Cecilia Canessa, MD
Professor of Cellular And Molecular PhysiologyCards
Appointments
Contact Info
Cellular & Molecular Physiology
PO Box 208026, 333 Cedar Street
New Haven, CT 06520-8026
United States
About
Titles
Professor of Cellular And Molecular Physiology
Appointments
Cellular & Molecular Physiology
ProfessorPrimary
Other Departments & Organizations
- Cellular & Molecular Physiology
- Graduate Program in Cellular and Molecular Physiology
- Nephrology
- Yale Ventures
Education & Training
- MD
- Cayetano Heredia University Lima (1982)
- Residency
- Henepin County Medical Center, University of Minnesota
- Fellowship
- Univerisity of Alabama
Research
Overview
In
our laboratory we examine the structure, function and regulation of two
types of sodium channels: the Epithelial Na + Channel (ENaC) and Acid
Sensing Ion Channels (ASIC). These proteins are structurally related
but serve very different functions. ENaC is expressed in the apical
side of epithelial cells involved in sodium absorption such as in
kidney, lung and colon. Mutations in the human ENaC genes produce
disorders of whole-body sodium balance and are characterized by
hypertension or sodium wasting. Our current work centers on mechanisms
that regulate activity, expression and traffic of ENaC in epithelial
cells specifically, on the role of a kinase known as serum-and
glucocorticoid-induced kinase or Sgk1.
The
ASICs are expressed in neurons of the central and peripheral nervous
systems. External protons gate ASIC but other stimuli are likely to be
more important physiological agonists. These channels have been
implicated in many functions including nociception, mechanoperception
and modulation of synaptic transmission. Our work centers in the
elucidation of the biophysical properties and gating of ASICs from many
vertebrate species.
We
use a broad range of experimental approaches and techniques that
include electrophysiology (patch-clamp, two-electrode voltage clamp,
short-circuit current), cloning of channels from evolutionary distant
species, modifications of channels and their expression in oocytes,
cell lines and in mice either trangenics or knockins.
Medical Research Interests
Research at a Glance
Yale Co-Authors
Publications Timeline
Research Interests
Biff Forbush, PhD
Tong Wang, MD
Epithelial Sodium Channels
Kidney
Publications
2023
Phosphatases maintain low catalytic activity of SGK1: DNA damage resets the balance in favor of phosphorylation
Gu W, Zheng H, Canessa C. Phosphatases maintain low catalytic activity of SGK1: DNA damage resets the balance in favor of phosphorylation. Journal Of Biological Chemistry 2023, 299: 104941. PMID: 37343701, PMCID: PMC10372406, DOI: 10.1016/j.jbc.2023.104941.Peer-Reviewed Original ResearchCitationsAltmetricMeSH Keywords and ConceptsConceptsDNA-dependent protein kinaseCell survivalHsp90 chaperone complexDNA damage responseGlucocorticoid-induced kinase 1Inhibitor of phosphatasesChaperone complexGenotoxic stressDamage responseCatalytic subunitProtein kinaseNovel cancer therapiesKinase 1Stress conditionsDNA damageMolecular pathwaysSGK1 activityPP2ASGK1Cancer cellsDephosphorylationEndogenous inhibitorKinasePP5Phosphorylation
2019
A Mechanism for Desensitization of all Three Functional Mammalian Acid Sensing Ion Channels
Wu Y, Chen Z, Canessa C. A Mechanism for Desensitization of all Three Functional Mammalian Acid Sensing Ion Channels. Biophysical Journal 2019, 116: 36a. DOI: 10.1016/j.bpj.2018.11.237.Peer-Reviewed Original Research
2013
Heterogeneous nuclear ribonucleoprotein A2/B1 is a novel aldosterone target gene in the rat distal colon epithelium
de la Rosa D, Hernandez‐Diaz I, Morales S, Hernandez G, Salido E, Canessa C, Giraldez T. Heterogeneous nuclear ribonucleoprotein A2/B1 is a novel aldosterone target gene in the rat distal colon epithelium. The FASEB Journal 2013, 27: 1148.8-1148.8. DOI: 10.1096/fasebj.27.1_supplement.1148.8.Peer-Reviewed Original ResearchConceptsHnRNP A2/B1A2/B1Distal colonTarget tissuesAldosterone target tissuesHnRNP A2/B1 expressionRat distal colonRenal distal tubulesAldosterone target geneExtracellular volume homeostasisHeterogeneous nuclear ribonucleoprotein A2/B1Aldosterone levelsAcute increaseDistal colon epitheliumMineralocorticoid receptorDistal tubulesRat distal colon epitheliumHnRNP A2/B1 mRNAEpithelial targetsVolume homeostasisColon epitheliumB1 expressionEpithelial NaProtein expressionCell proliferation
2011
D433 Does Not Determine Ion Selectivity in ASIC1
Li T, Yang Y, Canessa C. D433 Does Not Determine Ion Selectivity in ASIC1. Biophysical Journal 2011, 100: 25a. DOI: 10.1016/j.bpj.2010.12.343.Peer-Reviewed Original Research
2010
The β1-β2 Linker in the Extracellular Domain of ASIC1 Determines Desensitization of ASIC1
Li T, Canessa C. The β1-β2 Linker in the Extracellular Domain of ASIC1 Determines Desensitization of ASIC1. Biophysical Journal 2010, 98: 702a. DOI: 10.1016/j.bpj.2009.12.3854.Peer-Reviewed Original Research
2009
Applications of Tissue Microarrays in Renal Physiology and Pathology
Mobasheri A, Cathro H, German A, Marples D, Martín‐vasallo P, Canessa C. Applications of Tissue Microarrays in Renal Physiology and Pathology. 2009, 97-118. DOI: 10.1002/9783527628612.ch8.Peer-Reviewed Original Research
2008
A proton‐independent function of ASIC in Ciona intestinalis
Coric T, Passamaneck Y, Zhang P, Di Gregorio A, Canessa C. A proton‐independent function of ASIC in Ciona intestinalis. The FASEB Journal 2008, 22: 945.4-945.4. DOI: 10.1096/fasebj.22.1_supplement.945.4.Peer-Reviewed Original ResearchConceptsCiona intestinalisAcid-sensitive ion channelsChordate nervous systemAscidian Ciona intestinalisLarval nervous systemPhysiological genomicsAdult nervous systemSequence similarityHigher vertebratesHeterologous systemsLarval neuronsSpliced formsASIC functionNervous systemLarval swimmingIon channelsASIC genesExtracellular protonsSodium channelsProton sensitivityIntestinalisMost neuronsSynaptic transmissionCionaVertebrates
2007
Multiple translational isoforms give functional specificity to serum‐ and glucocorticoid‐induced kinase 1 (Sgk1)
Arteaga M, Canessa C. Multiple translational isoforms give functional specificity to serum‐ and glucocorticoid‐induced kinase 1 (Sgk1). The FASEB Journal 2007, 21: a547-a548. DOI: 10.1096/fasebj.21.5.a547-d.Peer-Reviewed Original ResearchConceptsN-terminusFunctional specificityEvolutionary distant speciesCore kinase domainFOXO transcriptional factorAlternative translation initiationNumerous cellular processesDifferent cellular compartmentsGlucocorticoid-induced kinase 1Glycogen synthase kinase 3bDiversity of functionsDifferent N-terminiDistant speciesER membraneCellular processesTranslation initiationSingle kinaseCellular compartmentsKinase domainT kinaseTranscriptional factorsDistinct substratesKinase 1ER stressCell survivalMultiple Translational Isoforms Give Functional Specificity to Serum- and Glucocorticoid-induced Kinase 1
Arteaga MF, de la Rosa D, Alvarez JA, Canessa CM. Multiple Translational Isoforms Give Functional Specificity to Serum- and Glucocorticoid-induced Kinase 1. Molecular Biology Of The Cell 2007, 18: 2072-2080. PMID: 17377066, PMCID: PMC1877090, DOI: 10.1091/mbc.e06-10-0968.Peer-Reviewed Original ResearchCitationsAltmetricMeSH Keywords and ConceptsConceptsFunctional specificityKinase 1Core kinase domainGlycogen synthase kinase-3betaAlternative translation initiationDifferent cellular compartmentsSynthase kinase-3betaGlucocorticoid-induced kinase 1Different N-terminiActivation of SGK1ER membraneTranslation initiationCellular compartmentsKinase domainKinase-3betaUbiquitous kinaseTranscriptional factorsN-terminusDiverse processesEpithelial sodium channelLong isoformShort isoformER stressCell survivalTranslational isoforms
2006
An amphipathic helix targets serum and glucocorticoid-induced kinase 1 to the endoplasmic reticulum-associated ubiquitin-conjugation machinery
Arteaga MF, Wang L, Ravid T, Hochstrasser M, Canessa CM. An amphipathic helix targets serum and glucocorticoid-induced kinase 1 to the endoplasmic reticulum-associated ubiquitin-conjugation machinery. Proceedings Of The National Academy Of Sciences Of The United States Of America 2006, 103: 11178-11183. PMID: 16847254, PMCID: PMC1544061, DOI: 10.1073/pnas.0604816103.Peer-Reviewed Original ResearchCitationsAltmetricMeSH Keywords and ConceptsConceptsGlucocorticoid-induced kinase 1Kinase 1Endoplasmic reticulumRapid protein turnoverUbiquitin conjugation machineryHydrophobic motifER localizationMammalian cellsSubcellular localizationCytosolic substratesGene transcriptionProtein turnoverDegradation systemCell survivalStress conditionsReduction of hydrophobicityIon channelsSGK1HRD1Epithelial cellsRapid degradationReticulumMotifPathwayUb
News
News
- January 09, 2020
Cellular and Molecular Physiology Annual Retreat 2019
- December 06, 2018
Cellular and Molecular Physiology Annual Retreat 2018
- October 02, 2017
Cellular and Molecular Physiology Annual Retreat 2017
- October 04, 2016
Cellular and Molecular Physiology Annual Retreat 2016
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Contacts
Cellular & Molecular Physiology
PO Box 208026, 333 Cedar Street
New Haven, CT 06520-8026
United States