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AuthorDanjuma, Mohammed Ibn Mas’ud
AuthorAbouJabal, Bodoor
AuthorNaseralallah, Lina Mohammad Ahmad
AuthorElzouki, Abdelnaser
Available date2024-02-14T10:48:41Z
Publication Date2021-02-04
Publication NameLiver International
Identifierhttp://dx.doi.org/10.1111/liv.14861
CitationDanjuma, M. I. M. U., AbouJabal, B., Naseralallah, L. M. A., & Elzouki, A. (2021). HCV cirrhotic patients treated with direct‐acting antivirals: Detection of tubular dysfunction and resolution after viral clearance. Liver International, 41(5), 1171-1172.
ISSN1171-1172
URIhttps://www.scopus.com/inward/record.uri?partnerID=HzOxMe3b&scp=85102620791&origin=inward
URIhttp://hdl.handle.net/10576/51842
AbstractBilotti et al's1 recent excellent report on the prevalence of tubular and glomerular dysfunction in patients with HCV infection on direct-acting antiviral (DAA) agents, and their evolution following HCV clearance adds to recent attempts at exploring the subclinical role of KIM-1 (among other markers of tubular dysfunction) as early biomarkers of tubular damage. Her report showed urinary KIM-1 thresholds (4.7 [3.4-11.3] vs 2.1 [1.0-3.4] ng/mg, P < .001) in patients with tubular injury compared to their normal counterparts. The median KIM-1 threshold for tubular dysfunction in healthy volunteers and across various morbidities within the general population ranged between 0.059 and 2.15 ng/L and 3.5 and 7.1 ng/L respectively.2, 3 The comparatively higher levels of urinary KIM-1 (corrected for creatinine excretion) reported by Bilotti et al is probably attributable to a combination of upregulation of KIM-1 excretion by HCV viral infection itself; additional effect of DAA’s (possibly other drugs such as Cisplatin, Carboplatin and Tenofovir2) and, as yet to be determined, factor(s) associated with polymorphisms of the KIM-1 receptor (Figure1).
Languageen
PublisherWiley-Blackwell
Subjecttubular dysfunction
biomarkers
TitleHCV cirrhotic patients treated with direct-acting antivirals: Detection of tubular dysfunction and resolution after viral clearance
TypeArticle
Issue Number5
Volume Number41
dc.accessType Full Text


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