Literature DB >> 6861155

Production and molecular size heterogeneity of immunoreactive gastrin-releasing peptide in fetal and adult lungs and primary lung tumors.

K Yamaguchi, K Abe, T Kameya, I Adachi, S Taguchi, K Otsubo, N Yanaihara.   

Abstract

Gastrin-releasing peptide (GRP) is known to be a bombesin-like peptide present in mammalian tissues. Using GRP radioimmunoassay specific for carboxyl-terminal portion, the immunoreactive GRP (IR-GRP) content of 5 fetal lungs, 38 adult lungs, and 131 primary lung tumors was determined. All fetal lung extracts contained IR-GRP ranging from 31 to 140 ng/g, wet weight. IR-GRP was present in 7 to 21% of normal adult lungs and lung carcinomas other than small-cell carcinoma; the amount was not very large except in two cases of adenocarcinoma, in which 110 and 140 ng/g of IR-GRP were detected. In the case of small-cell carcinoma, IR-GRP was found in 23 of the 31 cases examined (74%), and nine (29%) of these contained large amounts of IR-GRP (100 to 14,000 ng/g). As for carcinoid tumors, IR-GRP was found in five of the 12 cases examined (42%), and large amounts of IR-GRP were detected in two cases (5,100 to 130,000 ng/g). Immunohistochemically, IR-GRP was found in the neuroendocrine cells of fetal lungs and in the tumor cells of primary lung tumors. When these tissue extracts were examined by bombesin radioimmunoassay that recognizes bombesin but not GRP, they did not contain immunoreactive bombesin, suggesting that IR-GRP in these tissues is more similar to GRP than to bombesin. Sephadex G-50 gel filtration always revealed two peaks of IR-GRP in both fetal lungs and IR-GRP-producing tumors. One was eluted at the position corresponding to that of porcine GRP (Peak 1) and the other, at the position just behind that of porcine GRP (14-27) (Peak 2). In the five fetal lungs, Peak 2 comprised more than 83% of the total IR-GRP. In the 12 IR-GRP-producing tumors examined, the ratio of these two peaks differed from case to case. Our data indicate that IR-GRP, which is present in fetal lung, is often produced by primary lung tumors, especially by small-cell carcinoma and carcinoid tumor, with molecular size heterogeneity.

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Year:  1983        PMID: 6861155

Source DB:  PubMed          Journal:  Cancer Res        ISSN: 0008-5472            Impact factor:   12.701


  30 in total

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2.  Pancreatic endocrine tumours associated with WDHA syndrome. An immunohistochemical and electron microscopic study.

Authors:  A Ooi; T Kameya; M Tsumuraya; K Yamaguchi; K Abe; Y Shimosato; N Yanaihara
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3.  Progastrin-releasing peptide as a diagnostic and therapeutic biomarker of small cell lung cancer.

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4.  Bronchial carcinoids: an analysis of 91 cases.

Authors:  H Mårtensson; G Böttcher; G Hambraeus; F Sundler; H Willen; A Nobin
Journal:  World J Surg       Date:  1987-06       Impact factor: 3.352

5.  Expression of the C-terminal peptide of human pro-bombesin in 361 lung endocrine tumours, a reliable marker and possible prognostic indicator for small cell carcinoma.

Authors:  Q A Hamid; B J Addis; D R Springall; N B Ibrahim; M A Ghatei; S R Bloom; J M Polak
Journal:  Virchows Arch A Pathol Anat Histopathol       Date:  1987

6.  Immunohistochemical examination of lung cancers using monoclonal antibodies reacting with sialosylated Lewisx and sialosylated Lewisa.

Authors:  K Kasai; T Kameya; T Okuda; P I Terasaki; Y Iwaki
Journal:  Virchows Arch A Pathol Anat Histopathol       Date:  1986

7.  Gastrin releasing peptide is a selective mitogen for small cell lung carcinoma in vitro.

Authors:  S Weber; J E Zuckerman; D G Bostwick; K G Bensch; B I Sikic; T A Raffin
Journal:  J Clin Invest       Date:  1985-01       Impact factor: 14.808

Review 8.  Signal transduction pathways: new targets in oncology.

Authors:  R K Sweeb; J H Beijnen
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9.  Gastrin-releasing peptide, a mammalian analog of bombesin, is present in human neuroendocrine lung tumors.

Authors:  D G Bostwick; K A Roth; C J Evans; J D Barchas; K G Bensch
Journal:  Am J Pathol       Date:  1984-11       Impact factor: 4.307

10.  Peptide hormone production by adenocarcinomas of the lung; its morphologic basis and histogenetic considerations.

Authors:  T Kameya; Y Shimosato; T Kodama; M Tsumuraya; T Koide; K Yamaguchi; K Abe
Journal:  Virchows Arch A Pathol Anat Histopathol       Date:  1983
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