Abstract

The ultimate aim of this research proposal is to decode the molecular and biochemical definition of the recovery-adaptation process of phototransduction and of a new process probably linked with the synaptic transmission of the retina. The foundation of the project is the cloning the native rod outer segment membrane guanylate cyclase (ROS-GC), the enzyme pivotal to both the transduction processes of vision and also to the retinal neuronal synaptic activity. Recent evidence indicates that the enzyme exhibits these two activities by acting as a double-sensor of Ca/2+. It has two switches. One switch inhabits and the other switch stimulates the enzymes at micromolar concentrations of Ca/2+. The inhibitory switch is linked to phototransduction and the stimulatory switch to retinal synaptic activity. The major objective is to elucidate the most basic molecular mechanisms involved in the inhibitory and stimulatory switching components of ROS-GC. Recent evidences indicates that the intracellular segment of ROS-GC is modular in nature and the modules are specific for diverse Ca/2+ signals linked to the two processes. Signals related to both processes are mediated by the Ca/2+ binding proteins: GCAP1 and GCAP2 in phototransduction and S100beta in synaptic transmission. Domains of three distinct modules of ROS-GC involved in GCAPs and S100beta stimulation of ROS-GC have been localized and termed Ca/2+-regulated modules (CRMs): CRM1 is linked to GCAP1 signaling. CRM2 to S100beta and CRM3 to GCAP2. A second form of ROS-GC, ROS-GC2, has been cloned from the retina, and is also Ca/2+ modulated, suggesting its linkage to phototransduction. Neither its linkage to synaptic transduction nor its modular nature has been established.
Specific Aims (1-5) as stated below are to determine: (1) sequence motifs of CRM1, CRM2 and CRM3 which act as """"""""turn on"""""""" switches for GCAP1, GCAP2 and S100beta; (2) the Ca/2+-induced folding changes in the GCAPs and S100beta sequence motifs critical in ROS-GC; (3) sequence motifs of GCAP1, GCAP2 and S100beta needed to interact with CRM1, CRM2 and CRM3; (4) the mechanisms of ROS-GC2 activation by GCAPs, 1 and 2; and (5) if ROS-GC2 is also modulated by Ca/2+ in a stimulatory fashion. If it is, determine its mechanism of modulation. The combined tools of biochemistry, genetic remodeling, computer simulation-molecular modeling, and immunology will be used to accomplish these most basic goals, which have direct ramifications in understanding the molecular processes related to vision and retinal neurological disorders.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Eye Institute (NEI)
Type
Research Project (R01)
Project #
5R01EY010828-07
Application #
6329545
Study Section
Visual Sciences C Study Section (VISC)
Program Officer
Mariani, Andrew P
Project Start
1994-08-01
Project End
2002-11-30
Budget Start
2000-12-01
Budget End
2001-11-30
Support Year
7
Fiscal Year
2001
Total Cost
$364,795
Indirect Cost

  Institution

Name
University of Medicine & Dentistry of NJ
Department
Anatomy/Cell Biology
Type
Schools of Osteopathy
DUNS #
City
Stratford
State
NJ
Country
United States
Zip Code
08084

  Publications

Duda, Teresa; Venkataraman, Venkateswar; Ravichandran, Sarangan et al. (2005) ATP-regulated module (ARM) of the atrial natriuretic factor receptor guanylate cyclase. Peptides 26:969-84
Krishnan, Anuradha; Venkataraman, Venkateswar; Fik-Rymarkiewicz, Ewa et al. (2004) Structural, biochemical, and functional characterization of the calcium sensor neurocalcin delta in the inner retinal neurons and its linkage with the rod outer segment membrane guanylate cyclase transduction system. Biochemistry 43:2708-23
Duda, Teresa; Fik-Rymarkiewicz, Ewa; Venkataraman, Venkateswar et al. (2004) Calcium-modulated ciliary membrane guanylate cyclase transduction machinery: constitution and operational principles. Mol Cell Biochem 267:107-22
Duda, Teresa; Sharma, Rameshwar K (2004) S100B-modulated Ca2+-dependent ROS-GC1 transduction machinery in the gustatory epithelium: a new mechanism in gustatory transduction. FEBS Lett 577:393-8
Hwang, Ji-Young; Lange, Christian; Helten, Andreas et al. (2003) Regulatory modes of rod outer segment membrane guanylate cyclase differ in catalytic efficiency and Ca(2+)-sensitivity. Eur J Biochem 270:3814-21
Venkataraman, Venkateswar; Duda, Teresa; Vardi, Noga et al. (2003) Calcium-modulated guanylate cyclase transduction machinery in the photoreceptor--bipolar synaptic region. Biochemistry 42:5640-8
Subbaraya, Iswari; Zhao, Chong; Duda, Teresa (2003) Structure and Ca2+ regulation of frog photoreceptor guanylate cyclase, ROS-GC1. Mol Cell Biochem 254:9-19
Duda, Teresa; Koch, Karl-Wilhelm (2002) Calcium-modulated membrane guanylate cyclase in synaptic transmission? Mol Cell Biochem 230:107-16
Duda, Teresa; Koch, Karl-Wilhelm; Venkataraman, Venkateswar et al. (2002) Ca(2+) sensor S100beta-modulated sites of membrane guanylate cyclase in the photoreceptor-bipolar synapse. EMBO J 21:2547-56
Sharma, Rameshwar K (2002) Evolution of the membrane guanylate cyclase transduction system. Mol Cell Biochem 230:3-30

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