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Gene/Protein
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Target Concepts:
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Query: UMLS:C0162871 (
abdominal aortic aneurysm
)
8,664
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Polyclonal antibodies have been raised against four 16 residue peptides with sequences taken from the C-terminal quarter of the human
cytoplasmic dynein heavy chain
. The sites are downstream from a known microtubule-binding domain associated with the "stalk" that protrudes from the motor domain. The antisera were assayed using bacterially expressed proteins with amino acid sequences taken from the human
cytoplasmic dynein heavy chain
. Every antiserum reacted specifically with the appropriate expressed protein and with pig brain cytoplasmic dynein, whether the protein molecules were denatured on Western blots or were in a folded state. But, whereas three of the four antisera recognized freshly purified cytoplasmic dynein, the fourth reacted only with dynein that had been allowed to denature a little. After affinity purification against the expressed domains, whole IgG molecules and Fab fragments were assayed for their effect on dynein activity in in vitro microtubule-sliding assays. Of the three anti-peptides that reacted with fresh dynein, one inhibited motility but the others did not. The way these peptides are exposed on the surface is compatible with a model whereby the dynein motor domain is constructed from a ring of
AAA
protein modules, with the C-terminal module positioned on the surface that interacts with microtubules. We have tentatively identified an additional
AAA
module in the dynein heavy chain sequence, which would be consistent with a heptameric ring.
...
PMID:Antibodies to cytoplasmic dynein heavy chain map the surface and inhibit motility. 1129 44
Sequence comparisons and structural analyses show that the dynein heavy chain motor subunit is related to the
AAA
family of chaperone-like ATPases. The core structure of the dynein motor unit derives from the assembly of six
AAA
domains into a hexameric ring. In dynein, the first four
AAA
domains contain consensus nucleotide triphosphate-binding motifs, or P-loops. The recent structural models of dynein heavy chain have fostered the hypothesis that the energy derived from hydrolysis at P-loop 1 acts through adjacent P-loop domains to effect changes in the attachment state of the microtubule-binding domain. However, to date, the functional significance of the P-loop domains adjacent to the ATP hydrolytic site has not been demonstrated. Our results provide a mutational analysis of P-loop function within the first and third
AAA
domains of the Drosophila
cytoplasmic dynein heavy chain
. Here we report the first evidence that P-loop-3 function is essential for dynein function. Significantly, our results further show that P-loop-3 function is required for the ATP-induced release of the dynein complex from microtubules. Mutation of P-loop-3 blocks ATP-mediated release of dynein from microtubules, but does not appear to block ATP binding and hydrolysis at P-loop 1. Combined with the recent recognition that dynein belongs to the family of
AAA
ATPases, the observations support current models in which the multiple
AAA
domains of the dynein heavy chain interact to support the translocation of the dynein motor down the microtubule lattice.
...
PMID:The third P-loop domain in cytoplasmic dynein heavy chain is essential for dynein motor function and ATP-sensitive microtubule binding. 1268 93
