Three different fibronectin mRNAs arise by alternative splicing within the coding region

Jean E. Schwarzbauer; John W. Tamkun; Ihor R. Lemischka; Richard O. Hynes

Three different fibronectin mRNAs arise by alternative splicing within the coding region

Jean E. Schwarzbauer, John W. Tamkun, Ihor R. Lemischka, Richard O. Hynes

Research output: Contribution to journal › Article › peer-review

Abstract

We report the isolation of cDNA clones for fibronectin from a rat liver library prepared in the expression vector, λgt11. Restriction mapping and DNA sequencing of these clones establish the sequence of the C-terminal 35% of rat fibronectin, covering the cell-, heparin-, and fibrin-binding domains. The cell- and heparin-binding regions have homologous repeating sequences. Based on the sequence data and S1 nuclease mapping, we conclude that there are at least three different fibronectin mRNAs in rat liver which differ in coding potential. The three RNAs appear to arise by alternative splicing within the coding region and are probably all encoded by a single gene. The implications of these results for the structure and function of fibronectin and the differences between various types of fibronectin are discussed. © 1983.

Original language	English
Pages (from-to)	421-431
Number of pages	10
Journal	Cell
Volume	35
Issue number	2
Publication status	Published - Dec 1983

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title = "Three different fibronectin mRNAs arise by alternative splicing within the coding region",

abstract = "We report the isolation of cDNA clones for fibronectin from a rat liver library prepared in the expression vector, λgt11. Restriction mapping and DNA sequencing of these clones establish the sequence of the C-terminal 35% of rat fibronectin, covering the cell-, heparin-, and fibrin-binding domains. The cell- and heparin-binding regions have homologous repeating sequences. Based on the sequence data and S1 nuclease mapping, we conclude that there are at least three different fibronectin mRNAs in rat liver which differ in coding potential. The three RNAs appear to arise by alternative splicing within the coding region and are probably all encoded by a single gene. The implications of these results for the structure and function of fibronectin and the differences between various types of fibronectin are discussed. {\textcopyright} 1983.",

author = "Schwarzbauer, {Jean E.} and Tamkun, {John W.} and Lemischka, {Ihor R.} and Hynes, {Richard O.}",

year = "1983",

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language = "English",

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T1 - Three different fibronectin mRNAs arise by alternative splicing within the coding region

AU - Schwarzbauer, Jean E.

AU - Tamkun, John W.

AU - Lemischka, Ihor R.

AU - Hynes, Richard O.

PY - 1983/12

Y1 - 1983/12

N2 - We report the isolation of cDNA clones for fibronectin from a rat liver library prepared in the expression vector, λgt11. Restriction mapping and DNA sequencing of these clones establish the sequence of the C-terminal 35% of rat fibronectin, covering the cell-, heparin-, and fibrin-binding domains. The cell- and heparin-binding regions have homologous repeating sequences. Based on the sequence data and S1 nuclease mapping, we conclude that there are at least three different fibronectin mRNAs in rat liver which differ in coding potential. The three RNAs appear to arise by alternative splicing within the coding region and are probably all encoded by a single gene. The implications of these results for the structure and function of fibronectin and the differences between various types of fibronectin are discussed. © 1983.

AB - We report the isolation of cDNA clones for fibronectin from a rat liver library prepared in the expression vector, λgt11. Restriction mapping and DNA sequencing of these clones establish the sequence of the C-terminal 35% of rat fibronectin, covering the cell-, heparin-, and fibrin-binding domains. The cell- and heparin-binding regions have homologous repeating sequences. Based on the sequence data and S1 nuclease mapping, we conclude that there are at least three different fibronectin mRNAs in rat liver which differ in coding potential. The three RNAs appear to arise by alternative splicing within the coding region and are probably all encoded by a single gene. The implications of these results for the structure and function of fibronectin and the differences between various types of fibronectin are discussed. © 1983.

M3 - Article

C2 - 6317187

SN - 1097-4172

VL - 35

SP - 421

EP - 431

JO - Cell

JF - Cell

IS - 2

ER -

Three different fibronectin mRNAs arise by alternative splicing within the coding region

Abstract

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