Your search keyword '"Qianghu Wang"' showing total 5 results

1. Sex-based clinical and immunological differences in COVID-19

Author

Yun Cai, Wei Wu, Xinyi Xia, Shukui Wang, Mengyan Zhu, Ning Li, Hongshan Chen, Lu Li, Lingxiang Wu, Bin Huang, Zhihua Wang, Wanlin Li, Kening Li, Min Wu, Ziyu Wang, Qianghu Wang, Lishen Zhang, and Jie Li

Subjects

0301 basic medicine, Adult, Male, medicine.medical_specialty, Lymphocyte, Immunology, Infectious and parasitic diseases, RC109-216, Antibodies, Viral, Gastroenterology, Immunoglobulin G, 03 medical and health sciences, 0302 clinical medicine, Immune system, Internal medicine, medicine, Humans, 030212 general & internal medicine, Risk factor, Survival analysis, Aged, Sex Characteristics, biology, business.industry, SARS-CoV-2, Hazard ratio, COVID-19, Middle Aged, Prognosis, Lymphocyte Subsets, 030104 developmental biology, Infectious Diseases, medicine.anatomical_structure, Antibody Formation, biology.protein, Sex, Female, Antibody, business, Sex characteristics, Research Article

Abstract

BackgroundMales and females differ in their immunological responses to foreign pathogens. However, most of the current COVID-19 clinical practices and trials do not take the sex factor into consideration.MethodsWe performed a sex-based comparative analysis for the clinical outcomes, peripheral immune cells, and severe acute respiratory syndrome coronavirus (SARS-CoV-2) specific antibody levels of 1558 males and 1499 females COVID-19 patients from a single center. The lymphocyte subgroups were measured by Flow cytometry. The total antibody, Spike protein (S)-, receptor binding domain (RBD)-, and nucleoprotein (N)- specific IgM and IgG levels were measured by chemiluminescence.ResultsWe found that male patients had approximately two-fold rates of ICU admission (4.7% vs. 2.7% in males and females, respectively,P = 0.005) and mortality (3% vs. 1.4%, in males and females, respectively,P = 0.004) than female patients. Survival analysis revealed that the male sex is an independent risk factor for death from COVID-19 (adjusted hazard ratio [HR] = 2.22, 95% confidence interval [CI]: 1.3–3.6,P = 0.003). The level of inflammatory cytokines in peripheral blood was higher in males during hospitalization. The renal (102/1588 [6.5%] vs. 63/1499 [4.2%], in males and females, respectively,P = 0.002) and hepatic abnormality (650/1588 [40.9%] vs. 475/1499 [31.7%],P = 0.003) were more common in male patients than in female patients. By analyzing dynamic changes of lymphocyte subsets after symptom onset, we found that the percentage of CD19+ B cells and CD4+ T cells was generally higher in female patients during the disease course of COVID-19. Notably, the protective RBD-specific IgG against SARS-CoV-2 sharply increased and reached a peak in the fourth week after symptom onset in female patients, while gradually increased and reached a peak in the seventh week after symptom onset in male patients.ConclusionsMales had an unfavorable prognosis, higher inflammation, a lower percentage of lymphocytes, and indolent antibody responses during SARS-CoV-2 infection and recovery. Early medical intervention and close monitoring are important, especially for male COVID-19 patients.

Published

2021

2. Implications of cardiac markers in risk-stratification and management for COVID-19 patients

Author

Wei Wu, Tingting Zhang, Xinyi Xia, Weiwei Duan, Yan Hong, Rong Ding, Pengping Li, Yuan Liang, Lingxiang Wu, Han Shen, Xuesong Li, Wenhua You, Yi Han, Yong Ji, Mengyan Zhu, Hongshan Chen, Kening Li, Xin Wang, Xin Tang, Jie Li, Ziyu Wang, Qianghu Wang, and Bin Huang

Subjects

Male, medicine.medical_specialty, China, Coronavirus disease 2019 (COVID-19), Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), Receptor expression, Coronary Artery Disease, 030204 cardiovascular system & hematology, Critical Care and Intensive Care Medicine, Risk Assessment, Coronary artery disease, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, medicine, Humans, 030304 developmental biology, Aged, Retrospective Studies, 0303 health sciences, RC86-88.9, business.industry, Mortality rate, Research, Hazard ratio, COVID-19, Medical emergencies. Critical care. Intensive care. First aid, Retrospective cohort study, Middle Aged, medicine.disease, Cardiac markers, Prognosis, Hospitalization, Risk stratification, Cardiology, Female, business, SARS-CoV-2 receptor, Biomarkers

Abstract

Background COVID-19 has resulted in high mortality worldwide. Information regarding cardiac markers for precise risk-stratification is limited. We aim to discover sensitive and reliable early-warning biomarkers for optimizing management and improving the prognosis of COVID-19 patients. Methods A total of 2954 consecutive COVID-19 patients who were receiving treatment from the Wuhan Huoshenshan Hospital in China from February 4 to April 10 were included in this retrospective cohort. Serum levels of cardiac markers were collected after admission. Coronary artery disease diagnosis and survival status were recorded. Single-cell RNA-sequencing and bulk RNA-sequencing from different cohorts of non-COVID-19 were performed to analyze SARS-CoV-2 receptor expression. Results Among 2954 COVID-19 patients in the analysis, the median age was 60 years (50–68 years), 1461 (49.5%) were female, and 1515 (51.3%) were severe/critical. Compared to mild/moderate (1439, 48.7%) patients, severe/critical patients showed significantly higher levels of cardiac markers within the first week after admission. In severe/critical COVID-19 patients, those with abnormal serum levels of BNP (42 [24.6%] vs 7 [1.1%]), hs-TNI (38 [48.1%] vs 6 [1.0%]), α- HBDH (55 [10.4%] vs 2 [0.2%]), CK-MB (45 [36.3%] vs 12 [0.9%]), and LDH (56 [12.5%] vs 1 [0.1%]) had a significantly higher mortality rate compared to patients with normal levels. The same trend was observed in the ICU admission rate. Severe/critical COVID-19 patients with pre-existing coronary artery disease (165/1,155 [10.9%]) had more cases of BNP (52 [46.5%] vs 119 [16.5%]), hs-TNI (24 [26.7%] vs 9.6 [%], α- HBDH (86 [55.5%] vs 443 [34.4%]), CK-MB (27 [17.4%] vs 97 [7.5%]), and LDH (65 [41.9%] vs 382 [29.7%]), when compared with those without coronary artery disease. There was enhanced SARS-CoV-2 receptor expression in coronary artery disease compared with healthy controls. From regression analysis, patients with five elevated cardiac markers were at a higher risk of death (hazards ratio 3.4 [95% CI 2.4–4.8]). Conclusions COVID-19 patients with pre-existing coronary artery disease represented a higher abnormal percentage of cardiac markers, accompanied by high mortality and ICU admission rate. BNP together with hs-TNI, α- HBDH, CK-MB and LDH act as a prognostic biomarker in COVID-19 patients with or without pre-existing coronary artery disease.

Published

2021

3. Suppression of RAF/MEK or PI3K synergizes cytotoxicity of receptor tyrosine kinase inhibitors in glioma tumor-initiating cells.

Author

Takashi Shingu, Holmes, Lindsay, Henry, Verlene, Qianghu Wang, Latha, Khatri, Gururaj, Anupama E., Gibson, Laura A., Doucette, Tiffany, Lang, Frederick F., Ganesh Rao, Liang Yuan, Sulman, Erik P., Farrell, Nicholas P., Priebe, Waldemar, Hess, Kenneth R., Wang, Yaoqi A., Jian Hu, Bögler, Oliver, Shingu, Takashi, and Wang, Qianghu

Subjects

GLIOMAS, CANCER cell culture, TARGETED drug delivery, PROTEIN-tyrosine kinase inhibitors, AUTOPHAGY, APOPTOSIS, PHOSPHORYLATION, CELLULAR signal transduction, ANIMAL experimentation, ANTINEOPLASTIC agents, CELL lines, CELL physiology, DRUG synergism, MICE, PHOSPHOTRANSFERASES, RESEARCH funding, STEM cells, TRANSFERASES, CHEMICAL inhibitors, PROTEIN kinase inhibitors, PHARMACODYNAMICS, THERAPEUTICS

Abstract

Background: The majority of glioblastomas have aberrant receptor tyrosine kinase (RTK)/RAS/phosphoinositide 3 kinase (PI3K) signaling pathways and malignant glioma cells are thought to be addicted to these signaling pathways for their survival and proliferation. However, recent studies suggest that monotherapies or inappropriate combination therapies using the molecular targeted drugs have limited efficacy possibly because of tumor heterogeneities, signaling redundancy and crosstalk in intracellular signaling network, indicating necessity of rationale and methods for efficient personalized combination treatments. Here, we evaluated the growth of colonies obtained from glioma tumor-initiating cells (GICs) derived from glioma sphere culture (GSC) in agarose and examined the effects of combination treatments on GICs using targeted drugs that affect the signaling pathways to which most glioma cells are addicted.Methods: Human GICs were cultured in agarose and treated with inhibitors of RTKs, non-receptor kinases or transcription factors. The colony number and volume were analyzed using a colony counter, and Chou-Talalay combination indices were evaluated. Autophagy and apoptosis were also analyzed. Phosphorylation of proteins was evaluated by reverse phase protein array and immunoblotting.Results: Increases of colony number and volume in agarose correlated with the Gompertz function. GICs showed diverse drug sensitivity, but inhibitions of RTK and RAF/MEK or PI3K by combinations such as EGFR inhibitor and MEK inhibitor, sorafenib and U0126, erlotinib and BKM120, and EGFR inhibitor and sorafenib showed synergy in different subtypes of GICs. Combination of erlotinib and sorafenib, synergistic in GSC11, induced apoptosis and autophagic cell death associated with suppressed Akt and ERK signaling pathways and decreased nuclear PKM2 and β-catenin in vitro, and tended to improve survival of nude mice bearing GSC11 brain tumor. Reverse phase protein array analysis of the synergistic treatment indicated involvement of not only MEK and PI3K signaling pathways but also others associated with glucose metabolism, fatty acid metabolism, gene transcription, histone methylation, iron transport, stress response, cell cycle, and apoptosis.Conclusion: Inhibiting RTK and RAF/MEK or PI3K could induce synergistic cytotoxicity but personalization is necessary. Examining colonies in agarose initiated by GICs from each patient may be useful for drug sensitivity testing in personalized cancer therapy. [ABSTRACT FROM AUTHOR]

Published

2016

4. Systematically characterizing and prioritizing chemosensitivity related gene based on Gene Ontology and protein interaction network

Author

Yan Li, Xiaowen Chen, Teng Huang, Xin Chen, Yingli Lv, Peng Wang, Xia Li, Wei Jiang, and Qianghu Wang

Subjects

lcsh:Internal medicine, lcsh:QH426-470, Antineoplastic Agents, Biology, Interaction network, Cell Line, Tumor, Neoplasms, Gene expression, Genetics, Humans, Genetics(clinical), Protein Interaction Maps, Related gene, lcsh:RC31-1245, Gene, Genetics (clinical), Molecular Sequence Annotation, Human genetics, Gene Expression Regulation, Neoplastic, lcsh:Genetics, ROC Curve, Cancer cell, Identification (biology), DNA microarray, Drug Screening Assays, Antitumor, Research Article, Genes, Neoplasm

Abstract

Background The identification of genes that predict in vitro cellular chemosensitivity of cancer cells is of great importance. Chemosensitivity related genes (CRGs) have been widely utilized to guide clinical and cancer chemotherapy decisions. In addition, CRGs potentially share functional characteristics and network features in protein interaction networks (PPIN). Methods In this study, we proposed a method to identify CRGs based on Gene Ontology (GO) and PPIN. Firstly, we documented 150 pairs of drug-CCRG (curated chemosensitivity related gene) from 492 published papers. Secondly, we characterized CCRGs from the perspective of GO and PPIN. Thirdly, we prioritized CRGs based on CCRGs’ GO and network characteristics. Lastly, we evaluated the performance of the proposed method. Results We found that CCRG enriched GO terms were most often related to chemosensitivity and exhibited higher similarity scores compared to randomly selected genes. Moreover, CCRGs played key roles in maintaining the connectivity and controlling the information flow of PPINs. We then prioritized CRGs using CCRG enriched GO terms and CCRG network characteristics in order to obtain a database of predicted drug-CRGs that included 53 CRGs, 32 of which have been reported to affect susceptibility to drugs. Our proposed method identifies a greater number of drug-CCRGs, and drug-CCRGs are much more significantly enriched in predicted drug-CRGs, compared to a method based on the correlation of gene expression and drug activity. The mean area under ROC curve (AUC) for our method is 65.2%, whereas that for the traditional method is 55.2%. Conclusions Our method not only identifies CRGs with expression patterns strongly correlated with drug activity, but also identifies CRGs in which expression is weakly correlated with drug activity. This study provides the framework for the identification of signatures that predict in vitro cellular chemosensitivity and offers a valuable database for pharmacogenomics research.

Published

2012

5. Systematically characterizing and prioritizing chemosensitivity related gene based on Gene Ontology and protein interaction network.

Author

Xin Chen, Wei Jiang, Qianghu Wang, Teng Huang, Peng Wang, Yan Li, Xiaowen Chen, Yingli Lv, and Xia Li

Subjects

GENES, GENE expression, ANTINEOPLASTIC agents, CANCER chemotherapy, CANCER cells, GENETIC regulation

Abstract

Background: The identification of genes that predict in vitro cellular chemosensitivity of cancer cells is of great importance. Chemosensitivity related genes (CRGs) have been widely utilized to guide clinical and cancer chemotherapy decisions. In addition, CRGs potentially share functional characteristics and network features in protein interaction networks (PPIN). Methods: In this study, we proposed a method to identify CRGs based on Gene Ontology (GO) and PPIN. Firstly, we documented 150 pairs of drug-CCRG (curated chemosensitivity related gene) from 492 published papers. Secondly, we characterized CCRGs from the perspective of GO and PPIN. Thirdly, we prioritized CRGs based on CCRGs' GO and network characteristics. Lastly, we evaluated the performance of the proposed method. Results: We found that CCRG enriched GO terms were most often related to chemosensitivity and exhibited higher similarity scores compared to randomly selected genes. Moreover, CCRGs played key roles in maintaining the connectivity and controlling the information flow of PPINs. We then prioritized CRGs using CCRG enriched GO terms and CCRG network characteristics in order to obtain a database of predicted drug-CRGs that included 53 CRGs, 32 of which have been reported to affect susceptibility to drugs. Our proposed method identifies a greater number of drug-CCRGs, and drug-CCRGs are much more significantly enriched in predicted drug-CRGs, compared to a method based on the correlation of gene expression and drug activity. The mean area under ROC curve (AUC) for our method is 65.2%, whereas that for the traditional method is 55.2%. Conclusions: Our method not only identifies CRGs with expression patterns strongly correlated with drug activity, but also identifies CRGs in which expression is weakly correlated with drug activity. This study provides the framework for the identification of signatures that predict in vitro cellular chemosensitivity and offers a valuable database for pharmacogenomics research. [ABSTRACT FROM AUTHOR]

Published

2012