Reduced Neoantigen Expression Revealed by Longitudinal Multiomics as a Possible Immune Evasion Mechanism in Glioma

Nejo Takahide; Matsushita Hirokazu; Karasaki Takahiro; Nomura Masashi; Saito Kuniaki; Tanaka Shota; Takayanagi Shunsaku; Hana Taijun; Takahashi Satoshi; Kitagawa Yosuke; Koike Tsukasa; Kobayashi Yukari; Nagae Genta; Yamamoto Shogo; Ueda Hiroki; Tatsuno Kenji; Narita Yoshitaka; Nagane Motoo; Ueki Keisuke; Nishikawa Ryo; Aburatani Hiroyuki; Mukasa Akitake; Saito Nobuhito; Kakimi Kazuhiro

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Reduced Neoantigen Expression Revealed by Longitudinal Multiomics as a Possible Immune Evasion Mechanism in Glioma

机译：减少纵向多组合的新宿生表达，作为胶质瘤可能的免疫逃避机制

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Immune-based therapies have shown limited efficacy in glioma thus far. This might be at least in part due to insufficient numbers of neoantigens, thought to be targets of immune attack. In addition, we hypothesized that dynamic genetic and epigenetic tumor evolution in gliomas might also affect the mutation/neoantigen landscape and contribute to treatment resistance through immune evasion. Here, we investigated changes in the neoantigen landscape and immunologic features during glioma progression using exome and RNA-seq of paired primary and recurrent tumor samples obtained from 25 WHO grade II-IV glioma patients (glioblastoma, IDH-wild-type, n = 8; grade II-III astrocytoma, IDH-mutant, n = 9; and grade II-III oligodendroglioma, IDH-mutant, 1p/19-qcodeleted, n = 8). The number of missense mutations, predicted neoantigens, or expressed neoantigens was not signif-icantly different between primary and recurrent tumors. However, we found that in individual patients the ratio of expressed neoantigens to predicted neoantigens, designated the "neoantigen expression ratio," decreased significantly at recurrence (P = 0.003). This phenomenon was particularly pronounced for "high-affinity," "clonal," and "passenger gene-derived" neoantigens. Gene expression and IHC analyses suggested that the decreased neoantigen expression ratio was associated with intact antigen presentation machinery, increased tumorinfiltrating immune cells, and ongoing immune responses. Our findings imply that decreased expression of highly immunogenic neoantigens, possibly due to persistent immune selection pressure, might be one of the immune evasion mechanisms along with tumor clonal evolution in some gliomas.

机译：迄今为止，免疫基疗法在胶质瘤中显示出有限的疗效。这可能至少部分地是由于Neoantigens数量不足，被认为是免疫发作的目标。此外，我们假设胶质瘤中的动态遗传和表观遗传肿瘤演化也可能影响突变/新洲植物景观，并通过免疫逃避有助于治疗抵抗力。在这里，我们研究了使用Exome和RNA-SEQ的胶质瘤进展期间Neoantigen景观和免疫功能的变化，并使用25级-Chio-IV级胶质瘤患者（胶质母细胞瘤，IDH-野生型，N = 8 ; II-III级星形细胞瘤，IDH-突变体，N = 9;和III级-III oligodendroglioma，IDH-突变体，1p / 19-qcodeleted，n = 8）。畸形突变，预测的新稻垣或表达新南尼斯的数量在原发性和复发性肿瘤之间并不意识到。然而，我们发现，在个体患者中，表达的新抗原与预测新稻草的比例指定了“新洲人表达比”，在复发时显着降低（p = 0.003）。这种现象特别明显为“高亲和力”，“克隆，”和“乘客基因衍生”的新奥地格。基因表达和IHC分析表明，新洲垣珍苯表达比率下降与完整的抗原呈现机械，增加肿瘤除去免疫细胞，以及正在进行的免疫应答。我们的研究结果意味着，可能是由于持续的免疫选择压力，可能是由于持续的免疫选择压力的表达，可能是一些胶质瘤中的肿瘤挤压机制之一。

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《Cancer immunology research.》 |2019年第7期|共14页
作者
Nejo Takahide; Matsushita Hirokazu; Karasaki Takahiro; Nomura Masashi; Saito Kuniaki; Tanaka Shota; Takayanagi Shunsaku; Hana Taijun; Takahashi Satoshi; Kitagawa Yosuke; Koike Tsukasa; Kobayashi Yukari; Nagae Genta; Yamamoto Shogo; Ueda Hiroki; Tatsuno Kenji; Narita Yoshitaka; Nagane Motoo; Ueki Keisuke; Nishikawa Ryo; Aburatani Hiroyuki; Mukasa Akitake; Saito Nobuhito; Kakimi Kazuhiro;
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作者单位

Univ Tokyo Dept Neurosurg Grad Sch Med Tokyo Japan;

Univ Tokyo Hosp Dept Immunotherapeut Tokyo Japan;

Univ Tokyo Hosp Dept Immunotherapeut Tokyo Japan;

Univ Tokyo Dept Neurosurg Grad Sch Med Tokyo Japan;

Kyorin Univ Fac Med Dept Neurosurg Tokyo Japan;

Univ Tokyo Dept Neurosurg Grad Sch Med Tokyo Japan;

Univ Tokyo Dept Neurosurg Grad Sch Med Tokyo Japan;

Univ Tokyo Dept Neurosurg Grad Sch Med Tokyo Japan;

Univ Tokyo Dept Neurosurg Grad Sch Med Tokyo Japan;

Univ Tokyo Dept Neurosurg Grad Sch Med Tokyo Japan;

Univ Tokyo Dept Neurosurg Grad Sch Med Tokyo Japan;

Univ Tokyo Hosp Dept Immunotherapeut Tokyo Japan;

Univ Tokyo Genome Sci Div Res Ctr Adv Sci &

Technol Tokyo Japan;

Univ Tokyo Genome Sci Div Res Ctr Adv Sci &

Technol Tokyo Japan;

Univ Tokyo Genome Sci Div Res Ctr Adv Sci &

Technol Tokyo Japan;

Univ Tokyo Genome Sci Div Res Ctr Adv Sci &

Technol Tokyo Japan;

Natl Canc Ctr Dept Neurosurg &

Neurooncol Tokyo Japan;

Kyorin Univ Fac Med Dept Neurosurg Tokyo Japan;

Dokkyo Med Univ Dept Neurosurg Mibu Tochigi Japan;

Saitama Med Univ Int Med Ctr Dept Neurooncol Neurosurg Saitama Japan;

Univ Tokyo Genome Sci Div Res Ctr Adv Sci &

Technol Tokyo Japan;

Univ Tokyo Dept Neurosurg Grad Sch Med Tokyo Japan;

Univ Tokyo Dept Neurosurg Grad Sch Med Tokyo Japan;

Univ Tokyo Hosp Dept Immunotherapeut Tokyo Japan;

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正文语种 eng
中图分类肿瘤学;
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专利

1. Reduced Neoantigen Expression Revealed by Longitudinal Multiomics as a Possible Immune Evasion Mechanism in Glioma [J] . Nejo Takahide, Matsushita Hirokazu, Karasaki Takahiro, Cancer immunology research. . 2019,第7期

机译：减少纵向多组合的新宿生表达，作为胶质瘤可能的免疫逃避机制
2. Lack of B7 expression, not human leukocyte antigen expression, facilitates immune evasion by human malignant gliomas. [J] . Anderson RC, Anderson DE, Elder JB, Neurosurgery . 2007,第6期

机译：缺乏B7表达而不是人类白细胞抗原表达会促进人类恶性神经胶质瘤的免疫逃避。
3. Integrative genomic analysis reveals mechanisms of immune evasion in P . falciparum malaria [J] . Mame Massar Dieng, A?ssatou Diawara, Vinu Manikandan, Nature Communications . 2020,第1期

机译：综合基因组分析显示了P中免疫逃逸的机制。疟疾疟疾
4. Characterizing Canine Glioma as a Naturally Occurring Model for Immune Evasion in Human Glioma [C] . American College of Veterinary Internal Medicine Forum Conference . 2019

机译：将犬胶质瘤表征为人类胶质瘤免疫逃避天然存在的模型
5. Merkel cell polyomavirus-specific T cell responses, immune evasion mechanisms & immune therapy in Merkel cell carcinoma [D] . Afanasiev, Olga Kochan 2013

机译：默克尔细胞多瘤病毒特异的T细胞反应，免疫逃逸机制和免疫疗法在默克尔细胞癌中的作用
6. P04.14 Multiomics analysis on primary and recurrent paired tumors reveals a possible immune evasion mechanism through reduced neoantigen expression in some glioma [O] . T Nejo, H Matsushita, T Karasaki, 2018

机译：P04.14对原发性和复发性配对肿瘤的多组学分析揭示了某些胶质瘤中新抗原表达减少可能导致的免疫逃逸机制
7. Enriched environment reduces glioma growth through immune and non-immune mechanisms in mice [O] . Garofalo, Stefano, D'Alessandro, Giuseppina, Chece, Giuseppina, 2015

机译：丰富的环境通过小鼠的免疫和非免疫机制减少神经胶质瘤的生长

Reduced Neoantigen Expression Revealed by Longitudinal Multiomics as a Possible Immune Evasion Mechanism in Glioma

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