Concurrent Mutations of K-ras Oncogene at Codons 12 and 22 in Colon Cancer

doi:10.1093/jjco/hyf043

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Japanese Journal of Clinical Oncology 32:219-221 (2002)
© 2002 Foundation for Promotion of Cancer Research

Concurrent Mutations of K-ras Oncogene at Codons 12 and 22 in Colon Cancer

Yasuyuki Miyakura¹^,2, Kokichi Sugano², Noriko Fukayama², Fumio Konishi³ and Hideo Nagai¹^,+

¹ Department of Surgery, Jichi Medical School, Minami Kawachi, Tochigi, ² Oncogene Research Unit/Cancer Prevention Unit, Tochigi Cancer Center Research Institute, Utsunomiya and ³ Department of Surgery, Jichi Medical School Omiya Medical Center, Saitama, Japan

K-ras mutation is the most common oncogenic alteration in varioushuman cancers including colorectal carcinomas. Point mutationshave the potential to activate the K-ras gene if they occurin the critical coding sequences. Almost all of these mutationshave been localized in codons 12, 13 and 61. We report a caseof colon cancer presenting point mutations at both codons 12and 22 of the K-ras gene. PCR-SSCP and subsequent sequencingrevealed that GGT (glycine, wild-type) to AGT (serine) substitutionat codon 12 and CAG (glutamine, wild-type) to CGG (arginine)substitution at codon 22 occurred in the same allele.

⁺ For reprints and all correspondence: K. Sugano, Oncogene ResearchUnit/Cancer Prevention Unit, Tochigi Cancer Center ResearchInstitute, 4–9–13 Yohnan, Utsunomiya, Tochigi 320-0834,Japan

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