Sequence of mdr3 cDNA encoding a human P-glycoprotein
We have determined the sequence of the human mdr3 gene using cDNA derived from liver RNA. The mdr3 gene codes for a member of a family of membrane proteins, the P-glycoproteins, overproduced in many multi-drug-resistant (MDR) cell lines. Like its relatives, the protein encoded by mdr3 has a deduced...
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Veröffentlicht in: | Gene 1988-11, Vol.71 (2), p.401-411 |
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Zusammenfassung: | We have determined the sequence of the human
mdr3 gene using cDNA derived from liver RNA. The
mdr3 gene codes for a member of a family of membrane proteins, the P-glycoproteins, overproduced in many multi-drug-resistant (MDR) cell lines. Like its relatives, the protein encoded by
mdr3 has a deduced
M
r of 140 000, which is presumably increased by glycosylation after synthesis. The sequence consists of two similar halves, each with a series of six hydrophobic segments that may form a membrane channel. The halves also possess nucleotide-binding consensus sequences, which presumably act as ATPases and drive drug transport. The presumed ATPase domains are all but identical to those of the human
mdr1 gene product [Chen et al., Cell 47 (1986) 381–389]. We attribute this high level of sequence conservation to the repeated gene conversion that is evident from segments in which
mdr1 and
mdr3 differ only in a few silent mutations. Divergence between P-glycoprotein family members is greatest at the N terminus and in the 60 amino acid linker connecting the two halves. In the putative
trans-membrane domains approx. 80% of the amino acids are conserved between the products of
mdr1 and
mdr3. Although the function of
mdr3 is not yet known, its high homology with
mdr1 suggests that it also encodes an efflux pump with broad specificity. |
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ISSN: | 0378-1119 1879-0038 |
DOI: | 10.1016/0378-1119(88)90057-1 |