Immunohistochemistry - microarray analysis of patients with peritoneal metastases of appendiceal or colorectal origin

Danielle E Green; Thejus T Jayakrishnan; Michael Hwang; Sam G Pappas; T Clark Gamblin; Kiran K Turaga

doi:10.3389/fsurg.2014.00050

Immunohistochemistry - microarray analysis of patients with peritoneal metastases of appendiceal or colorectal origin

Front Surg. 2015 Jan 5:1:50. doi: 10.3389/fsurg.2014.00050. eCollection 2014.

Authors

Danielle E Green¹, Thejus T Jayakrishnan¹, Michael Hwang¹, Sam G Pappas², T Clark Gamblin¹, Kiran K Turaga¹

Affiliations

¹ Division of Surgical Oncology, Department of Surgery, Medical College of Wisconsin , Milwaukee, WI , USA.
² Division of Surgical Oncology, Department of Surgery, Loyola University Medical Center , Maywood, IL , USA.

Abstract

Background: The value of immunohistochemistry (IHC)-microarray analysis of pathological specimens in the management of patients is controversial, although preliminary data suggest potential benefit. We describe the characteristics of patients undergoing a commercially available IHC-microarray method in patients with peritoneal metastases (PM) and the feasibility of this technique in this population.

Methods: We retrospectively analyzed consecutive patients with pathologically confirmed PM from appendiceal or colorectal primary who underwent Caris Molecular Intelligence(™) testing. IHC, microarray, FISH, and mutational analysis were included and stratified by Peritoneal Carcinomatosis Index (PCI) score, histology, and treatment characteristics. Statistical analysis was performed using non-parametric tests.

Results: Our study included 5 patients with appendiceal and 11 with colorectal PM. The median age of patients was 51 (IQR 39-65) years, with 11 (68%) female. The median PCI score of the patients was 17 (IQR 10-25). Hyperthermic intra-peritoneal chemoperfusion was performed in 4 (80%) patients with appendiceal primary tumors and 4 (36%) with colorectal primary. KRAS mutations were encountered in 40% of appendiceal vs. 30% colorectal tumors, while BRAF mutations were seen in 40% of colorectal PM and none of the patients with appendiceal PM (p = 0.06). IHC biomarker expression was not significantly different between the two primaries. Sufficient tumor for microarray analysis was found in 44% (n = 7) patients, which was not associated with previous use of chemotherapy (p > 0.20 for 5-FU/LV, Irinotecan and Oxaliplatin).

Conclusion: In a small sample of patients with PM, the feasibility and results of IHC-microarray staining based on a commercially available test is reported. The apparent high incidence of the BRAF mutation in patients with PM may potentially offer opportunities for novel therapeutics and suggest that IHC-microarray is a method that can be used in this population.

Keywords: DNA mutational analysis; appendiceal neoplasms; colorectal neoplasms; immunohistochemistry; microarray analysis; peritoneal neoplasms.