Actin-isoform Pattern As a Marker of Normal or Pathological Smooth-muscle and Fibroblastic Tissues

Overview

Journal Differentiation

Publisher Elsevier

Specialties Cell Biology
Reproductive Medicine

Date 1987 Jan 1

PMID 3596085

Citations 36

Authors

O Skalli

J Vandekerckhove

G Gabbiani

Affiliations

Soon will be listed here.

Abstract

The relative proportions of actin isoforms present in smooth-muscle (SM) and fibroblastic human and non-human tissue extracts were examined by densitometric evaluation of Coomassie-Blue-stained spots in two-dimensional polyacrylamide gel electrophoresis (2D-PAGE) as well as by quantification of radiolabeled actin NH2-terminal peptide spots separated by two-dimensional paper electrophoresis. SM tissues contained alpha- and gamma-SM as well as beta- and gamma-cytoplasmic (CY) actins in different proportions in different organs. Species differences with respect to the ratios of the isoactins were also observed. Moreover, during pregnancy, both human and rat myometrium exhibited a changed actin-isoform pattern, there being an increased proportion of gamma-actin. Analysis of the NH2-terminal peptides showed that, in human myometrium, this was essentially due to an increase in the amount of the gamma-SM isoform. Fibroblastic tissues were found to contain only the beta- and gamma-CY isoforms, the ratio being approximately 2.6:1. Thus, the presence or absence of alpha-actin provides a reliable biochemical criterion for distinguishing between fibroblastic and SM cell populations and/or tissues. This distinction and the evaluation of changes in isoactin ratios may be useful in the study of differentiation as well as physiological and pathological phenomena, and for determining the origin of certain soft-tissue tumours.

Citing Articles

Regulation of actin isoforms in cellular and developmental processes.

Kashina A Semin Cell Dev Biol. 2020; 102:113-121.

PMID: 32001148 PMC: 7214208. DOI: 10.1016/j.semcdb.2019.12.003.

RAAS inhibitors directly reduce diabetes-induced renal fibrosis via growth factor inhibition.

Koszegi S, Molnar A, Lenart L, Hodrea J, Balogh D, Lakat T J Physiol. 2018; 597(1):193-209.

PMID: 30324679 PMC: 6312411. DOI: 10.1113/JP277002.

ACTA2 mutation and postpartum hemorrhage: a case report.

Cooper K, Brown S BMC Med Genet. 2017; 18(1):143.

PMID: 29202781 PMC: 5715517. DOI: 10.1186/s12881-017-0505-5.

Single Stem Cell Imaging and Analysis Reveals Telomere Length Differences in Diseased Human and Mouse Skeletal Muscles.

Tichy E, Sidibe D, Tierney M, Stec M, Sharifi-Sanjani M, Hosalkar H Stem Cell Reports. 2017; 9(4):1328-1341.

PMID: 28890163 PMC: 5639167. DOI: 10.1016/j.stemcr.2017.08.003.

Smoothelin, a new marker to determine the origin of liver fibrogenic cells.

Lepreux S, Guyot C, Billet F, Combe C, Balabaud C, Bioulac-Sage P World J Gastroenterol. 2014; 19(48):9343-50.

PMID: 24409061 PMC: 3882407. DOI: 10.3748/wjg.v19.i48.9343.