Villin: a cytoskeletal protein and a differentiation marker expressed in some human adenocarcinomas.

6533b820fe1ef96bd127a4fc

RESEARCH PRODUCT

Villin: a cytoskeletal protein and a differentiation marker expressed in some human adenocarcinomas.

Daniel Louvard Roland Moll Sylvie Robine Brigitte Dudouet

subject

Pathology medicine.medical_specialty Fluorescent Antibody Technique macromolecular substances Chromophobe cell Adenocarcinoma digestive system Metastasis Immunoenzyme Techniques medicine Biomarkers Tumor Humans biology Microfilament Proteins Antibodies Monoclonal medicine.disease Primary tumor Microscopy Fluorescence Dysplasia biology.protein Immunologic Techniques Adenocarcinoma Immunohistochemistry Villin Carrier Proteins Clear cell

description

We studied the expression of villin, a microfilament-associated, actin-binding protein typical of brush-border microvilli, in a variety of human carcinomas by applying immunofluorescence microscopy to frozen sections and immunoblotting methods to tissue extracts using a rabbit antiserum and a monoclonal antibody specific for villin. All of the 24 primary and metastatic colorectal adenocarcinomas tested were uniformly and strongly positive for villin, with the immunocytochemical labeling concentrated at the luminal cell margin. In poorly differentiated tumor areas, rudimentary tubules were stained. All of the six tubular adenocarcinomas of the stomach studied as well as two adenocarcinomas of the gall bladder and a hepatocellular carcinoma were also villin-positive. Villin was detectable in 12 of 14 adenocarcinomas of the pancreas; in some of these cases, its distribution was heterogeneous. Among 21 renal cell carcinomas investigated, positivity for villin was seen in nine of 13 clear cell tumors (especially those of grade II), and in all four chromophilic cell tumors; however, all four chromophobe cell tumors studied were negative. Four of 11 endometrial but none of nine ovarian carcinomas were (uniformly or focally) villin positive. Of 18 adenocarcinomas of the lung studied, one was uniformly and four focally positive for villin, while the remainder were negative. All of the other epithelial tumors studied, including 12 adenocarcinomas of the breast and seven epithelial or biphasic pleural mesotheliomas, were villin negative. Our results show that the expression of villin in intestinal epithelial cells is consistently maintained in their corresponding carcinomas, even when the organized brush-border structure has been lost. The presence of villin in some endometrial and pulmonary adenocarcinomas--in contrast to its absence in the respective normal epithelia--suggests that this protein is newly expressed during hyperplasia, dysplasia, or carcinogenesis. Determining the presence or absence of villin and its immunocytochemical staining pattern in metastatic adenocarcinomas may be of some help in determining the type and site of the primary tumor.

year	journal	country	edition	language
1987-12-01	Virchows Archiv. B, Cell pathology including molecular pathology

10.1007/bf02899208 https://pubmed.ncbi.nlm.nih.gov/2894090