Frontiers in Oncology (Jun 2022)

Immune Activation, Exhaustion and Senescence Profiles as Possible Predictors of Cancer in Liver Transplanted Patients

  • Maria Raffaella Petrara,
  • Sarah Shalaby,
  • Elena Ruffoni,
  • Martina Taborelli,
  • Francesco Carmona,
  • Silvia Giunco,
  • Silvia Giunco,
  • Paola Del Bianco,
  • Pierluca Piselli,
  • Diego Serraino,
  • Umberto Cillo,
  • Riccardo Dolcetti,
  • Riccardo Dolcetti,
  • Patrizia Burra,
  • Anita De Rossi,
  • Anita De Rossi

DOI
https://doi.org/10.3389/fonc.2022.899170
Journal volume & issue
Vol. 12

Abstract

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Liver transplanted (LT) patients for hepatocellular carcinoma (LT-HCC) or for other causes (LT-no-HCC) may develop post-transplantation malignancies. Although immune activation and senescence are frequently implicated in cancer development, no data is available on their possible role as biomarkers predictive of tumor onset in this setting. A total of 116 patients were investigated: the 45 LT-HCC patients were older than the 71 LT-non-HCC (p=0.011), but comparable for sex, HCV, HBV infection and immunosuppressive treatment. At baseline, the numbers of activated and senescent-like circulating cells were significantly higher in LT-HCC patients than in LT-no-HCC ones. After a median follow-up of 26.8 months, 6 post-transplant malignancies (PTM) occurred: 4 in LT-HCC (8.9%) and 2 in LT-no-HCC (2.8%) patients. Overall, subjects with high percentages of activated and exhausted T and B cells at baseline were at higher risk of PTM. Notably, within the LT-HCC group, a higher percentage of senescence-like T cells was also associated with cancer development. Moreover, patients with PTM had higher telomere erosion and higher levels of circulating PAMPs (16S rDNA) and DAMPs (mtDNA) when compared with matched patients without PTM. Overall, these findings suggest that immune activation and exhaustion may be useful to predict the risk of PTM occurrence, regardless of the cause of transplantation. In LT-HCC, T-cell senescence represents an additional risk factor for tumor onset.

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