Transepithelial potential difference#TEPD in the kidney

The diagnosis of cystic fibrosis (CF) is usually based on high chloride concentrations in sweat, characteristic clinical findings (including sinopulmonary infections), and/or family history. However, a small portion of patients with cystic fibrosis, especially those with "mild" mutations of the cystic fibrosis transmembrane regulator (CFTR) ion channel, have near-normal sweat tests.{{cn|date=April 2025}}

In these cases, a useful diagnostic adjunct involves measuring the nasal transepithelial potential difference (i.e. the charge on the respiratory epithelial surface as compared to interstitial fluid). Individuals with cystic fibrosis have a significantly more negative nasoepithelial surface than normal, due to increased luminal sodium absorption.{{cn|date=April 2025}}

In most exocrine glands, the CFTR protein normally secretes chloride ions into the lumen, and also has a tonic inhibitory effect on the opening of the apical sodium channel (which absorbs sodium into the cell). Impaired CFTR functioning directly reduces ductal epithelial chloride secretion and indirectly increases sodium absorption through lack of CFTR's inhibitory effect on the apical sodium channel. The result is dehydrated mucus and a widened, negative transepithelial potential difference.{{citation needed|date=August 2017}}

The nasal TEPD is increased in cystic fibrosis, making it a potential diagnostic tool for this disorder.{{cite journal | vauthors = Hay JG, Geddes DM | title = Transepithelial potential difference in cystic fibrosis | journal = Thorax | volume = 40 | issue = 7 | pages = 493–6 | date = July 1985 | pmid = 4035615 | pmc = 460118 | doi = 10.1136/thx.40.7.493 }}

In the kidney, TEPD contributes to tubular reabsorption.{{citation needed|date=August 2017}}

Transepithelial / transendothelial electrical resistance (TEER) is an electrophysiological technique widely adopted for use in organ-on-a-chip systems. It uses ohmic contact resistance to serve as a proxy for the permeability of a cellular monolayer. TEER therefore enables researchers to miniaturize assays such as Caco-2 permeability, Blood–brain barrier transfer, or membrane integrity assays in microfluidic systems.{{cite journal | vauthors = Srinivasan B, Kolli AR, Esch MB, Abaci HE, Shuler ML, Hickman JJ | title = TEER measurement techniques for in vitro barrier model systems | language = en-US | journal = Journal of Laboratory Automation | volume = 20 | issue = 2 | pages = 107–26 | date = April 2015 | pmid = 25586998 | pmc = 4652793 | doi = 10.1177/2211068214561025 }} TEER has proven to be a highly sensitive and reliable method to confirm the integrity and permeability of in vitro barrier models. Because it is non-invasive and offers the advantage of continuously monitoring living cells throughout their various stages of growth and differentiation, it is widely accepted as a standard validation tool.{{Cite journal |last1=Zidarič |first1=Tanja |last2=Gradišnik |first2=Lidija |last3=Velnar |first3=Tomaž |date=2022-04-01 |title=Astrocytes and human artificial blood-brain barrier models |journal=Bosnian Journal of Basic Medical Sciences |volume=22 |issue=5 |pages=651–672 |language=en |doi=10.17305/bjbms.2021.6943 |pmid=35366791 |pmc=9519155 |issn=1840-4812|doi-access=free }}

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Category:Membrane biology

Category:Cystic fibrosis