不完全弗氏佐剂可减少精氨酸酶,增强疫苗部位微环境中的 Th1 优势、TLR 信号和 CD40 配体表达。
Incomplete Freund's adjuvant reduces arginase and enhances Th1 dominance, TLR signaling and CD40 ligand expression in the vaccine site microenvironment.
机构信息
Surgery, University of Virginia, Charlottesville, Virginia, USA.
Biology, University of Virginia, Charlottesville, Virginia, USA.
出版信息
J Immunother Cancer. 2020 Apr;8(1). doi: 10.1136/jitc-2020-000544.
BACKGROUND
Immunogenicity of cancer vaccines is impacted by adjuvants and schedule, but systematic assessments of their effects have not been performed. Montanide ISA-51, an incomplete Freund's adjuvant (IFA), is used in many vaccine trials, but concerns have been raised about negative effects in murine studies. We found in humans that IFA enhances systemic immune responses and that repeat vaccination at one site (same site vaccination (SSV)) creates tertiary lymphoid structures (TLS) in the vaccine site microenvironment (VSME). We hypothesized that vaccination with peptides+IFA+pICLC or SSV×3 with peptides in IFA would create an immunogenic milieu locally at the VSME, with activated dendritic cells (DC), TLS-associated chemokines and a Th1-dominant VSME.
METHODS
Biopsies of the VSME were obtained from participants on two clinical trials who were immunized with multiple melanoma peptides (MELITAC 12.1) in adjuvants comprising IFA and/or the TLR3-agonist pICLC. Biopsies were obtained either a week after one vaccine or a week after SSV×3. Controls included normal skin and skin injected with IFA without peptides. Gene expression analysis was performed by RNAseq.
RESULTS
VSME samples were evaluated from 27 patients. One vaccine with peptides in pICLC+IFA enhanced expression of CD80, CD83, CD86 (p<0.01), CD40 and CD40L (p<0.0001) over normal skin; these effects were significantly enhanced for SSV with peptides+IFA. Vaccines containing pICLC increased expression of TBX21 (T-bet) but did not decrease GATA3 over normal skin, whereas SSV with peptides in IFA dramatically enhanced TBX21 and decreased GATA3, with high expression of IFNγ and STAT1. SSV with peptides in IFA also reduced arginase-1 (ARG1) expression and enhanced expression of TLR adapter molecules TICAM-1 (TRIF) and MYD88. Furthermore, SSV with IFA and peptides also enhanced expression of chemokines associated with TLS formation.
CONCLUSIONS
These findings suggest that SSV with peptides in IFA enhances CD40L expression by CD4 T cells, supports a Th1 microenvironment, with accumulation of activated and mature DC. Increased expression of TLR adaptor proteins after SSV with peptides in IFA might implicate effects of the skin microbiome. Reduced ARG1 may reflect diminished suppressive myeloid activity in the VSME.
TRIAL REGISTRATION NUMBER
(NCT00705640, NCT01585350).
背景
癌症疫苗的免疫原性受佐剂和方案的影响,但尚未对其影响进行系统评估。Montanide ISA-51 是一种不完全弗氏佐剂(IFA),已在许多疫苗试验中使用,但在小鼠研究中已提出对其产生负面影响的担忧。我们在人类中发现 IFA 增强了全身免疫反应,并且在一个部位(相同部位接种(SSV))重复接种可在疫苗部位微环境(VSME)中形成三级淋巴结构(TLS)。我们假设用肽+IFA+pICLC 或 SSV×3 在 IFA 中接种肽会在 VSME 局部产生免疫环境,具有激活的树突状细胞(DC)、TLS 相关趋化因子和以 Th1 为主的 VSME。
方法
从参加两种临床试验的参与者的 VSME 中获得活检,这些参与者用多种黑色素瘤肽(MELITAC 12.1)在包含 IFA 和/或 TLR3 激动剂 pICLC 的佐剂中进行免疫接种。在一次疫苗接种后一周或 SSV×3 后一周获得活检。对照包括正常皮肤和注射 IFA 而没有肽的皮肤。通过 RNAseq 进行基因表达分析。
结果
从 27 名患者中评估了 VSME 样本。一种含有 pICLC+IFA 的肽疫苗增强了 CD80、CD83、CD86(p<0.01)、CD40 和 CD40L(p<0.0001)的表达,与正常皮肤相比,这些作用明显增强;而 SSV 中含有肽和 IFA 则显著增强了 TBX21(T-bet)的表达,同时降低了 GATA3 的表达,伴有 IFNγ 和 STAT1 的高表达。含有 pICLC 的疫苗增加了 TBX21 的表达,但没有降低正常皮肤中的 GATA3,而 SSV 中含有肽和 IFA 则大大增强了 TBX21 并降低了 GATA3,同时伴有 IFNγ 和 STAT1 的高表达。SSV 中含有肽和 IFA 还降低了精氨酸酶-1(ARG1)的表达,并增强了 TLR 接头分子 TICAM-1(TRIF)和 MYD88 的表达。此外,SSV 中含有 IFA 和肽也增强了与 TLS 形成相关的趋化因子的表达。
结论
这些发现表明,SSV 中含有肽和 IFA 可增强 CD4 T 细胞中 CD40L 的表达,支持 Th1 微环境,并伴有激活和成熟的 DC 积累。SSV 中含有肽和 IFA 后 TLR 接头蛋白表达增加可能暗示了皮肤微生物组的作用。ARG1 的减少可能反映了 VSME 中抑制性髓样活性的降低。
试验注册号
(NCT00705640,NCT01585350)。
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