). The mutational status of the matched pairs was highly concordant (> 90% concordance for all five genes). Clonality analysis of array CGH data suggested that multiple CRC primary tumors or treatment-associated effects were likely etiologies for mutational and/or copy number profile differences between primary tumors and metastases.

Conclusion: For determining RAS, BRAF, and PIK3CA mutational status, genotyping of the primary CRC is sufficient for most patients. Biopsy of a metastatic site should be considered in patients with a history of multiple primary carcinomas and in the case of TP53 for patients who have undergone interval treatment with radiation or cytotoxic chemotherapies.

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