Abstract

African trypanosomiasis, also known as sleeping sickness, is a vector-borne parasitic disease caused by Trypanosoma brucei. It threatens over 60 million people in 36 countries of sub-Saharan Africa where health systems are least effective, or even non-existent. There are no effective vaccines and satisfactory drugs for the treatment, and the development of new drugs for the disease is urgently needed. Trypanosome infections are now referred as 'most neglected diseases', and need more research efforts. Microtubules are very critical for the parasite cell division as well as flagellar motility. Cellulr division and locomotion are essential for the trypanosome survival. Therefore, tubulin inhibitors are expected to be promising anti-trypanosomiasis agents, since they interfere with microtubule dynamics and suppress both trypanosome cell division and cell movement. Tubulin is a well-recognized molecular target for anti- trypanosome drug development. On the other hand, tubulin is also a mature molecular target for anti- cancer drug development. Many tubulin inhibitors are first chemotherapy for cancer treatment in clinic. However, these tubulin inhibitors show very weak inhibitory activity to the trypanosome cell growth, because there are clear differences between trypanosome and mammalian tubulin. Currently, the task is to develop selective tubulin inhibitors only interfering with trypanosome cells. We identified several lead compounds selectively decreasing trypanosome cell viability from a tubulin inhibitor library initially develoed as anti-cancer agents. A structure-activity relationship (SAR) was summarized based on the anti-trypanosome cell activity of these compounds. The pharmacophore of the tubulin inhibitors enhancing the mammalian cell growth inhibition was different to the pharmacophore promoting the parasite growth inhibition. The results encourage us to expect that more selective and potent tubulin inhibitors against trypanosomiasis could be developed based on the preliminary SAR. To test the hypothesis, we will focus on three research aims listed below: 1) Optimize the lead compounds to generate more selective and potent tubulin inhibitors against trypanosomiasis. We will use medicinal chemistry approaches to design and synthesize new analogs, and test the compounds with trypanosome and human cell growth assays. More potent compounds with lesser toxicity will be identified. 2) Determine the tubulin polymerization inhibitory activity of the selected compounds. We will use tubulin proteins originally isolated fro mammalian and trypanosome cells to test the protein selectivity of the drug candidates. 3) Determine the in vivo anti-trypanosome activity and the bioavailability of the drug candidates. The oral activity and blood brain barrier passing ability of the drug candidates will be determined with animals.

Public Health Relevance

Human African trypanosomiasis, also known as sleeping sickness and a vector-borne parasitic disease caused by Trypanosoma brucei, threatens over 60 million people in 36 countries of sub-Saharan Africa. Currently, there are no effective vaccines and satisfactory drugs for the treatments, and the development of new drugs for the disease is urgently needed. However, research interest of large pharmaceutical companies focusing on the disease is very limited due to the low profit of the agents targeting the disease. Trypanosome infections are now referred as 'most neglected diseases', and need more research. We focus our efforts on developing novel treatments for this orphan disease.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Academic Research Enhancement Awards (AREA) (R15)
Project #
1R15AI103889-01
Application #
8434287
Study Section
Special Emphasis Panel (ZRG1-IDM-C (92))
Program Officer
Rogers, Martin J
Project Start
2013-01-15
Project End
2015-12-31
Budget Start
2013-01-15
Budget End
2015-12-31
Support Year
1
Fiscal Year
2013
Total Cost
$436,500
Indirect Cost
$136,500

  Institution

Name
Cleveland State University
Department
Chemistry
Type
Schools of Arts and Sciences
DUNS #
010841617
City
Cleveland
State
OH
Country
United States
Zip Code
44115

  Publications

Petty, Aaron; Idippily, Nethrie; Bobba, Viharika et al. (2018) Design and synthesis of small molecule agonists of EphA2 receptor. Eur J Med Chem 143:1261-1276
Bobba, Viharika; Nanavaty, Vishal; Idippily, Nethrie D et al. (2017) Synthesis and biological evaluation of selective tubulin inhibitors as anti-trypanosomal agents. Bioorg Med Chem 25:3215-3222
Nanavaty, Vishal; Lama, Rati; Sandhu, Ranjodh et al. (2016) Orally Active and Selective Tubulin Inhibitors as Anti-Trypanosome Agents. PLoS One 11:e0146289
Voggu, Ramakrishna R; Zhou, Xiang; Su, Bin et al. (2015) A Simple and Rapid LC-MS/MS Method for the Determination of BMCL26 a Novel Anti-Parasitic Agent in Rat Plasma. J Anal Bioanal Tech 6:
Zhong, Bo; Lama, Rati; Kulman, Daniel G et al. (2014) Lead optimization of dual tubulin and Hsp27 inhibitors. Eur J Med Chem 80:243-53
Zhong, Bo; Chennamaneni, Snigdha; Lama, Rati et al. (2013) Synthesis and anticancer mechanism investigation of dual Hsp27 and tubulin inhibitors. J Med Chem 56:5306-20