Literature DB >> 26862952

NRASQ61R Mutation-specific Immunohistochemistry is Highly Specific for Either NRASQ61R or KRASQ61R Mutation in Colorectal Carcinoma.

John Turchini1, Juliana Andrici, Loretta Sioson, Adele Clarkson, Nicole Watson, Christopher W Toon, Phillip Shepherd, Daniel Ng, Amanda Dixon-McIver, Paul Oei, Anthony J Gill.   

Abstract

Anti-epidermal growth factor receptor-targeted therapy is only indicated in RAS wild-type colorectal carcinomas (CRCs). It is recommended that both NRAS and KRAS mutation testing to be performed before a CRC is considered RAS wild-type. Given that mutation-specific immunohistochemistry (IHC) has been shown to be sensitive and specific for the detection of NRAS mutations in melanoma, we assessed the specificity of NRAS mutation-specific IHC in CRC. IHC was performed on tissue microarrays containing 2823 consecutive CRC undergoing surgery with curative intent using a novel mutation-specific antibody to the protein produced by the NRAS mutation (clone SP174). Tissue microarrays were assessed by 2 observers and all IHC-positive or equivocal cases were repeated on whole sections to confirm the result. Positive cases then underwent molecular testing by matrix-assisted laser desorption/ionization-time of flight polymerase chain reaction. In total, 22 of 2823 (0.8%) CRCs demonstrated confirmed positive staining with complete interobserver concordance. RAS mutations were confirmed in all IHC-positive CRCs. In total, 11 cases harbored the NRASQ61R mutation. Surprisingly, 11 cases demonstrated the KRASQ61R mutation. We conclude that mutation-specific IHC with this currently available NRASQ61R antibody is highly specific for the presence of either NRASQ61R or KRASQ61R mutations in CRC. We caution that we did not assess the sensitivity of IHC and that this antibody does not detect other RAS mutations. Therefore, negative staining does not exclude a clinically significant RAS mutation. However, positive staining confirms the presence of an NRASQ61R or KRASQ61R mutation without the need for further molecular testing.

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Year:  2017        PMID: 26862952     DOI: 10.1097/PAI.0000000000000333

Source DB:  PubMed          Journal:  Appl Immunohistochem Mol Morphol        ISSN: 1533-4058


  5 in total

1.  SP174 Antibody Lacks Specificity for NRAS Q61R and Cross-Reacts With HRAS and KRAS Q61R Mutant Proteins in Malignant Melanoma.

Authors:  Anna Felisiak-Goląbek; Shingo Inaguma; Artur Kowalik; Bartosz Wasąg; Zeng-Feng Wang; Sebastian Zięba; Liliana Pięciak; Janusz Ryś; Janusz Kopczynski; Maarit Sarlomo-Rikala; Stanislaw Góźdź; Jerzy Lasota; Markku Miettinen
Journal:  Appl Immunohistochem Mol Morphol       Date:  2018-01

Review 2.  Personal Mutanomes Meet Modern Oncology Drug Discovery and Precision Health.

Authors:  Feixiong Cheng; Han Liang; Atul J Butte; Charis Eng; Ruth Nussinov
Journal:  Pharmacol Rev       Date:  2018-12-13       Impact factor: 25.468

3.  Medullary Thyroid Carcinoma: Survival Analysis and Evaluation of Mutation-Specific Immunohistochemistry in Detection of Sporadic Disease.

Authors:  S Jayakody; J Reagh; M Bullock; A Aniss; R Clifton-Bligh; D Learoyd; B Robinson; L Delbridge; S Sidhu; A J Gill; M Sywak
Journal:  World J Surg       Date:  2018-05       Impact factor: 3.352

4.  NRAS Q61R immunohistochemical staining in thyroid pathology: sensitivity, specificity and utility.

Authors:  Maelle Saliba; Nora Katabi; Snjezana Dogan; Bin Xu; Ronald A Ghossein
Journal:  Histopathology       Date:  2021-08-03       Impact factor: 7.778

5.  The Diagnostic Utility of RAS Q61R Mutation-specific Immunohistochemistry in Epithelial-Myoepithelial Carcinoma.

Authors:  Masato Nakaguro; Maki Tanigawa; Hideaki Hirai; Yoshinari Yamamoto; Makoto Urano; Reisuke H Takahashi; Aoi Sukeda; Yuki Okumura; Shogo Honda; Koichiro Tasaki; Akira Shimizu; Kiyoaki Tsukahara; Yuichiro Tada; Jun Matsubayashi; William C Faquin; Peter M Sadow; Toshitaka Nagao
Journal:  Am J Surg Pathol       Date:  2021-07-01       Impact factor: 6.298

  5 in total

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