DOG1 overexpression is associated with mismatch repair deficiency and BRAF mutations but unrelated to cancer progression in colorectal cancer

被引:1
|
作者
Jansen, Kristina [1 ,2 ]
Kluth, Martina [1 ]
Blessin, Niclas C. [1 ]
Hube-Magg, Claudia [1 ]
Neipp, Michael [3 ]
Mofid, Hamid [4 ]
Larusson, Hannes [4 ]
Daniels, Thies [5 ]
Isbert, Christoph [6 ]
Coerper, Stephan [7 ]
Ditterich, Daniel [8 ]
Rupprecht, Holger [9 ]
Goetz, Albert [10 ]
Bernreuther, Christian [1 ]
Sauter, Guido [1 ]
Uhlig, Ria [1 ]
Wilczak, Waldemar [1 ]
Simon, Ronald [1 ]
Steurer, Stefan [1 ]
Burandt, Eike [1 ]
Perez, Daniel [2 ]
Izbicki, Jakob R. [2 ]
Jacobsen, Frank [1 ]
Clauditz, Till S. [1 ]
Marx, Andreas H. [1 ,11 ]
Krech, Till [1 ,12 ]
机构
[1] Univ Med Ctr Hamburg Eppendorf, Inst Pathol, Martinistr 52, D-20246 Hamburg, Germany
[2] Univ Med Ctr Hamburg Eppendorf, Gen Visceral & Thorac Surg Dept & Clin, Hamburg, Germany
[3] Itzehoe Med Ctr, Gen Vasc & Visceral Surg Clin, Itzehoe, Germany
[4] Regio Clin Pinneberg, Gen Visceral Thorac & Vasc Surg Clin, Pinneberg, Germany
[5] Albertinen Hosp, Gen Visceral & Tumor Surg Clin, Hamburg, Germany
[6] Amalie Sieveking Hosp, Dept Gen Gastrointestinal & Colorectal Surg, Hamburg, Germany
[7] Gen Hosp Martha Maria Hosp Nuernberg, Dept Surg, Nurnberg, Germany
[8] Gen Hosp Neustadt Aisch, Dept Surg, Neustadt, Germany
[9] Acad Hosp Neumarkt, Dept Thorac Surg, Neumarkt Oberpfalz, Germany
[10] Gen Hosp Roth, Dept Surg, Roth, Germany
[11] Acad Hosp Fuerth, Dept Pathol, Furth, Germany
[12] Clin Ctr Osnabrueck, Inst Pathol, Osnabruck, Germany
关键词
DOG1; Colon Cancer; Tissue micro array; Immunohistochemistry; INTERSTITIAL-CELLS; GASTRIC-CANCER; TMEM16A; EXPRESSION; ANO1; INHIBITION; EGFR; DOG1/TMEM16A; CONTRIBUTES; ACTIVATION;
D O I
10.14670/HH-18-475
中图分类号
Q2 [细胞生物学];
学科分类号
071009 ; 090102 ;
摘要
Introduction. The transmembrane channel protein DOG1 (Discovered on GIST1) is normally expressed in the gastrointestinal interstitial cells of Cajal and also in gastrointestinal stroma tumors arising from these cells. However, there is also evidence for a relevant role of DOG1 expression in colorectal cancers. This study was undertaken to search for associations between DOG1 expression and colon cancer phenotype and key molecular alterations. Methods. A tissue microarray containing samples from more than 1,800 colorectal cancer patients was analyzed by immunohistochemistry. Results. DOG1 immunostaining was detected in 503 (30.2%) of 1,666 analyzable colorectal cancers and considered weak in 360 (21.6%), moderate in 78 (4.7%), and strong in 65 (3.9%). Strong DOG1 immunostaining was associated with advanced pT stage (p=0.0367) and nodal metastases (p=0.0145) but these associations were not retained in subgroups of 1,135 mismatch repair proficient and 86 mismatch repair deficient tumors. DOG1 positivity was significantly linked to several molecular tumor features including mismatch repair deficiency (p=0.0034), BRAF mutations (p<0.0001), nuclear p53 accumulation (p=0.0157), and PD-L1 expression (p=0.0199) but unrelated to KRAS mutations and the density of tumor infiltrating CD8 positive lymphocytes. Conclusion. Elevated DOG1 expression is frequent in colorectal cancer and significantly linked to important molecular alterations. However, DOG1 overexpression is largely unrelated to histopathological parameters of cancer aggressiveness and may thus not serve as a prognostic parameter for this tumor entity.
引用
收藏
页码:739 / 748
页数:10
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