Tumor-associated high endothelial venules mediate lymphocyte entry into tumors and predict response to PD-1 plus CTLA-4 combination immunotherapy

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不同严重程度鼻炎患者尘螨舌下特异性免疫治疗临床效果观察

目的　评估不同严重程度变应性鼻炎（allergic rhinitis，AR）患儿进行规范化舌下特异性免疫治疗（sublingual immunotherapy， SLIT）的疗效。方法　选取2017年5—12月首都儿科研究所附属儿童医院耳鼻喉科就诊的3～14岁对粉尘螨过敏的AR患儿181例， 按治疗方式不同分为对照组（n＝92， 给予常规药物治疗）和SLIT组（n＝89， 给予尘螨特异性免疫治疗）； 采用AR评分标准， 根据患儿鼻部症状总评分（total nasal symptoms score， TNSS）， 将对照组分为轻度组（n＝35）、中度组（n＝28）和重度组（n＝29）；将SLIT分为轻度组（n＝27）、中度组（n＝33）和重度组（n＝29）。收集第6个月、 1年、 2年的随访数据， 分别对患儿进行TNSS、 鼻炎用药评分（total rhinitis medication scores， TRMS）和视觉模拟量表（visual analogue scale，VAS）评分。结果　（1）治疗2年后， SLIT组与对照组患儿TNSS评分分别为0.61±0.73、 1.61±1.17， TRMS分别为0.21±0.41、 0.59±0.70， VAS分别为0.63±0.70、 1.53±1.24， 两组间差异有统计学意义， Z值分别为6.269、 4.139、5.174， P值均＜0.05； （2）轻度组（n＝62）组内分析： SLIT组（n＝27）与对照组（n＝35）比较， 治疗6个月、 1年， 两组的TNSS、 TRMS、 VAS差异均无统计学意义（Z值分别为-0.108、 0.232、 0.788， 0.774、 0.033、 -0.718； P值均＞0.05）； 治疗2年时两组的TRMS、 VAS差异无统计学意义（Z值分别为0.230、 1.255， P＞0.05）， TNSS在两组间差异有统计学意义（Z值为2.528， P值均＜0.05）； （3）中度组（n＝61）组内分析： 与对照组（n＝28）比较， SLIT组（n＝33）治疗6个月， TRMS、 VAS在两组间差异均无统计学意义（Z值分别为-0.413、 0.412， P值均＞0.05）， 但两组的TNSS差异有统计学意义（Z值为2.397， P＜0.05）； 治疗1年、2年的TNSS、 TRMS、 VAS两组间比较， 差异均有统计学意义（Z值分别为4.952、 2.740、 3.293； 4.743、 2.505、 3.330； P值均＜0.05）； （4）重度组（n＝58）组内分析： 与对照组（n＝29）比较， SLIT组（n＝29）治疗6个月、 1年、 2年的TNSS、 TRMS、 VAS在两组间差异均有统计学意义（Z值分别为2.567、 2.086、 2.781， 4.996、 4.264、 2.756， 4.253、 4.480、 4.515， P值均＜0.05）。结论　采用标准化粉尘螨滴剂舌下治疗尘螨致敏AR患儿， 治疗2年可获得较单纯药物治疗更佳的疗效， 尤其在病情严重患儿，其获益更大。     

Replicative senescence of human dermal fibroblasts affects structural and functional aspects of the Golgi apparatus

It is well recognized that the world population is ageing rapidly. Therefore, it is important to understand ageing processes at the cellular and molecular levels to predict the onset of age‐related diseases and prevent them. Recent research has focused on the identification of ageing biomarkers, including those associated with the properties of the Golgi apparatus. In this context, Golgi‐mediated glycosylation of proteins has been well characterized. Additionally, other studies show that the secretion of many compounds, including pro‐inflammatory cytokines and extracellular matrix–degrading enzymes, is modified during ageing, resulting in physical and functional skin degradation. Since the Golgi apparatus is a central organelle of the secretory pathway, we investigated its structural organization in senescent primary human dermal fibroblasts using confocal and electron microscopy. In addition, we monitored the expression of Golgi‐related genes in the same cells. Our data showed a marked alteration in the Golgi morphology during replicative senescence. In contrast to its small and compact structure in non‐senescent cells, the Golgi apparatus exhibited a large and expanded morphology in senescent fibroblasts. Our data also demonstrated that the expression of many genes related to Golgi structural integrity and function was significantly modified in senescent cells, suggesting a relationship between Golgi apparatus function and ageing.     

Marr and Reductionism

David Marr's three-level method for completely understanding a cognitive system and the importance he attaches to the computational level are so familiar as to scarcely need repeating. Fewer seem to recognize that Marr defends his famous method by criticizing the “reductionistic approach.” This sets up a more interesting relationship between Marr and reductionism than is usually acknowledged. I argue that Marr was correct in his criticism of the reductionists of his time—they were only describing (cellular activity), not explaining (cognitive functions). But a careful metascientific account of reductionistic neuroscience over the past two decades reveals that Marr's criticisms no longer have force. Contemporary neuroscience now explains cognition directly, although in a fashion—causal-mechanistically—quite different than Marr recommended. So while Marr was correct to reject the reductionism of his day and offer an alternative method for genuinely explaining cognition, contemporary cognitive scientists now owe us a new defense of Marr's famous method and the advantages of its explanations over the type now pursued successfully in current reductionist neuroscience. There are familiar reasons for thinking that this debt will not be paid easily.     

Therapeutic strategies for the costimulatory molecule OX40 in T-cell-mediated immunity

The T cell co-stimulatory molecule OX40 and its cognate ligand OX40L have attracted broad research interest as a therapeutic target in T cell-mediated diseases. Accumulating preclinical evidence highlights the therapeutic efficacy of both agonist and blockade of the OX40–OX40L interaction. Despite this progress, many questions about the immuno-modulator roles of OX40 on T cell function remain unanswered. In this review we summarize the impact of the OX40–OX40L interaction on T cell subsets, including Th1, Th2, Th9, Th17, Th22, Treg, Tfh, and CD8⁺ T cells, to gain a comprehensive understanding of anti-OX40 mAb-based therapies. The potential therapeutic application of the OX40–OX40L interaction in autoimmunity diseases and cancer immunotherapy are further discussed; OX40–OX40L blockade may ameliorate autoantigen-specific T cell responses and reduce immune activity in autoimmunity diseases. We also explore the rationale of targeting OX40–OX40L interactions in cancer immunotherapy. Ligation of OX40 with targeted agonist anti-OX40 mAbs conveys activating signals to T cells. When combined with other therapeutic treatments, such as anti-PD-1 or anti-CTLA-4 blockade, cytokines, chemotherapy, or radiotherapy, the anti-tumor activity of agonist anti-OX40 treatment will be further enhanced. These data collectively suggest great potential for OX40-mediated therapies.     

Racial differences in characteristics and prognoses between Asian and white patients with nonsmall cell lung cancer receiving atezolizumab: An ancillary analysis of the POPLAR and OAK studies

This study aimed to compare the differences in characteristics and prognoses between Asian and white patients receiving immunotherapy for nonsmall cell lung cancer (NSCLC). We studied 390 patients who received atezolizumab as part of the POPLAR or OAK trial, and analyzed the differences in baseline characteristics, outcomes and genetic mutations in blood samples between Asian and white patients. Overall survival (OS) was longer in Asian compared to white patients (median OS: 18.7 vs. 11.1 months; p = 0.005). Race was identified as an independent prognostic factor for OS (Asian vs. white: hazard ratio 0.647, 95% confidence interval 0.447–0.936, p = 0.021), together with performance status, histology, baseline sum of the longest tumor diameters (BLSLD) and number of metastatic sites. The two groups also differed in terms of characteristics including smoking history, BLSLD, epidermal growth factor receptor (EGFR) mutation frequency, programmed death-ligand 1 expression and blood-based tumor-mutation burden. Blood mutations of STK11, EGFR, KEAP1, POLE, GRM3, ATM and STAG2 were associated with treatment response, and TP53, KEAP1, APC, RB1, CREBBP, EPHA5 and STAG2 mutations were associated with OS. The blood-based mutation profiles differentiated between Asian and white patients, especially in relation to EGFR (23.8 vs. 8.5%), TP53 (30.2 vs. 46.9%) and STK11 (1.6 vs. 12.3%) mutations (all p < 0.05). The different clinicopathological features and mutation profiles in Asian and white patients may explain the superior outcome following atezolizumab treatment in Asian patients with NSCLC. The results of this study have important implications for further studies on racial disparities in relation to immunotherapy.