Abstract

Cytoplasmic motility processes that direct the movement of specific molecules, supramolecular structures, and organelles to particular locations in the cell are essential in eukaryotes. Defining the mechanisms behind these processes is important in understanding both how cells function normally, and how they malfunction in medical conditions such as cancer, aneuploidy, infertility, and paralysis. It has become evident that many cellular components move by being pulled along microtubules by forceproducing """"""""motor"""""""" proteins. My research focuses on kinesin, a recently discovered motor protein that is capable of moving plastic beads along microtubules in vitro. My long term goals are 1) to define kinesin's biological functions, and 2) to learn the molecular details of how kinesin accomplishes those functions in the cell. To achieve these goals, we are studying kinesin in Drosophila using genetics, molecular genetics, biochemistry, and cytology. With collaborators, I have characterized Drosophila kinesin, prepared antibodies against the force-producing element, the kinesin heavy chain, and cloned and characterized the Drosophila kinesin heavy chain gene. Recently, I have isolated 13 lethal mutations in the kinesin heavy chain gene (khc). To determine how the heavy chain works in vivo, we will determine what structural features of the heavy chain are required for viability. The genetic lesions in each of the 13 mutations in hand and in another 40 that we propose to isolate will be located by DNA heteroduplex mismatch cleavage, and identified by partial sequence analysis. I expect this work to define the location of important functional sites in the kinesin heavy chain, and to illuminate some of the biochemistry operative at those sites. The information gained in this study will allow development of refined molecular models of kinesin structure/function and subsequent tests of those models by in vitro mutagenesis. We have begun to identify what kinesin's biological functions are by analysis of the effects of loss of kinesin function caused by heavy chain mutations. The data suggest that kinesin function is critical in neuronal tissue, and that its primary role there may be in axonal transport. This hypothesis will be tested by examining the structure and function of neurons in khc mutant and control larvae, using electron microscopy and electrophysiology. The kinesin heavy chain is a maternally loaded protein, so determining what kinesin's functions are in oocytes and embryos will be done by 1) germline clonal analysis of khc null alleles, and 2) studying dominant interactions of khc alleles with other mutations known to cause problems with microtubule-based motility processes. Preliminary results indicate that kinesin participates in meiotic chromosome segregation. I expect further analysis to identify other cellular processes that depend on kinesin function, and to define how kinesin participates in those processes.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
5R01GM046295-02
Application #
3305705
Study Section
Cellular Biology and Physiology Subcommittee 1 (CBY)
Project Start
1991-08-01
Project End
1996-07-31
Budget Start
1992-08-01
Budget End
1993-07-31
Support Year
2
Fiscal Year
1992
Total Cost
Indirect Cost

  Institution

Name
Indiana University Bloomington
Department
Type
Schools of Arts and Sciences
DUNS #
006046700
City
Bloomington
State
IN
Country
United States
Zip Code
47401

  Publications

Lim, Angeline; Rechtsteiner, Andreas; Saxton, William M (2017) Two kinesins drive anterograde neuropeptide transport. Mol Biol Cell 28:3542-3553
Monteith, Corey E; Brunner, Matthew E; Djagaeva, Inna et al. (2016) A Mechanism for Cytoplasmic Streaming: Kinesin-Driven Alignment of Microtubules and Fast Fluid Flows. Biophys J 110:2053-65
Djagaeva, Inna; Rose, Debra J; Lim, Angeline et al. (2012) Three routes to suppression of the neurodegenerative phenotypes caused by kinesin heavy chain mutations. Genetics 192:173-83
Liu, Song; Sawada, Tomoyo; Lee, Seongsoo et al. (2012) Parkinson's disease-associated kinase PINK1 regulates Miro protein level and axonal transport of mitochondria. PLoS Genet 8:e1002537
Macias, Hector; Moran, Angel; Samara, Yazeed et al. (2011) SLIT/ROBO1 signaling suppresses mammary branching morphogenesis by limiting basal cell number. Dev Cell 20:827-40
Moua, Pangkong; Fullerton, Donna; Serbus, Laura R et al. (2011) Kinesin-1 tail autoregulation and microtubule-binding regions function in saltatory transport but not ooplasmic streaming. Development 138:1087-92
Albertson, Roger; Cao, Jian; Hsieh, Tao-shih et al. (2008) Vesicles and actin are targeted to the cleavage furrow via furrow microtubules and the central spindle. J Cell Biol 181:777-90
Barkus, Rosemarie V; Klyachko, Olga; Horiuchi, Dai et al. (2008) Identification of an axonal kinesin-3 motor for fast anterograde vesicle transport that facilitates retrograde transport of neuropeptides. Mol Biol Cell 19:274-83
Saunders, Adam M; Powers, James; Strome, Susan et al. (2007) Kinesin-5 acts as a brake in anaphase spindle elongation. Curr Biol 17:R453-4
Horiuchi, Dai; Collins, Catherine A; Bhat, Pavan et al. (2007) Control of a kinesin-cargo linkage mechanism by JNK pathway kinases. Curr Biol 17:1313-7

Showing the most recent 10 out of 31 publications