| Literature DB >> 34998840 |
Franziska Erlmeier1, Benedict Bruecher2, Christine Stöhr3, Edwin Herrmann2, Iris Polifka3, Abbas Agaimy3, Lutz Trojan4, Philipp Ströbel5, Frank Becker6, Christian Wülfing2, Peter Barth7, Michael Stöckle6, Michael Staehler8, Christian Stief8, Axel Haferkamp9, Markus Hohenfellner9, Stephan Macher-Göppinger10, Bernd Wullich11, Joachim Noldus12, Walburgis Brenner13, Frederik C Roos14, Bernhard Walter11, Wolfgang Otto15, Maximilian Burger15, Andres Jan Schrader2, Arndt Hartmann3, Yvonne Mondorf16, Philipp Ivanyi16, Marie Mikuteit17, Sandra Steffens2.
Abstract
The tyrosine-protein kinase c-Met plays a decisive role in numerous cellular processes, as a proto-oncogene that supports aggressive tumor behavior. It is still unknown whether c-Met could be relevant for prognosis of papillary RCC (pRCC). Specimen collection was a collaboration of the PANZAR consortium. Patients' medical history and tumor specimens were collected from 197 and 110 patients with type 1 and 2 pRCC, respectively. Expression of cMET was determined by immunohistochemistry. In total, cMET staining was evaluable in of 97 of 197 type 1 and 63 of 110 type 2 pRCC cases. Five-year overall survival revealed no significant difference in dependence of cMET positivity (cMET- vs. cMET+: pRCC type 1: 84.8% vs. 80.3%, respectively [p = 0.303, log-rank]; type 2: 71.4% vs. 64.4%, respectively [p = 0.239, log-rank]). Interestingly, the subgroup analyses showed a significant difference for cMET expression in T stage and metastases of the pRCC type 2 (p = 0.014, p = 0.022, chi-square). The cMET-positive type 2 collective developed more metastases than the cMET-negative cohort (pRCC type 2 M+: cMET-: 2 [4.3%] vs. cMET+: 12 [19%]). cMET expression did not qualify as a prognostic marker in pRCC for overall survival.Entities:
Keywords: Outcome; Papillary renal cell carcinoma; Prognosis; Survival; cMET
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Year: 2022 PMID: 34998840 DOI: 10.1016/j.humpath.2021.12.007
Source DB: PubMed Journal: Hum Pathol ISSN: 0046-8177 Impact factor: 3.466