Drosophila lacking dfmr1 activity show defects in circadian output and fail to maintain courtship interest.

Authors

Thomas C Dockendorff
Henry S Su
Sean M J McBride
Zhaohai Yang
Catherine H Choi
Kathleen K Siwicki
Amita Sehgal
Thomas A Jongens

Publication/Presentation Date

6-13-2002

Abstract

Fragile X mental retardation is a prominent genetic disorder caused by the lack of the FMR1 gene product, a known RNA binding protein. Specific physiologic pathways regulated by FMR1 function have yet to be identified. Adult dfmr1 (also called dfxr) mutant flies display arrhythmic circadian activity and have erratic patterns of locomotor activity, whereas overexpression of dFMR1 leads to a lengthened period. dfmr1 mutant males also display reduced courtship activity which appears to result from their inability to maintain courtship interest. Molecular analysis fails to reveal any defects in the expression of clock components; however, the CREB output is affected. Morphological analysis of neurons required for normal circadian behavior reveals subtle abnormalities, suggesting that defects in axonal pathfinding or synapse formation may cause the observed behavioral defects.

Volume

34

Issue

6

First Page

973

Last Page

984

ISSN

0896-6273

Published In/Presented At

Dockendorff, T. C., Su, H. S., McBride, S. M., Yang, Z., Choi, C. H., Siwicki, K. K., Sehgal, A., & Jongens, T. A. (2002). Drosophila lacking dfmr1 activity show defects in circadian output and fail to maintain courtship interest. Neuron, 34(6), 973–984. https://doi.org/10.1016/s0896-6273(02)00724-9

Disciplines

Medicine and Health Sciences

PubMedID

12086644

Department(s)

Fellows and Residents

Document Type

Article