Abstract

The overall objective is to better understand the pathophysiology of diarrheal diseases and to discover drugs potentially useful for treating these diseases. This will be approached by understanding regulation of basal intestinal electrolyte absorption and stimulated secretion and using this information to modify active intestinal transport in such a way as to be useful in therapy of diarrheal diseases; that is, stimulating absorption or inhibiting secretion. Emphasis in probing regulation will be on how intracellular calcium affects intestinal Na and C1 absorption and C1 secretion. Studies will be done in rabbit ileum. The bulk of the studies will define the role of second messengers on ileal Na and C1 absorption using brush border membrane vesicles - emphasis will be on the effect of Ca++/calmodulin, protein kinase C, cAMP and cGMP on Na and C1 influx processes. By performing these studies with and without ATP, it will be determined whether Ca++/calmodulin and protein kinase C act by regulating phosphorylation/dephosphorylation in the brush border. We will define the role of protein kinase C in regulation of rabbit ileal transport using intact tissue studies and correlating measurements of protein kinase C activity in ileal absorptive cells with changes in the linked NaC1 absorptive process localized to the same cells. In order to understand the role of calcium in regulation of transport, levels of free calcium in the cytosol of single intestinal epithelial cells will be measured with a fluorescence microscope-digitizing system-computer using the fluorescent dye Fura-2. Methodologies to be used include: radioisotopic flux measurements of Na and C1 using the Ussing chamber-voltage clamp technique to measure active electrolyte transport; Na and C1 influx measurements into purified brush border membrane vesicles over short periods of time to quantify the initial rates of the entry processes; identification of phosphorylated peptides by SDS-PAGE; and measurements of cytosol free Ca++ by fluorescence microscopy-image processing.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Project (R01)
Project #
5R01DK026523-11
Application #
3227942
Study Section
General Medicine A Subcommittee 2 (GMA)
Project Start
1988-06-01
Project End
1992-11-30
Budget Start
1989-12-01
Budget End
1990-11-30
Support Year
11
Fiscal Year
1990
Total Cost
Indirect Cost

  Institution

Name
Johns Hopkins University
Department
Type
Schools of Medicine
DUNS #
045911138
City
Baltimore
State
MD
Country
United States
Zip Code
21218

  Publications

Singh, Varsha; Yang, Jianbo; Yin, Jianyi et al. (2018) Cholera toxin inhibits SNX27-retromer-mediated delivery of cargo proteins to the plasma membrane. J Cell Sci 131:
Yin, Jianyi; Tse, Chung-Ming; Avula, Leela Rani et al. (2018) Molecular Basis and Differentiation-Associated Alterations of Anion Secretion in Human Duodenal Enteroid Monolayers. Cell Mol Gastroenterol Hepatol 5:591-609
Cil, Onur; Phuan, Puay-Wah; Gillespie, Anne Marie et al. (2017) Benzopyrimido-pyrrolo-oxazine-dione CFTR inhibitor (R)-BPO-27 for antisecretory therapy of diarrheas caused by bacterial enterotoxins. FASEB J 31:751-760
Cha, Boyoung; Yang, Jianbo; Singh, Varsha et al. (2017) PDZ domain-dependent regulation of NHE3 protein by both internal Class II and C-terminal Class I PDZ-binding motifs. J Biol Chem 292:8279-8290
Yu, Huimin; Hasan, Nesrin M; In, Julie G et al. (2017) The Contributions of Human Mini-Intestines to the Study of Intestinal Physiology and Pathophysiology. Annu Rev Physiol 79:291-312
Sarker, Rafiquel; Cha, Boyoung; Kovbasnjuk, Olga et al. (2017) Phosphorylation of NHE3-S719 regulates NHE3 activity through the formation of multiple signaling complexes. Mol Biol Cell 28:1754-1767
Qiang, Xiaoling; Liotta, Anthony S; Shiloach, Joseph et al. (2017) New melanocortin-like peptide of E. coli can suppress inflammation via the mammalian melanocortin-1 receptor (MC1R): possible endocrine-like function for microbes of the gut. NPJ Biofilms Microbiomes 3:31
In, Julie G; Foulke-Abel, Jennifer; Estes, Mary K et al. (2016) Human mini-guts: new insights into intestinal physiology and host-pathogen interactions. Nat Rev Gastroenterol Hepatol 13:633-642
Foulke-Abel, Jennifer; In, Julie; Yin, Jianyi et al. (2016) Human Enteroids as a Model of Upper Small Intestinal Ion Transport Physiology and Pathophysiology. Gastroenterology 150:638-649.e8
Saxena, Kapil; Blutt, Sarah E; Ettayebi, Khalil et al. (2016) Human Intestinal Enteroids: a New Model To Study Human Rotavirus Infection, Host Restriction, and Pathophysiology. J Virol 90:43-56

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