Pyrosequencing evaluation of low-frequency KRAS mutant alleles for EGF receptor therapy selection in metastatic colorectal carcinoma

Author:

Natalicchio Maria Iole1,Improta Giuseppina2,Zupa Angela2,Cursio Olga Elisabetta3,Stampone Emanuela1,Possidente Luciana2,Teresa Gerardi Assunta Maria4,Vita Giulia5,Martini Maurizio6,Cassano Alessandra3,Piccoli Claudia7,Romito Sante8,Aieta Michele9,Antonetti Raffaele1,Barone Carlo3,Landriscina Matteo4

Affiliation:

1. Molecular Biology Laboratory, Riuniti Hospital, Foggia, Italy

2. Laboratory of Clinical Research & Molecular Diagnostics, IRCCS, Referral Cancer Center of Basilicata, Rionero in Vulture (PZ), Italy

3. Medical Oncology Unit, Catholic University, Rome, Italy

4. Medical Oncology Unit, Department of Medical & Surgical Sciences, University of Foggia, Foggia, Italy

5. Pathology Unit, IRCCS, Referral Cancer Center of Basilicata, Rionero in Vulture (PZ), Italy

6. Pathology Unit, Catholic University of Sacred Heart, Rome, Italy

7. Department of Clinical & Experimental Medicine, University of Foggia, Italy

8. Medical Oncology Unit, Riuniti Hospital, Foggia, Italy

9. Medical Oncology Unit, IRCCS, Referral Cancer Center of Basilicata, Rionero in Vulture (PZ), Italy

Abstract

ABSTRACT:  Aim: To evaluate whether pyrosequencing (PS) improves the KRAS mutational status predictive value. Patients & methods: A retrospective analysis of KRAS mutations by PS and direct sequencing (DS) in 192 metastatic colorectal carcinomas (mCRCs), subgrouped in 51 KRAS mutated at PS and 141 KRAS wild-type at DS. Results: DS failed to detect low-frequency KRAS mutations in four out of 51 mCRCs, whereas PS detected 12 additional low-frequency KRAS mutations in 141 mCRCs KRAS wild-type at DS. After reanalyzing by PS 97 KRAS wild-type tumors treated with anti-EGF receptor (EGFR) antibodies, nine additional mutations were revealed in nonresponders, whereas none of responders exhibited a KRAS-mutated genotype. Of note, KRAS-mutated tumors upon PS showed a worst progression-free survival after EGFR therapy. Finally, PS allowed the detection of additional NRAS, BRAF and exon 20 PIK3CA mutations mostly in KRAS wild-type mCRCs resistant to EGFR therapy. Conclusion: PS detection of low-frequency mutations may improve the KRAS predictive value for EGFR therapy selection.

Publisher

Future Medicine Ltd

Subject

Cancer Research,Oncology,General Medicine

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