Genetic alterations and tumor immune attack in Yo paraneoplastic cerebellar degeneration

被引:0
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作者
Mathilde Small
Isabelle Treilleux
Coline Couillault
Daniel Pissaloux
Géraldine Picard
Sandrine Paindavoine
Valery Attignon
Qing Wang
Véronique Rogemond
Stéphanie Lay
Isabelle Ray-Coquard
Jacobus Pfisterer
Florence Joly
Andreas Du Bois
Dimitri Psimaras
Nathalie Bendriss-Vermare
Christophe Caux
Bertrand Dubois
Jérôme Honnorat
Virginie Desestret
机构
[1] Institut NeuroMyogène,French Reference Center on Paraneoplastic Neurological Syndrome
[2] Equipe Synaptopathies et Autoanticorps (SynatAc),Department of Biopathology
[3] INSERM U1217/UMR CRS 5310,Cancer Genomics Platform, Department of Translational Research
[4] Hospices civils de Lyon,Department of Oncology, Groupe GINECO
[5] University of Lyon,undefined
[6] Université Claude Bernard Lyon 1,undefined
[7] Centre Leon Berard,undefined
[8] INSERM 1052,undefined
[9] CNRS 5286,undefined
[10] Centre Leon Berard,undefined
[11] Centre de Recherche en Cancérologie de Lyon,undefined
[12] Centre Leon Berard,undefined
[13] Centre Leon Berard,undefined
[14] Gynecologic Oncology Center,undefined
[15] Centre Francois Baclesse,undefined
[16] Groupe GINECO,undefined
[17] Kliniken Essen Mitte,undefined
来源
Acta Neuropathologica | 2018年 / 135卷
关键词
Paraneoplastic cerebellar degeneration; Ovarian cancer; Autoantigen-encoding gene mutations; Anti-tumor immunity;
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摘要
Paraneoplastic cerebellar degenerations with anti-Yo antibodies (Yo-PCD) are rare syndromes caused by an auto-immune response against neuronal antigens (Ags) expressed by tumor cells. However, the mechanisms responsible for such immune tolerance breakdown are unknown. We characterized 26 ovarian carcinomas associated with Yo-PCD for their tumor immune contexture and genetic status of the 2 onconeural Yo-Ags, CDR2 and CDR2L. Yo-PCD tumors differed from the 116 control tumors by more abundant T and B cells infiltration occasionally organized in tertiary lymphoid structures harboring CDR2L protein deposits. Immune cells are mainly in the vicinity of apoptotic tumor cells, revealing tumor immune attack. Moreover, contrary to un-selected ovarian carcinomas, 65% of our Yo-PCD tumors presented at least one somatic mutation in Yo-Ags, with a predominance of missense mutations. Recurrent gains of the CDR2L gene with tumor protein overexpression were also present in 59% of Yo-PCD patients. Overall, each Yo-PCD ovarian carcinomas carried at least one genetic alteration of Yo-Ags. These data demonstrate an association between massive infiltration of Yo-PCD tumors by activated immune effector cells and recurrent gains and/or mutations in autoantigen-encoding genes, suggesting that genetic alterations in tumor cells trigger immune tolerance breakdown and initiation of the auto-immune disease.
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页码:569 / 579
页数:10
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