The long term goal of this research project is to achieve quantitative understandings of system-level E. coli chemotaxis behaviors and their underlying molecular level mechanisms. We will develop mathematical models of protein interaction network and its dynamics based on structural and biochemical details of the chemotaxis signaling pathway. These models will be studied by using analytical analysis and numerical simulation methods. The results from these models will be used to explain experimental data and make testable predictions. The iterative comparison between models and experimental data will be used to improve/refine the models. Taken together with quantitative experiments, these predictive models allow us to test different hypotheses in order to understand the underlying molecular mechanisms for emergent biological behaviors. In this proposal, we will focus on studying two essential aspects of the bacterial chemotaxis pathway: 1) The structure-function relationship for the chemoreceptor cluster. The bacterial chemoreceptors form polar clusters with the adaptor protein CheW and the histidine kinase CheA. By using the latest structure information of the chemoreceptor cluster and functional measurements, we will develop a structure-based model to investigate how chemical signal propogates through the heterogeneous protein cluster and how the signal can be amplified by the large extended chemoreceptor array. 2) Signal integration and adaption of the bacterial flagellar motor. The bacterial flaglellar motor is composed of ~20 different types of proteins. It can sense the intracellular chemical signal (CheY-P) and switch its rotational direction (CW and CCW) accordingly. It can also sense the mechanical signal, the load, and generates a corresponding torque to drive the load to rotate at a certain angular speed. We will develop an integrated model to describe both the mechanical motion (rotation) and the switching dynamics of the motor in a thermodynamically consistent framework. We will use this integrated model to investigate how the flagellar motor's switching dynamics can be affected by changes in its mechanical environment (load, torque). We will introduce different feedback interactions in our model to investigate the possible origins of the recently observed motor adaptation to external chemical and mechanical signals. The model predictions will be tested with experimental measurements to determine the molecular mechanism for motor adaptation. In summary, we plan to investigate and understand how different proteins in multi- component protein complexes (such as the chemoreceptor cluster and the flagellar motor) work together to sense, to respond, and to adapt to different (chemical and/or physical) signals.

Public Health Relevance

The concepts and tools developed in the quantitative, system-level modeling of a complete sensory signal transduction pathway and motility will be useful in understanding sensory systems and motility in higher organisms, including human. The molecular level understanding of the bacterial chemotaxis pathway is important to study the role of bacterial pathogens in human health.

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
2R01GM081747-08
Application #
9025262
Study Section
Prokaryotic Cell and Molecular Biology Study Section (PCMB)
Program Officer
Deatherage, James F
Project Start
2007-09-24
Project End
2019-08-31
Budget Start
2015-09-22
Budget End
2016-08-31
Support Year
8
Fiscal Year
2015
Total Cost
$265,240
Indirect Cost
$90,240
Name
Ibm Thomas J. Watson Research Center
Department
Type
DUNS #
084006741
City
Yorktown Heights
State
NY
Country
United States
Zip Code
10598
Tu, Yuhai; Cao, Yuansheng (2018) Design principles and optimal performance for molecular motors under realistic constraints. Phys Rev E 97:022403
Tu, Yuhai; Rappel, Wouter-Jan (2018) Adaptation of Living Systems. Annu Rev Condens Matter Phys 9:183-205
Mello, Bernardo A; Pan, Wenlin; Hazelbauer, Gerald L et al. (2018) A dual regulation mechanism of histidine kinase CheA identified by combining network-dynamics modeling and system-level input-output data. PLoS Comput Biol 14:e1006305
Fei, Chenyi; Cao, Yuansheng; Ouyang, Qi et al. (2018) Design principles for enhancing phase sensitivity and suppressing phase fluctuations simultaneously in biochemical oscillatory systems. Nat Commun 9:1434
Renault, Thibaud T; Abraham, Anthony O; Bergmiller, Tobias et al. (2017) Bacterial flagella grow through an injection-diffusion mechanism. Elife 6:
Cao, Li-Hui; Yang, Dong; Wu, Wei et al. (2017) Odor-evoked inhibition of olfactory sensory neurons drives olfactory perception in Drosophila. Nat Commun 8:1357
Li, Zhaojun; Cai, Qiuxian; Zhang, Xuanqi et al. (2017) Barrier Crossing in Escherichia coli Chemotaxis. Phys Rev Lett 118:098101
Cao, Li-Hui; Jing, Bi-Yang; Yang, Dong et al. (2016) Distinct signaling of Drosophila chemoreceptors in olfactory sensory neurons. Proc Natl Acad Sci U S A 113:E902-11
Lan, Ganhui; Tu, Yuhai (2016) Information processing in bacteria: memory, computation, and statistical physics: a key issues review. Rep Prog Phys 79:052601
Sartori, Pablo; Tu, Yuhai (2015) Free energy cost of reducing noise while maintaining a high sensitivity. Phys Rev Lett 115:118102

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