Trypanosoma brucei is the unicellular parasitic protozoa, which causes a fatal disease, African sleeping sickness in human beings and a similar disease in domestic animals. The parasite possesses a single mitochondrion with a concatenated network of mitochondrial DNA known as kinetoplast. In spite of this complex structure, mitochondrial DNA in this protozoal parasite encodes only a few proteins. Thus, similar to the biology of other eukaryotes, the majority of the mitochondrial proteins in T. brucei need to be imported to mitochondria after their synthesis on the cytosolic ribosomes. Our long-term goal is to understand the mitochondrial biogenesis, particularly the mechanistic details of mitochondrial protein import in T. brucei. Many nuclear encoded mitochondrial proteins are crucial for the survival of the mammalian bloodstream forms and many more are needed for the insect or the procyclic form of T. brucei. However, mitochondrial protein import mechanisms are least understood in this group of earliest eukaryotes. In spite of the conservation observed in mitochondrial protein translocases (Toms and Tims) from fungi to mammals, most homologs for these proteins have remained undetectable in trypanosomatid genome databases. In our laboratory, we have recently established an in vitro system for protein import into T. brucei mitochondria. We also have identified and characterized an ortholog of Tim17 from T. brucei. We found that T. brucei Tim17 (TbTim17) is critical for the survival of the procyclic form. It is needed for mitochondrial biogenesis, cell cycle progression and also for cellular morphogenesis. ? ? Based on our preliminary results, we hypothesize that TbTim17 plays a central role in mitochondrial biogenesis, which is crucial for many cellular functions in T. brucei.
The specific aims for this project are: (1) to evaluate the role of TbTim17 in the import of key proteins into the mitochondria of the bloodstream and procyclic forms of T. brucei; (2) to identify and characterize mitochondrial proteins associated with TbTim17; and (3) to analyze the structure-function relationship of the TbTim17 for understanding the mechanism of its action. We will use RNAi strategies and our rigorously characterized in vitro protein import system to evaluate the role of TbTim17 in mitochondrial protein import. We will isolate a TbTim17-containing protein complex and identify and characterize trypanosome specific proteins associated with TbTim17. Furthermore, we will perform various mutagenesis analyses to evaluate the structural domains of TbTim17 critical for its function and protein-protein interactions. By accomplishing specific aims 1-3, we will elucidate mitochondrial protein import mechanisms in T. brucei and also identify unique and essential protein importer molecules that could be exploited as the target for rational chemotherapeutic intervention. ? ? ?

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Enhancement Award (SC1)
Project #
5SC1GM081146-02
Application #
7478117
Study Section
Special Emphasis Panel (ZGM1-MBRS-8 (BV))
Program Officer
Shapiro, Bert I
Project Start
2007-08-01
Project End
2011-07-31
Budget Start
2008-08-01
Budget End
2009-07-31
Support Year
2
Fiscal Year
2008
Total Cost
$278,350
Indirect Cost
Name
Meharry Medical College
Department
Microbiology/Immun/Virology
Type
Schools of Medicine
DUNS #
041438185
City
Nashville
State
TN
Country
United States
Zip Code
37208
Smith Jr, Joseph T; Singha, Ujjal K; Misra, Smita et al. (2018) Divergent Small Tim Homologues Are Associated with TbTim17 and Critical for the Biogenesis of TbTim17 Protein Complexes in Trypanosoma brucei. mSphere 3:
Weems, Ebony; Singha, Ujjal K; Smith, Joseph T et al. (2017) The divergent N-terminal domain of Tim17 is critical for its assembly in the TIM complex in Trypanosoma brucei. Mol Biochem Parasitol 218:4-15
Singha, Ujjal K; Hamilton, VaNae; Chaudhuri, Minu (2015) Tim62, a Novel Mitochondrial Protein in Trypanosoma brucei, Is Essential for Assembly and Stability of the TbTim17 Protein Complex. J Biol Chem 290:23226-39
Weems, Ebony; Singha, Ujjal K; Hamilton, VaNae et al. (2015) Functional complementation analyses reveal that the single PRAT family protein of trypanosoma brucei is a divergent homolog of Tim17 in saccharomyces cerevisiae. Eukaryot Cell 14:286-96
Fullerton, Marjorie; Singha, Ujjal K; Duncan, Melanie et al. (2015) Down regulation of Tim50 in Trypanosoma brucei increases tolerance to oxidative stress. Mol Biochem Parasitol 199:9-18
Haubrich, Brad A; Singha, Ujjal K; Miller, Matthew B et al. (2015) Discovery of an ergosterol-signaling factor that regulates Trypanosoma brucei growth. J Lipid Res 56:331-41
Leaver, David J; Patkar, Presheet; Singha, Ujjal K et al. (2015) Fluorinated Sterols Are Suicide Inhibitors of Ergosterol Biosynthesis and Growth in Trypanosoma brucei. Chem Biol 22:1374-83
Hamilton, Vanae; Singha, Ujjal K; Smith, Joseph T et al. (2014) Trypanosome alternative oxidase possesses both an N-terminal and internal mitochondrial targeting signal. Eukaryot Cell 13:539-47
Duncan, Melanie R; Fullerton, Marjorie; Chaudhuri, Minu (2013) Tim50 in Trypanosoma brucei possesses a dual specificity phosphatase activity and is critical for mitochondrial protein import. J Biol Chem 288:3184-97
Nes, Craigen R; Singha, Ujjal K; Liu, Jialin et al. (2012) Novel sterol metabolic network of Trypanosoma brucei procyclic and bloodstream forms. Biochem J 443:267-77

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