Lung microbiome is defined as the specific microbiota of lung. Lung microbiome can make the lung in a state of chronic inflammation through direct destruction, activation of inflammatory cells and release of inflammatory factors, and then progress to lung cancer. There are significant differences in lung microbiome between lung cancer patients and healthy people. Some specific microbial flora can be used as a diagnostic marker of lung cancer. Specific microbial communities are related to the efficacy of immunotherapy, and microbial composition may be used as a marker of immune-related adverse events. There are both challenges and opportunities for research on the relationship between lung microbiome and lung cancer. This review will focus on the significance and value of lung microbiome in the occurrence, diagnosis and immunotherapy of lung cancer, in order to provide a reference for basic and clinical researchers in related fields.
Objective To summarize the research status and prospect of immunotherapy for biliary tract cancer (BTC). Method The literatures about immunotherapy of BTC at home and abroad in recent years were reviewed. Results Surgical resection was still the first choice and only radical treatment for BTC. However, the recurrence rate of BTC was high, and most of the patients were in the middle and late stage with metastasis and lose the opportunity of operation. Patients with local progression, metastasis or recurrence could only receive chemotherapy and other comprehensive treatment, but they could not get satisfactory results. The continuous update of targeted drugs brings new hope for drug therapy of BTC, and immunotherapy had become a new treatment of tumor targeted therapy following radiotherapy and chemotherapy. ConclusionImmunotherapy can be used as an option for the treatment of advanced BTC and its postoperative recurrence and metastasis, and has attracted more and more attention.
Objective To understand the latest research progress of chemotherapy, targeted therapy and immunotherapy drugs in the treatment of metastatic colorectal cancer. Method The literature on the efficacy of different treatment drugs for metastatic colorectal cancer in recent years both domestically and internationally was retrieved and reviewed. Results There had been many clinical research progress in the treatment of metastatic colorectal cancer, new drugs had emerged, targeted drugs were particularly prominent, and more trials of therapeutic drugs and drug combination treatment regimens were also being carried out. Different treatment methods were applied to patients according to the mutation status of RAS/RAF and the expression of mismatch repair protein, the survival benefit varied greatly. Conclusion Precision medicine is becoming increasingly important, screening patients to choose appropriate treatment modality can further improve survival benefit.
ObjectiveTo construct a prognostic prediction model for hepatocellular carcinoma (HCC) based on disulfidptosis-associated genes (DAGs) and ferroptosis-associated genes (FAGs) using data from The Cancer Genome Atlas (TCGA) and International Cancer Genome Consortium (ICGC) databases and explore the immune characteristics and antitumor drug sensitivity of HCC patients with high- and low-risk score. MethodsThe transcriptomic and clinical data of HCC were downloaded from the TCGA and ICGC databases. The expression levels of DAGs and FAGs were extracted. Subsequently, the differentially expressed and prognostically relevant DAGs and FAGs (DFAGs) were screened through differential expression and prognostic analysis. A prognostic prediction model for HCC was constructed by LASSO regression analysis. The prognostic value of risk factors was evaluated using univariate and multivariate Cox regression analyses, Kaplan-Meier survival analysis, receiver operating characteristic curves, principal component analysis, and t-distributed stochastic neighbor embedding. Gene Ontology (GO) and Kyoto Encyclopedia of Genes and Genomes (KEGG) enrichment analyses were performed to further elucidate the mechanisms of genes associated with HCC prognosis. The impact of risk factors on immune cells and immune cells functions was analyzed using single-sample gene set enrichment analysis. Based on the Genomics of Drug Sensitivity in Cancer database, the oncoPredict package was used to predict responses to antitumor drugs in for different risk groups. ResultsFour DFAGs (SLC7A11, SLC1A5, G6PD, and LRPPRC) with respective risk coefficients of 0.0350, 0.0442, 0.1597, and 0.0132 were selected to construct the prognostic prediction model. The risk score of prognostic prediction model was calculated as: Risk score =(0.0350×SLC7A11 expression level) + (0.0442×SLC1A5 expression level) + (0.159 7×G6PD expression level) + (0.013 2×LRPPRC expression level). The multivariate Cox regression analysis indicated that a high-risk score was an independent risk factor for HCC patient survival [HR (95%CI) = 5.414 (1.918, 15.279), P<0.001]. Both TCGA and ICGC datasets demonstrated that the high-risk patients had significantly worse survival than low-risk patients (P<0.001 and P=0.003, respectively). Enrichment analysis revealed that the risk-associated genes influenced HCC progression through multiple pathways, such as immune response, cell cycle, glycolysis, gluconeogenesis. Immune analysis showed that the high-risk patients exhibited increased infiltration of immunosuppressive cells, such as activated dendritic cells, macrophages, and regulatory T cells, while natural killer cell infiltration was significantly reduced. The drug sensitivity analysis suggested that the high-risk HCC patients might respond better to 5-fluorouracil, afatinib, cyclophosphamide, and lapatinib, whereas the low-risk patients might benefit more from oxaliplatin and sorafenib. ConclusionsHCC prognosis prediction model based on DFAGs in this study suggests a certain predictive value for the survival of HCC patients in the data from both TCGA and ICGC datasets. There are significant differences in pionts of immune cells infiltration and immune cells functions between high-risk and low-risk HCC patients. Additionally, significant differences exist in sensitivity to targeted drugs and chemotherapeutic drugs. This model can provide some references for immunotherapy, personalized treatment, and prognosis evaluation of HCC patients.
Objective To summarize current research status of sperm protein 17 (SP17) in breast cancer. Method Bysearching PubMed, Web of Science, CNKI, and Wanfang databases, the studies about expression and function of SP17 in the breast cancer were summarized. Results SP17 only expressed in the breast cancer tissue but not in the normal breast tissue. The result of the study showed that SP17 was only detected in the metastatic stage of tumor cells. The preclinical trails found that the breast cancer cells with SP17 positive expression could be killed by the specific T lymphocyte. Conclusions SP17 might be a potential target of immunotherapy of breast cancer, it might promote metastasis of cancer. More studies are needed to further explore its function in tumor development, thus accelerate its application in clinical practice.
It is very limited that the benefit of perioperative chemotherapy in early non-small cell lung cancer (NSCLC), and the 5-year survival rate is only 5% higher than surgery. Antibodies that block programmed cell death protein 1/programmed death receptor-ligand 1 significantly improve the survival of advanced NSCLC. The value of immunotherapy in early NSCLC is also being explored. This paper firstly summarized and analyzed the progress of immunotherapy in the perioperative period of NSCLC. Secondly, the safety and feasibility of surgical resection after neoadjuvant immunotherapy were discussed. Finally, the clinical value of different therapeutic efficacy prediction indicators was summarized, in order to clarify the current status of immunotherapy in the perioperative period, so as to improve the clinical benefits of early NSCLC patients.
Objective To detect the anti-colon cancer ability of whole cell lysates pulsed dendritic cell (DC) which acts as an adjuvant. Methods Whole cell lysates of LoVo cells were extracted with freeze thawing method, then the monocyte-derived DC were pulsed with this cellular antigen. Subsequently, the capability of antigen pulsed DC to promote T lymphocytes proliferation and the ability of T lymphocytes to kill LoVo cells were detected by 3H-TdR incorporation and lactate dehydrogenase release methods, respectively. Results The whole cell lysates of LoVo cells pulsed DC significantly stimulated T cells proliferation, and the cytotoxicity abilities of primed T cells to kill LoVo cells were also enhanced. Conclusion Tumor cell lysates which act as the cellular antigen to pulse DC can improve the efficacy of anti-cancer immune response, which provides us an experimental evidence for cancer immunotherapy.
ObjectiveTo analyze the efficacy and safety of immunotherapy and bevacizumab combined with chemotherapy (BIC), bevacizumab combined with chemotherapy (BC), chemotherapy (CT), immunotherapy combined with chemotherapy (IC), bevacizumab combined with immunotherapy (BI), bevacizumab (B) in the first-line treatment of advanced wild-type non-squamous non-small cell lung cancer. MethodsThe PubMed, Embase, Cochrane Library and Web of Science databases were searched to collect phase Ⅱ/Ⅲ randomized controlled trials (RCTs) related to the objectives of the study from January 2010 to December 1, 2022. After two investigators independently screened the literatures, extracted the data and evaluated the risk of bias of the included studies, a reticular meta-analysis was performed using R 3.6.1 software. ResultsA total of 11 RCTs were finally included, including 5 329 patients and six treatment combinations. Meta-analysis results showed that BIC was superior to CT for progression-free survival (PFS) (HR=0.34, 95% CI 0.18 to 0.69), but BIC did not show a significant advantage over the other groups for overall survival (OS). Bayesian ranking results showed that the BIC group had the greatest probability in terms of OS, PFS, and ORR. Among all programmed death ligand 1 (PD-L1) expressing subgroups, there was no significant difference in OS between BIC, BC, IC, CT, BI, and B. Compared with CT, IC was significantly improved in OS (HR=0.68, 95%CI 0.52 to 0.92), PFS (HR=0.58, 95%CI 0.45 to 0.75), and ORR (HR=0.47, 95%CI 0.33 to 0.66). ConclusionIn the first-line treatment of wild-type advanced non-squamous NSCLC, immunotherapy and bevacizumab combined with chemotherapy may improve the efficacy in the short term, but do not change the long-term survival time. Immunotherapy combined with chemotherapy can significantly improve the survival time and prognosis of patients compared with chemotherapy alone. Due to the limited quantity and quality of the included studies, more high-quality studies are needed to verify the above conclusion.