Ben Topham, Millie de Vries, Maria Nonis, Rebecca van Berkel, Juliet M Pullar, Nicholas J Magon, Margreet C M Vissers, Margaret J Currie, Bridget A Robinson, David Gibbs, Abel Ang, Gabi U Dachs
{"title":"接受免疫治疗的患者血液中的维生素 C 水平及其与单核细胞亚型和表观遗传修饰的关系。","authors":"Ben Topham, Millie de Vries, Maria Nonis, Rebecca van Berkel, Juliet M Pullar, Nicholas J Magon, Margreet C M Vissers, Margaret J Currie, Bridget A Robinson, David Gibbs, Abel Ang, Gabi U Dachs","doi":"10.3390/epigenomes8020017","DOIUrl":null,"url":null,"abstract":"<p><p>The treatment of metastatic melanoma has been revolutionised by immunotherapy, yet a significant number of patients do not respond, and many experience autoimmune adverse events. Associations have been reported between patient outcome and monocyte subsets, whereas vitamin C (ascorbate) has been shown to mediate changes in cancer-stimulated monocytes in vitro. We therefore investigated the relationship of ascorbate with monocyte subsets and epigenetic modifications in patients with metastatic melanoma receiving immunotherapy. Patients receiving immunotherapy were compared to other cancer cohorts and age-matched healthy controls. Ascorbate levels in plasma and peripheral blood-derived mononuclear cells (PBMCs), monocyte subtype and epigenetic markers were measured, and adverse events, tumour response and survival were recorded. A quarter of the immunotherapy cohort had hypovitaminosis C, with plasma and PBMC ascorbate levels significantly lower than those from other cancer patients or healthy controls. PBMCs from the immunotherapy cohort contained similar frequencies of non-classical and classical monocytes. DNA methylation markers and intracellular ascorbate concentration were correlated with monocyte subset frequency in healthy controls, but correlation was lost in immunotherapy patients. No associations between ascorbate status and immune-related adverse events or tumour response or overall survival were apparent.</p>","PeriodicalId":55768,"journal":{"name":"Epigenomes","volume":"8 2","pages":""},"PeriodicalIF":2.5000,"publicationDate":"2024-04-30","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"https://www.ncbi.nlm.nih.gov/pmc/articles/PMC11130941/pdf/","citationCount":"0","resultStr":"{\"title\":\"Blood Vitamin C Levels of Patients Receiving Immunotherapy and Relationship to Monocyte Subtype and Epigenetic Modification.\",\"authors\":\"Ben Topham, Millie de Vries, Maria Nonis, Rebecca van Berkel, Juliet M Pullar, Nicholas J Magon, Margreet C M Vissers, Margaret J Currie, Bridget A Robinson, David Gibbs, Abel Ang, Gabi U Dachs\",\"doi\":\"10.3390/epigenomes8020017\",\"DOIUrl\":null,\"url\":null,\"abstract\":\"<p><p>The treatment of metastatic melanoma has been revolutionised by immunotherapy, yet a significant number of patients do not respond, and many experience autoimmune adverse events. Associations have been reported between patient outcome and monocyte subsets, whereas vitamin C (ascorbate) has been shown to mediate changes in cancer-stimulated monocytes in vitro. We therefore investigated the relationship of ascorbate with monocyte subsets and epigenetic modifications in patients with metastatic melanoma receiving immunotherapy. Patients receiving immunotherapy were compared to other cancer cohorts and age-matched healthy controls. Ascorbate levels in plasma and peripheral blood-derived mononuclear cells (PBMCs), monocyte subtype and epigenetic markers were measured, and adverse events, tumour response and survival were recorded. A quarter of the immunotherapy cohort had hypovitaminosis C, with plasma and PBMC ascorbate levels significantly lower than those from other cancer patients or healthy controls. PBMCs from the immunotherapy cohort contained similar frequencies of non-classical and classical monocytes. DNA methylation markers and intracellular ascorbate concentration were correlated with monocyte subset frequency in healthy controls, but correlation was lost in immunotherapy patients. 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引用次数: 0
摘要
免疫疗法给转移性黑色素瘤的治疗带来了革命性的变化,但仍有相当多的患者对这种疗法没有反应,许多患者还出现了自身免疫不良反应。有报道称,患者的预后与单核细胞亚群之间存在关联,而维生素 C(抗坏血酸)已被证明能在体外介导癌症刺激单核细胞的变化。因此,我们研究了抗坏血酸与接受免疫疗法的转移性黑色素瘤患者的单核细胞亚群和表观遗传学改变之间的关系。我们将接受免疫疗法的患者与其他癌症患者和年龄匹配的健康对照组进行了比较。测量了血浆和外周血单核细胞(PBMCs)中的抗坏血酸水平、单核细胞亚型和表观遗传标记物,并记录了不良事件、肿瘤反应和存活率。免疫疗法队列中有四分之一的患者维生素 C 过低,血浆和外周血单核细胞抗坏血酸水平明显低于其他癌症患者或健康对照组。免疫疗法组群的 PBMC 中含有相似频率的非典型和典型单核细胞。在健康对照组中,DNA 甲基化标记物和细胞内抗坏血酸浓度与单核细胞亚群频率相关,但在免疫治疗患者中则失去了相关性。抗坏血酸状态与免疫相关不良事件、肿瘤反应或总生存期之间没有明显的关联。
Blood Vitamin C Levels of Patients Receiving Immunotherapy and Relationship to Monocyte Subtype and Epigenetic Modification.
The treatment of metastatic melanoma has been revolutionised by immunotherapy, yet a significant number of patients do not respond, and many experience autoimmune adverse events. Associations have been reported between patient outcome and monocyte subsets, whereas vitamin C (ascorbate) has been shown to mediate changes in cancer-stimulated monocytes in vitro. We therefore investigated the relationship of ascorbate with monocyte subsets and epigenetic modifications in patients with metastatic melanoma receiving immunotherapy. Patients receiving immunotherapy were compared to other cancer cohorts and age-matched healthy controls. Ascorbate levels in plasma and peripheral blood-derived mononuclear cells (PBMCs), monocyte subtype and epigenetic markers were measured, and adverse events, tumour response and survival were recorded. A quarter of the immunotherapy cohort had hypovitaminosis C, with plasma and PBMC ascorbate levels significantly lower than those from other cancer patients or healthy controls. PBMCs from the immunotherapy cohort contained similar frequencies of non-classical and classical monocytes. DNA methylation markers and intracellular ascorbate concentration were correlated with monocyte subset frequency in healthy controls, but correlation was lost in immunotherapy patients. No associations between ascorbate status and immune-related adverse events or tumour response or overall survival were apparent.