Affiliation:
1. the Department of Medicine III, University of Tokyo (Japan) School of Medicine.
Abstract
Accumulating evidence has suggested that homeodomain-containing proteins play critical roles in regulating the tissue-specific gene expression essential for tissue differentiation and in determining the temporal and spatial patterns of development. In order to elucidate the mechanisms of human heart development, we have isolated a human homologue of the murine cardiac homeobox gene
Csx
(also called
Nkx-2.5)
and denoted it as
CSX1.
The amino acid sequence of the
CSX1
homeodomain is 100% and 67% identical to that of murine
Csx/Nkx-2.5
and
Drosophila tinman,
respectively.
CSX1
has at least three isoforms generated by an alternative splicing mechanism. One of these isoforms (
CSX1a
) encodes a protein of ≈35 kD that possesses the homeodomain, whereas the other two (
CSX1b
and
CSX1c
) encode a truncated protein of ≈12 kD that is identical to the
CSX1a
protein at the amino-terminal 112 amino acids but lacks the homeodomain. Northern blot analysis showed that
CSX1
transcripts are abundantly expressed in both fetal and adult hearts, but no signal was detected in other human tissues examined. Amplification of each isoform by reverse transcriptase–polymerase chain reaction revealed that all of the three isoforms are expressed in fetal and adult hearts and that the homeobox-containing isoform
CSX1a
is most abundant. The homeodomain-containing protein encoded by
CSX1a
binds to
Csx/Nkx-2.5
binding sequences and transactivates the sequence-containing luciferase reporter gene. Unexpectedly, the homeodomain-lacking protein encoded by
CSX1b
also transactivates the reporter gene, although
CSX1b
does not bind to the
Csx
/
Nkx-2.5
binding sequences. The highly conserved homeodomain sequence in evolution and the restricted expression in the heart suggest that
CSX1
plays an important role in the development and differentiation of the human heart and that there may be two different mechanisms in transcriptional regulation by the
CSX1
protein, homeodomain-dependent and -independent mechanisms.
Publisher
Ovid Technologies (Wolters Kluwer Health)
Subject
Cardiology and Cardiovascular Medicine,Physiology
Cited by
68 articles.
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