KIT (CD117) Expression in a Subset of Non-Small Cell Lung Carcinoma (NSCLC) Patients
Author(s) -
Albert D. Donnenberg,
Ludovic Zimmerlin,
Rodney J. Landreneau,
James D. Luketich,
Vera S. Donnenberg
Publication year - 2012
Publication title -
plos one
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 0.99
H-Index - 332
ISSN - 1932-6203
DOI - 10.1371/journal.pone.0052885
Subject(s) - cd117 , pathology , flow cytometry , cd34 , cytokeratin , cd90 , cd44 , cancer research , biology , medicine , immunohistochemistry , cell , stem cell , microbiology and biotechnology , genetics
We have previously described the expression of CD44, CD90, CD117 and CD133 in NSCLC tumors, adjacent normal lung, and malignant pleural effusions (MPE). Here we describe the unique subset of tumors expressing CD117 (KIT), a potential therapeutic target. Tumor and adjacent tissue were collected from 58 patients. Six MPE were obtained before therapy. Tissue was paraffin embedded for immunofluorescent microscopy, disaggregated and stained for flow cytometry or cryopreserved for later culture. The effect of imatinib on CD117 high /KIT+ tumors was determined on first passage cells; absolute cell counts and flow cytometry were readouts for drug sensitivity of cell subsets. Primary tumors divided into KIT neg and KIT + by immunofluorescence. By more sensitive flow cytometric analysis, CD117+ cytokeratin+ cells were detected in all tissues (1.1% of cytokeratin+ cells in normal lung, 1.29% in KIT “negative” tumors, 40.7% in KIT + tumors, and 0.4% in MPE). In KIT + /CD117 high , but not KIT + /CD117 low tumors, CD117 was overexpressed 3.1-fold compared to normal lung. Primary cultures of CD117 high tumors were sensitive to imatinib (5 µM) in short term culture. We conclude that NSCLC tumors divide into CD117 low and CD117 high . Overexpression of CD117 in CD117 high NSCLC supports exploring KIT as a therapeutic target in this subset of patients.
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