TY - JOUR
T1 - Cytoskeleton-associated proteins of human lung cancer cells
AU - Bernal, Samuel D.
AU - Chen, Lan Bo
AU - Baylin, Stephen B.
AU - Shaper, Joel H.
AU - Gazdar, Adi F.
PY - 1983/4/1
Y1 - 1983/4/1
N2 - The proteins associated with the cytoskeietal framework of the major forms of lung cancer in culture were analyzed by two-dimensional gel electrophoresis of cytoskeietal framework (CSK) fractions. We have found that (a) small-cell carcinoma (SCC) lines, which differ from non-SCC lung carcinomas (adenocarci-noma, squamous carcinoma, and large-cell undifferentiated carcinoma) in morphology and growth characteristics, had a CSK composition different from that of non-SCC lines. Six separate SCC lines contained protein 1 (Mr 140, 000, pl 5.2), protein 2 (Mr 140.000, pl 5.1), protein 3 (Mr 190, 000, pl 7.6), and protein 4 (Mr190.000, pl 7.5) but lacked protein 5 (Mr 80, 000, pl 6.1), protein 6 (Mr48, 000, pl 5.6), and protein 7 (Mr 55, 000, pl 5.5); four non-SCC lines lacked proteins 1 to 4 but contained proteins 5 to 7. Protein 7 was identified to be vimentin. (b) SCC lines, which have neuroendocrine properties, contained CSK proteins characteristic of neuroblastoma cells. Proteins 1 to 4 were found in all SCC lines, in two neuroblastoma lines, but not in other human cell lines, (c) SCC and non-SCC lines contained protein 8 (Mr 40, 000, pl 5.4) and protein 9 (Mr 48, 000 to 49, 000, pl 6.4), which comigrate with purified keratin. These proteins were also detected in other carcinomas but not in neuroblastoma, leukemia, and fibroblast cell lines, (d) Carcinomas of the lung were distinguishable from other carcinomas by their CSK components. Nonpulmonary carcinomas lacked proteins 1 to 4 which were found in SCC lines and also lacked proteins 5 and 6 found in non-SCC lung cancer cells. The differences in the content of CSK proteins between cell lines were not due to differences in the distribution of a given protein between CSK, soluble, and nuclear fractions. These studies may have biological and clinical importance since SCC has greater metastatic capacity and therapeutic responsiveness than non-SCC lung cancers. In addition, the identification of these CSK proteins by immunohistochemical staining in human lung cancers and normal bronchial epithelium could help clarify the lineage relationships between normal bronchial epithelial cells and the different forms of lung cancer and lead to more precise diagnostic classification of lung cancer biopsy specimens.
AB - The proteins associated with the cytoskeietal framework of the major forms of lung cancer in culture were analyzed by two-dimensional gel electrophoresis of cytoskeietal framework (CSK) fractions. We have found that (a) small-cell carcinoma (SCC) lines, which differ from non-SCC lung carcinomas (adenocarci-noma, squamous carcinoma, and large-cell undifferentiated carcinoma) in morphology and growth characteristics, had a CSK composition different from that of non-SCC lines. Six separate SCC lines contained protein 1 (Mr 140, 000, pl 5.2), protein 2 (Mr 140.000, pl 5.1), protein 3 (Mr 190, 000, pl 7.6), and protein 4 (Mr190.000, pl 7.5) but lacked protein 5 (Mr 80, 000, pl 6.1), protein 6 (Mr48, 000, pl 5.6), and protein 7 (Mr 55, 000, pl 5.5); four non-SCC lines lacked proteins 1 to 4 but contained proteins 5 to 7. Protein 7 was identified to be vimentin. (b) SCC lines, which have neuroendocrine properties, contained CSK proteins characteristic of neuroblastoma cells. Proteins 1 to 4 were found in all SCC lines, in two neuroblastoma lines, but not in other human cell lines, (c) SCC and non-SCC lines contained protein 8 (Mr 40, 000, pl 5.4) and protein 9 (Mr 48, 000 to 49, 000, pl 6.4), which comigrate with purified keratin. These proteins were also detected in other carcinomas but not in neuroblastoma, leukemia, and fibroblast cell lines, (d) Carcinomas of the lung were distinguishable from other carcinomas by their CSK components. Nonpulmonary carcinomas lacked proteins 1 to 4 which were found in SCC lines and also lacked proteins 5 and 6 found in non-SCC lung cancer cells. The differences in the content of CSK proteins between cell lines were not due to differences in the distribution of a given protein between CSK, soluble, and nuclear fractions. These studies may have biological and clinical importance since SCC has greater metastatic capacity and therapeutic responsiveness than non-SCC lung cancers. In addition, the identification of these CSK proteins by immunohistochemical staining in human lung cancers and normal bronchial epithelium could help clarify the lineage relationships between normal bronchial epithelial cells and the different forms of lung cancer and lead to more precise diagnostic classification of lung cancer biopsy specimens.
UR - http://www.scopus.com/inward/record.url?scp=0020645861&partnerID=8YFLogxK
UR - http://www.scopus.com/inward/citedby.url?scp=0020645861&partnerID=8YFLogxK
M3 - Article
C2 - 6299529
AN - SCOPUS:0020645861
SN - 0008-5472
VL - 43
SP - 1798
EP - 1808
JO - Cancer research
JF - Cancer research
IS - 4
ER -