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Naked Mole-Rat, a Rodent with an Apolipoprotein A-I Dimer.
Citation | “Naked Mole-Rat, A Rodent With An Apolipoprotein A-I Dimer.”. Lipids. . |
Center | UCSD-UCLA |
Author | Don L Puppione, Denise P Tran, Muhammad A Zenaidee, Sarada Charugundla, Julian P Whitelegge, Rochelle Buffenstein |
Keywords | Homodimer, Mass spectrometry, Rodentia, apoA-I, ApoE, hypoHDL |
Abstract |
A variety of rodents have been used as experimental animals in metabolic studies of plasma lipids and lipoproteins. These studies have included understanding the functional role of apolipoprotein A-I, the major protein on the surface of HDL. Reviewing the genomic database for entries for rodent apoA-I genes, it was discovered that the naked mole-rat (Heterocephalus glaber) gene encoded a protein with a cysteine at residue 28. Previously, two cases have been reported in which human heterozygotes had apoA-I with cysteine at residues 173 (apoA-I Milano) or at 151 (apoA-I Paris). Interestingly, both groups, in spite of having low levels of HDL and moderately elevated plasma triacylglycerols, had no evidence of cardiovascular disease. Moreover, the presence of the cysteine enabled the apoA-I to form both homodimers and heterodimers. Prior to this report, no other mammalian apoA-I has been found with a cysteine in its sequence. In addition, the encoded naked mole-rat protein had different amino acids at sites that were conserved in all other mammals. These differences resulted in naked mole-rat apoA-I having an unexpected neutral pI value, whereas other mammalian apoA-I have negative pI values. To verify these sequence differences and to determine if the N-terminal location of C28 precluded dimer formation, we conducted mass spectrometry analyses of apoA-I and other proteins associated with HDL. Consistent with the genomic data, our analyses confirmed the presence of C28 and the formation of a homodimer. Analysis of plasma lipids surprisingly revealed a profile similar to the human heterozygotes. |
Year of Publication |
2020
|
Journal |
Lipids
|
Date Published |
12/2020
|
ISSN Number |
1558-9307
|
DOI |
10.1002/lipd.12286
|
Alternate Journal |
Lipids
|
PMID |
33336429
|
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