Cells (Nov 2021)

What Do We Have to Know about PD-L1 Expression in Prostate Cancer? A Systematic Literature Review. Part 1: Focus on Immunohistochemical Results with Discussion of Pre-Analytical and Interpretation Variables

  • Andrea Palicelli,
  • Martina Bonacini,
  • Stefania Croci,
  • Cristina Magi-Galluzzi,
  • Sofia Cañete-Portillo,
  • Alcides Chaux,
  • Alessandra Bisagni,
  • Eleonora Zanetti,
  • Dario De Biase,
  • Beatrice Melli,
  • Francesca Sanguedolce,
  • Moira Ragazzi,
  • Maria Paola Bonasoni,
  • Alessandra Soriano,
  • Stefano Ascani,
  • Maurizio Zizzo,
  • Carolina Castro Ruiz,
  • Antonio De Leo,
  • Guido Giordano,
  • Matteo Landriscina,
  • Giuseppe Carrieri,
  • Luigi Cormio,
  • Daniel M. Berney,
  • Daniel Athanazio,
  • Jatin Gandhi,
  • Alberto Cavazza,
  • Giacomo Santandrea,
  • Alessandro Tafuni,
  • Magda Zanelli

DOI
https://doi.org/10.3390/cells10113166
Journal volume & issue
Vol. 10, no. 11
p. 3166

Abstract

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Immunotherapy targeting the PD-1–PD-L1 axis yielded good results in treating different immunologically ‘‘hot’’ tumors. A phase II study revealed good therapeutic activity of pembrolizumab in selected prostatic carcinoma (PC)-patients. We performed a systematic literature review (PRISMA guidelines), which analyzes the immunohistochemical expression of PD-L1 in human PC samples and highlights the pre-analytical and interpretation variables. Interestingly, 29% acinar PCs, 7% ductal PCs, and 46% neuroendocrine carcinomas/tumors were PD-L1+ on immunohistochemistry. Different scoring methods or cut-off criteria were applied on variable specimen-types, evaluating tumors showing different clinic-pathologic features. The positivity rate of different PD-L1 antibody clones in tumor cells ranged from 3% (SP142) to 50% (ABM4E54), excluding the single case tested for RM-320. The most tested clone was E1L3N, followed by 22C3 (most used for pembrolizumab eligibility), SP263, SP142, and 28-8, which gave the positivity rates of 35%, 11–41% (depending on different scoring systems), 6%, 3%, and 15%, respectively. Other clones were tested in <200 cases. The PD-L1 positivity rate was usually higher in tumors than benign tissues. It was higher in non-tissue microarray specimens (41–50% vs. 15%), as PC cells frequently showed heterogenous or focal PD-L1-staining. PD-L1 was expressed by immune or stromal cells in 12% and 69% cases, respectively. Tumor heterogeneity, inter-institutional preanalytics, and inter-observer interpretation variability may account for result biases.

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