Alternative splicing of exon 3 of the human growth hormone receptor is the result of an unusual genetic polymorphism

被引：58

作者：

StallingsMann, ML

Ludwiczak, RL

Klinger, KW

Rottman, F

机构：

[1] CASE WESTERN RESERVE UNIV, SCH MED, DEPT MOL BIOL & MICROBIOL, CLEVELAND, OH 44106 USA

[2] INTEGRATED GENET INC, FRAMINGHAM, MA 01701 USA

来源：

PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA | 1996年 / 93卷 / 22期

关键词：

D O I：

10.1073/pnas.93.22.12394

中图分类号：

O [数理科学和化学]; P [天文学、地球科学]; Q [生物科学]; N [自然科学总论];

学科分类号：

07 ; 0710 ; 09 ;

摘要：

Two isoforms of the human growth hormone receptor (hGHR), which differ in the presence (hGHRwt) or absence (hGHRd3) of exon 3, are expressed in the placenta, Specifically, three expression patterns are observed: only hGHRwt, only hGHRd3, or an approximately 1:1 combination of both isoforms. We investigated several potential regulatory mechanisms which might account for the expression of the hGHR isoforms, The frequency of hGHRd3 expression did not change when placentas from differing stages of gestation were examined, suggesting splicing was not developmentally regulated. However, when hGHR isoform expression patterns were examined in each component of a given placenta, it was evident that alternative splicing of exon 3 is individual-specific. Surprisingly, the individual-specific regulation of hGHR isoforms appears to be the result of a polymorphism in the hGHR gene. We analyzed hGHRwt and hGHRd3 expression in Hutterite pedigrees, and our results are consistent with a simple Mendelian inheritance of two differing alleles in which exon 3 is spliced in an ''all-or-none'' fashion. We conclude the alternative splicing of exon 3 in hGHR transcripts is the result of an unusual polymorphism which significantly alters splicing of the hGHR transcript and that the relatively high frequency (approximate to 10%) of homozygous hGHRd3 expression suggests the possibility it may play a role in polygenic determined events.

引用

页码：12394 / 12399

页数：6

共 27 条

[1] A SYSTEMATIC MUTATIONAL ANALYSIS OF HORMONE-BINDING DETERMINANTS IN THE HUMAN GROWTH-HORMONE RECEPTOR
BASS, SH
MULKERRIN, MG
WELLS, JA
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1991, 88 (10) : 4498 - 4502
[2] A HOT-SPOT OF BINDING-ENERGY IN A HORMONE-RECEPTOR INTERFACE
CLACKSON, T
WELLS, JA
[J]. SCIENCE, 1995, 267 (5196) : 383 - 386
[3] DECOUVELAERE C, 1995, CELL GROWTH DIFFER, V6, P477
[4] EXPRESSION OF 2 ISOFORMS OF THE HUMAN GROWTH-HORMONE RECEPTOR IN NORMAL LIVER AND HEPATOCARCINOMA
ESPOSITO, N
PATERLINI, P
KELLY, PA
POSTELVINAY, MC
FINIDORI, J
[J]. MOLECULAR AND CELLULAR ENDOCRINOLOGY, 1994, 103 (1-2) : 13 - 20
[5] ALTERNATIVE SPLICE-SITE SELECTION IN THE HUMAN GROWTH-HORMONE GENE TRANSCRIPT AND SYNTHESIS OF THE 20 KDA ISOFORM - ROLE OF HIGHER-ORDER TRANSCRIPT STRUCTURE
ESTES, PA
URBANEK, M
RAY, J
LIEBHABER, SA
COOKE, NE
[J]. ACTA PAEDIATRICA, 1994, 83 : 42 - 48
[6] GEORGE DL, 1981, HUM GENET, V57, P138
[7] CHARACTERIZATION OF THE HUMAN GROWTH-HORMONE RECEPTOR GENE AND DEMONSTRATION OF A PARTIAL GENE DELETION IN 2 PATIENTS WITH LARON-TYPE DWARFISM
GODOWSKI, PJ
LEUNG, DW
MEACHAM, LR
GALGANI, JP
HELLMISS, R
KERET, R
ROTWEIN, PS
PARKS, JS
LARON, Z
WOOD, WI
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1989, 86 (20) : 8083 - 8087
[8] Inoue Kunio, 1995, Gene Expression, V4, P177
[9] Inhibition by SR proteins of splicing of a regulated adenovirus pre-mRNA
Kanopka, A
Muhlemann, O
Akusjarvi, G
[J]. NATURE, 1996, 381 (6582) : 535 - 538
[10] Keller M. A., 1995, Gene Expression, V4, P217

← 1 2 3 →