OncoImmunology (Jan 2020)

Cancer testis antigens in myelodysplastic syndromes revisited: a targeted RNA-seq approach

  • Ana María Hurtado López,
  • Tzu Hua Chen-Liang,
  • María Zurdo,
  • Salvador Carrillo-Tornel,
  • Joaquín Panadero,
  • Eduardo José Salido,
  • Victor Beltrán,
  • Begoña Muiña,
  • MariLuz Amigo,
  • Noelia Navarro-Villamor,
  • Rosa Cifuentes,
  • Inés Calabria,
  • Ana Isabel Antón,
  • Raúl Teruel,
  • Manuel Muro,
  • Vicente Vicente,
  • Andrés Jerez

DOI
https://doi.org/10.1080/2162402X.2020.1824642
Journal volume & issue
Vol. 9, no. 1

Abstract

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Cancer-Testis antigens (CTA) are named after the tissues where they are mainly expressed: in germinal and in cancer cells, a process that mimics many gametogenesis features. Mapping accurately the CTA gene expression signature in myelodysplastic syndromes (MDS) and chronic myelomonocytic leukemia (CMML) is a prerequisite for downstream immune target-discovery projects. In this study, we take advantage of the use of azacitidine to treat high-risk MDS and CMML to draw the CTAs landscape, before and after treatment, using an ad hoc targeted RNA sequencing (RNA-seq) design for this group of low transcript genes. In 19 patients, 196 CTAs were detected at baseline. Azacitidine did not change the number of CTAs expressed, but it significantly increased or decreased expression in nine and five CTAs, respectively. TFDP3 and DDX53, emerged as the main candidates for immunotherapeutic targeting, as they showed three main features: i) a significant derepression on day +28 of cycle one in those patients who achieved complete remission with hypomethylating treatment (FC = 6, p = .008; FC = 2.1, p = .008, respectively), ii) similar dynamics at the protein level to what was observed at the RNA layer, and iii) to elicit significant specific cytotoxic immune responses detected by TFDP3 and DDX53 HLA-A*0201 tetramers. Our study addresses the unmet landscape of CTAs expression in MDS and CMML and revealed a previously unrecognized TFDP3 and DDX53 reactivation, detectable in plasma and able to elicit a specific immune response after one cycle of azacitidine.

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