Disrupted regulation of serpinB9 in circulating T cells is associated with an increased risk for post-transplant skin cancer.
Fleur S PetersA M A PeetersT P P van den BoschA L MooyaartJ van de WeteringM G H BetjesC C BaanK BoerPublished in: Clinical and experimental immunology (2019)
Cutaneous squamous cell carcinoma (cSCC) is a serious complication after organ transplantation and patients benefit from an early risk assessment. We hypothesized that functional differences in circulating T cells may represent risk factors for post-transplant cSCC development. Here, we analysed genome-wide DNA methylation of circulating T cells of kidney transplant recipients before the clinical onset of cSCC, to identify differences associated with post-transplant cSCC development. This analysis identified higher DNA methylation of SERPINB9, which is an intracellular inhibitor of granzyme B, a protein that induces apoptosis in target cells. High DNA methylation of SERPINB9 in circulating T cells was confirmed in a second patient cohort during recurrent cSCC, indicating that high SERPINB9 methylation represents a persistent risk factor for cSCC development. At the functional level, the inverse correlation between DNA methylation and messenger RNA expression present in non-cSCC patients was absent in the cSCC patients. Also, a significant difference in serpinB9 protein expression between cSCC patients and non-cSCC patients was observed. It was concluded that disturbed regulation of serpinB9 in circulating T cells represents a novel risk factor for post-transplant cSCC in kidney transplant recipients.
Keyphrases
- dna methylation
- end stage renal disease
- genome wide
- squamous cell carcinoma
- ejection fraction
- newly diagnosed
- chronic kidney disease
- risk assessment
- prognostic factors
- stem cells
- oxidative stress
- radiation therapy
- poor prognosis
- climate change
- small molecule
- endoplasmic reticulum stress
- induced apoptosis
- heavy metals
- bone marrow
- pi k akt
- nucleic acid