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Molecular patterns of isolated tubulitis differ from tubulitis with interstitial inflammation in early indication biopsies of kidney allografts

Publikace na Ústřední knihovna |
2020

Tento text není v aktuálním jazyce dostupný. Zobrazuje se verze "en".Abstrakt

The Banff 2019 kidney allograft pathology update excluded isolated tubulitis without interstitial inflammation (ISO-T) from the category of borderline (suspicious) for acute T cell-mediated rejection due to its proposed benign clinical outcome. In this study, we explored the molecular assessment of ISO-T.

ISO-T or interstitial inflammation with tubulitis (I+T) was diagnosed in indication biopsies within the first 14 postoperative days. The molecular phenotype of ISO-T was compared to I+T either by using RNA sequencing (n=16) or by Molecular Microscope Diagnostic System (MMDx, n=51).

RNA sequencing showed lower expression of genes related to interferon-y (p=1.5 *10(-16)), cytokine signaling (p=2.1 *10(-20)) and inflammatory response (p=1.0*10(-13)) in the ISO-T group than in I+T group. Transcripts with increased expression in the I+T group overlapped significantly with previously described pathogenesis-based transcript sets associated with cytotoxic and effector T cell transcripts, and with T cell-mediated rejection (TCMR).

MMDx classified 25/32 (78%) ISO-T biopsies and 12/19 (63%) I+T biopsies as no-rejection. ISO-T had significantly lower MMDx scores for interstitial inflammation (p=0.014), tubulitis (p=0.035) and TCMR (p=0.016) compared to I+T.

Fewer molecular signals of inflammation in isolated tubulitis suggest that this is also a benign phenotype on a molecular level.