Your search keyword '"Xiaodan Yao"' showing total 23 results

1. The suppression of HSPA8 attenuates NLRP3 ubiquitination through SKP2 to promote pyroptosis in sepsis-induced lung injury

Author

Jinlian Liu, Ke Song, Bingqi Lin, Zhenfeng Chen, Yan Liu, Xianshuai Qiu, Qi He, Zirui Zuo, Xiaodan Yao, Xiaoxia Huang, Zhuanhua Liu, Zhifeng Liu, Qiaobing Huang, and Xiaohua Guo

Subjects

HSPA8, SKP2, NLRP3 inflammasome, Pyroptosis, Alveolar epithelial cells, Acute lung injury, Biotechnology, TP248.13-248.65, Biology (General), QH301-705.5, Biochemistry, QD415-436

Abstract

Abstract Background Acute lung injury (ALI) is strongly associated with hospitalization and mortality in patients with sepsis. Recent evidence suggests that pyroptosis mediated by NLRP3(NOD-, LRR- and pyrin domain-containing 3) inflammasome activation plays a key role in sepsis. However, the mechanism of NLRP3 inflammasome activation in sepsis-induced lung injury remains unclear. Results in this study, we demonstrated that NLRP3 inflammasome was activated by the down-regulation of heat shock protein family A member 8 (HSPA8) in Lipopolysaccharide (LPS) and adenosine triphosphate (ATP)-treated mouse alveolar epithelial cells (AECs). Geranylgeranylacetone (GGA)-induced HSPA8 overexpression in cecum ligation and puncture (CLP) mice could significantly reduce systemic inflammatory response and mortality, effectively protect lung function, whilst HSPA8 inhibitor VER155008 aggravated this effect. The inhibition of HSPA8 was involved in sepsis induced acute lung injury by promoting pyroptosis of AECs. The down-regulation of HSPA8 activated NLRP3 inflammasome to mediate pyroptosis by promoting the degradation of E3 ubiquitin ligase S-phase kinase-associated protein 2 (SKP2). In addition, when stimulated by LPS and ATP, down-regulated SKP2 promoted pyroptosis of AECs by further attenuating ubiquitination of NLRP3. Adeno-associated virus 9-SKP2(AAV9-SKP2) could promote NLRP3 ubiquitination and degradation, alleviate lung injury and inhibit systemic inflammatory response in vivo. Conclusion in summary, our study shows there is strong statistical evidence that the suppression of HSPA8 mediates alveolar epithelial pyroptosis by promoting the degradation of E3 ubiquitin ligase SKP2 and subsequently attenuating the ubiquitination of NLRP3 to activate the NLRP3 inflammasome, which provides a new perspective and therapeutic target for the treatment of sepsis-induced lung injury.

Published

2024

2. Endothelial β-catenin upregulation and Y142 phosphorylation drive diabetic angiogenesis via upregulating KDR/HDAC9

Author

Zhenfeng Chen, Bingqi Lin, Xiaodan Yao, Jie Weng, Jinlian Liu, Qi He, Ke Song, Chuyu Zhou, Zirui Zuo, Xiaoxia Huang, Zhuanhua Liu, Qiaobing Huang, Qiulin Xu, and Xiaohua Guo

Subjects

Diabetic angiogenesis, Advanced glycation end products, β-catenin, Phosphorylation, KDR, HDAC9, Medicine, Cytology, QH573-671

Abstract

Abstract Background Diabetic angiogenesis is closely associated with disabilities and death caused by diabetic microvascular complications. Advanced glycation end products (AGEs) are abnormally accumulated in diabetic patients and are a key pathogenic factor for diabetic angiogenesis. The present study focuses on understanding the mechanisms underlying diabetic angiogenesis and identifying therapeutic targets based on these mechanisms. Methods In this study, AGE-induced angiogenesis serves as a model to investigate the mechanisms underlying diabetic angiogensis. Mouse aortic rings, matrigel plugs, and HUVECs or 293T cells were employed as research objects to explore this pathological process by using transcriptomics, gene promoter reporter assays, virtual screening and so on. Results Here, we found that AGEs activated Wnt/β-catenin signaling pathway and enhanced the β-catenin protein level by affecting the expression of β-catenin degradation-related genes, such as FZDs (Frizzled receptors), LRPs (LDL Receptor Related Proteins), and AXIN1. AGEs could also mediate β-catenin Y142 phosphorylation through VEGFR1 isoform5. These dual effects of AGEs elevated the nuclear translocation of β-catenin and sequentially induced the expression of KDR (Kinase Insert Domain Receptor) and HDAC9 (Histone Deacetylase 9) by POU5F1 and NANOG, respectively, thus mediating angiogenesis. Finally, through virtual screening, Bioymifi, an inhibitor that blocks VEGFR1 isoform5-β-catenin complex interaction and alleviates AGE-induced angiogenesis, was identified. Conclusion Collectively, this study offers insight into the pathophysiological functions of β-catenin in diabetic angiogenesis.

Published

2024

3. GRK3 is a poor prognosticator and serves as a therapeutic target in advanced gastric adenocarcinoma

Author

Yuan Li, Yibo Fan, Jinbang Xu, Longfei Huo, Ailing W. Scott, Jiankang Jin, Boxuan Yang, Shan Shao, Lang Ma, Ying Wang, Xiaodan Yao, Melissa Pool Pizzi, Matheus Sewastjanow Da Silva, Guoliang Zhang, Lijuan Zhuo, Eun Jeong Cho, Kevin N. Dalby, Namita D. Shanbhag, Zhenning Wang, Wenliang Li, Shumei Song, and Jaffer A. Ajani

Subjects

Gastric adenocarcinoma, GRK3, Hippo/YAP1, Prognosis, Peritoneal metastases, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Background G protein-coupled receptor (GPCR) is the most targeted protein family by the FDA-approved drugs. GPCR-kinase 3 (GRK3) is critical for GPCR signaling. Our genomic analysis showed that GRK3 expression correlated with poor prognosis of gastric adenocarcinoma (GAC) patients. However, GRK3’s functions and clinical utility in GAC progression and metastases are unknown. Methods We studied GRK3 expression in normal, primary, and metastatic GAC tissues. We identified a novel GRK3 inhibitor, LD2, through a chemical-library screen. Through genetic and pharmacologic modulations of GRK3, a series of functional and molecular studies were performed in vitro and in vivo. Impact of GRK3 on YAP1 and its targets was determined. Results GRK3 was overexpressed in GAC tissues compared to normal and was even higher in peritoneal metastases. Overexpression (OE) of GRK3 was significantly associated with shorter survival. Upregulation of GRK3 in GAC cells increased cell invasion, colony formation, and proportion of ALDH1 + cells, while its downregulation reduced these attributes. Further, LD2 potently and specifically inhibited GRK3, but not GRK2, a very similar kinase to GRK3. LD2 highly suppressed GAC cells’ malignant phenotypes in vitro. Mechanistically, GRK3 upregulated YAP1 in GAC tissues and its transcriptional downstream targets: SOX9, Birc5, Cyr61 and CTGF. Knockdown (KD) YAP1 rescued the phenotypes of GRK3 OE in GAC cells. GRK3 OE significantly increased tumor growth but LD2 inhibited tumor growth in the PDX model and dramatically suppressed peritoneal metastases induced by GRK3 OE. Conclusions GRK3, a poor prognosticator for survival, conferred aggressive phenotype. Genetic silencing of GRK3 or its inhibitor LD2 blunted GRK3-conferred malignant attributes, suggesting GRK3 as a novel therapeutic target in advanced GAC.

Published

2022

4. A new intronic quantitative PCR method led to the discovery of transformation from human ascites to murine malignancy in a mouse model

Author

Jiankang Jin, Longfei Huo, Yibo Fan, Ruiping Wang, Ailing W. Scott, Melissa Pool Pizzi, Xiaodan Yao, Shan Shao, Lang Ma, Matheus S. Da Silva, Kohei Yamashita, Katsuhiro Yoshimura, Boyu Zhang, Jingjing Wu, Linghua Wang, Shumei Song, and Jaffer A. Ajani

Subjects

intronic genomic qPCR, authentication and quantification of human and murine samples, patient-derived xenograft (PDX), human-to-murine oncogenic transformation, whole exosome sequencing (WES), tumor microenvironment (TME), Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

PurposeTo establish a fast and accurate detection method for interspecies contaminations in the patient-derived xenograft (PDX) models and cell lines, and to elucidate possible mechanisms if interspecies oncogenic transformation is detected.MethodsA fast and highly sensitive intronic qPCR method detecting Gapdh intronic genomic copies was developed to quantify if cells were human or murine or a mixture. By this method, we documented that murine stromal cells were abundant in the PDXs; we also authenticated our cell lines to be human or murine.ResultsIn one mouse model, GA0825-PDX transformed murine stromal cells into a malignant tumorigenic murine P0825 cell line. We traced the timeline of this transformation and discovered three subpopulations descended from the same GA0825-PDX model: epithelium-like human H0825, fibroblast-like murine M0825, and main passaged murine P0825 displayed differences in tumorigenic capability in vivo. P0825 was the most aggressive and H0825 was weakly tumorigenic. Immunofluorescence (IF) staining revealed that P0825 cells highly expressed several oncogenic and cancer stem cell markers. Whole exosome sequencing (WES) analysis revealed that TP53 mutation in the human ascites IP116-generated GA0825-PDX may have played a role in the human-to-murine oncogenic transformation.ConclusionThis intronic qPCR is able to quantify human/mouse genomic copies with high sensitivity and within a time frame of a few hours. We are the first to use intronic genomic qPCR for authentication and quantification of biosamples. Human ascites transformed murine stroma into malignancy in a PDX model.

Published

2023

5. Patient-derived cell lines and orthotopic mouse model of peritoneal carcinomatosis recapitulate molecular and phenotypic features of human gastric adenocarcinoma

Author

Shumei Song, Yan Xu, Longfei Huo, Shuangtao Zhao, Ruiping Wang, Yuan Li, Ailing W. Scott, Melissa Pool Pizzi, Ying Wang, Yibo Fan, Kazuto Harada, Jiankang Jin, Lang Ma, Xiaodan Yao, Namita D. Shanbhag, Qiong Gan, Sinchita Roy-Chowdhuri, Brian D. Badgwell, Zhenning Wang, Linghua Wang, and Jaffer A. Ajani

Subjects

Gastric adenocarcinoma, Peritoneal metastases, Patient-derived cell lines, Patient-derived xenograft, molecular profile, Patient-derived orthotopic model, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Background Gastric adenocarcinoma with peritoneal carcinomatosis (PC) is therapy resistant and leads to poor survival. To study PC in depth, there is an urgent need to develop representative PC-derived cell lines and metastatic models to study molecular mechanisms of PC and for preclinical screening of new therapies. Methods PC cell lines were developed from patient-derived PC cells. The tumorigenicity and metastatic potential were investigated by subcutaneously (PDXs) and orthotopically. Karyotyping, whole-exome sequencing, RNA-sequencing, and functional studies were performed to molecularly define the cell lines and compare genomic and phenotypic features of PDX and donor PC cells. Results We established three PC cell lines (GA0518, GA0804, and GA0825) and characterized them in vitro. The doubling times were 22, 39, and 37 h for GA0518, GA0804, and GA0825, respectively. Expression of cancer stem cell markers (CD44, ALDH1, CD133 and YAP1) and activation of oncogenes varied among the cell lines. All three PC cell lines formed PDXs. Interestingly, all three PC cell lines formed tumors in the patient derived orthotopic (PDO) model and GA0518 cell line consistently produced PC in mice. Moreover, PDXs recapitulated transcriptomic and phenotypic features of the donor PC cells. Finally, these cell lines were suitable for preclinical testing of chemotherapy and target agents in vitro and in vivo. Conclusion We successfully established three patient-derived PC cell lines and an improved PDO model with high incidence of PC associated with malignant ascites. Thus, these cell lines and metastatic PDO model represent excellent resources for exploring metastatic mechanisms of PC in depth and for target drug screening and validation by interrogating GAC for translational studies.

Published

2021

6. An improved strategy for CRISPR/Cas9 gene knockout and subsequent wildtype and mutant gene rescue.

Author

Jiankang Jin, Yan Xu, Longfei Huo, Lang Ma, Ailing W Scott, Melissa Pool Pizzi, Yuan Li, Ying Wang, Xiaodan Yao, Shumei Song, and Jaffer A Ajani

Subjects

Medicine, Science

Abstract

A fluorescence marker mOrange was inserted to the popular pLentiCrispr-V2 to create pLentiCrispr-V2-mOrange (V2mO) that contained both a puromycin selection and a fluorescent marker, making viral production and target transduction visible. Lentiviruses packaged with this plasmid and appropriate guide RNAs (gRNAs) successfully knocked out the genes RhoA, Gli1, and Gal3 in human gastric cancer cell lines. Cas9-gRNA editing efficiency could be estimated directly from Sanger electropherograms of short polymerase chain reaction products around the gRNA regions in Cas9-gRNA transduced cells. Single cloning of transduced target cell pools must be performed to establish stable knockout clones. Rescue of wildtype (RhoA and Gal3) and mutant (RhoA.Y42C) genes into knockout cells was successful only when cDNAs, where gRNAs bind, were modified by three nucleotides while the amino acid sequences remained unchanged. Stringent on-target CRISPR/Cas9 editing was observed in Gal3 gene, but not in RhoA gene since RhoA.Y42C already presented a nucleotide change in gRNA5 binding site. In summary, our improved strategy added these advantages: adding visual marker to the popular lentiviral system, monitoring lentiviral production and transduction efficiencies, cell-sorting Cas9+ cells in target cells by fluorescence-activated cell sorting, direct estimation of gene editing efficiency of target cell pools by short PCR electropherograms around gRNA binding sites, and successful rescue of wildtype and mutant genes in knockout cells, overcoming Cas9 editing by modifying cDNAs.

Published

2020

7. Patient-derived cell lines and orthotopic mouse model of peritoneal carcinomatosis recapitulate molecular and phenotypic features of human gastric adenocarcinoma

Author

Zhenning Wang, Xiaodan Yao, Qiong Gan, Jiankang Jin, Ruiping Wang, Yan Xu, Ying Wang, Brian D. Badgwell, Jaffer A. Ajani, Kazuto Harada, Linghua Wang, Shuangtao Zhao, Longfei Huo, Ailing W. Scott, Namita Shanbhag, Lang Ma, Shumei Song, Melissa Pool Pizzi, Yibo Fan, Yuan Li, and Sinchita Roy-Chowdhuri

Subjects

0301 basic medicine, Cancer Research, Patient-derived xenograft, molecular profile, Patient-derived orthotopic model, Adenocarcinoma, Transcriptome, 03 medical and health sciences, Mice, 0302 clinical medicine, In vivo, Cancer stem cell, Stomach Neoplasms, Cell Line, Tumor, Exome Sequencing, Animals, Humans, Gene Regulatory Networks, Peritoneal Neoplasms, RC254-282, YAP1, biology, Gastric adenocarcinoma, Sequence Analysis, RNA, Gene Expression Profiling, Research, CD44, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, In vitro, Gene Expression Regulation, Neoplastic, 030104 developmental biology, Peritoneal metastases, Oncology, Apoptosis, Cell culture, 030220 oncology & carcinogenesis, Karyotyping, biology.protein, Cancer research, Neoplasm Transplantation, Patient-derived cell lines

Abstract

Background Gastric adenocarcinoma with peritoneal carcinomatosis (PC) is therapy resistant and leads to poor survival. To study PC in depth, there is an urgent need to develop representative PC-derived cell lines and metastatic models to study molecular mechanisms of PC and for preclinical screening of new therapies. Methods PC cell lines were developed from patient-derived PC cells. The tumorigenicity and metastatic potential were investigated by subcutaneously (PDXs) and orthotopically. Karyotyping, whole-exome sequencing, RNA-sequencing, and functional studies were performed to molecularly define the cell lines and compare genomic and phenotypic features of PDX and donor PC cells. Results We established three PC cell lines (GA0518, GA0804, and GA0825) and characterized them in vitro. The doubling times were 22, 39, and 37 h for GA0518, GA0804, and GA0825, respectively. Expression of cancer stem cell markers (CD44, ALDH1, CD133 and YAP1) and activation of oncogenes varied among the cell lines. All three PC cell lines formed PDXs. Interestingly, all three PC cell lines formed tumors in the patient derived orthotopic (PDO) model and GA0518 cell line consistently produced PC in mice. Moreover, PDXs recapitulated transcriptomic and phenotypic features of the donor PC cells. Finally, these cell lines were suitable for preclinical testing of chemotherapy and target agents in vitro and in vivo. Conclusion We successfully established three patient-derived PC cell lines and an improved PDO model with high incidence of PC associated with malignant ascites. Thus, these cell lines and metastatic PDO model represent excellent resources for exploring metastatic mechanisms of PC in depth and for target drug screening and validation by interrogating GAC for translational studies.

Published

2021

8. Loss of ARID1A activates mTOR signaling and SOX9 in gastric adenocarcinoma—rationale for targeting ARID1A deficiency

Author

Yan Xu, Lulu Wang, Ruiping Wang, Ying Wang, Ailing W. Scott, Lang Ma, Melissa Pool Pizzi, Xiaodan Yao, Zhenning Wang, Yuan Li, Shumei Song, Yibo Fan, Xiaochuan Dong, Linghua Wang, Jaffer A. Ajani, Wei Zhao, Longfei Huo, Jiangkang Jin, Randy L. Johnson, and Guang Peng

Subjects

Gene knockdown, ARID1A, biology, Chemistry, Gastroenterology, Cancer, medicine.disease, Gene expression, Cancer cell, medicine, Cancer research, biology.protein, Phosphorylation, Mechanistic target of rapamycin, PI3K/AKT/mTOR pathway

Abstract

BackgroundGastric adenocarcinoma (GAC) is a lethal disease with limited therapeutic options. Genetic alterations in chromatin remodelling gene AT-rich interactive domain 1A (ARID1A) and mTOR pathway activation occur frequently in GAC. Targeting the mechanistic target of rapamycin (mTOR) pathway in unselected patients has failed to show survival benefit. A deeper understanding of GAC might identify a subset that can benefit from mTOR inhibition.MethodsGenomic alterations in ARID1A were analysed in GAC. Mouse gastric epithelial cells from CK19-Cre-Arid1Afl/fl and wild-type mice were used to determine the activation of oncogenic genes due to loss of Arid1A. Functional studies were performed to determine the significance of loss of ARID1A and the sensitivity of ARID1A-deficient cancer cells to mTOR inhibition in GAC.ResultsMore than 30% of GAC cases had alterations (mutations or deletions) of ARID1A and ARID1A expression was negatively associated with phosphorylation of S6 and SOX9 in GAC tissues and patient-derived xenografts (PDXs). Activation of mTOR signalling (increased pS6) and SOX9 nuclear expression were strongly increased in Arid1A−/− mouse gastric tissues which could be curtailed by RAD001, an mTOR inhibitor. Knockdown of ARID1A in GAC cell lines increased pS6 and nuclear SOX9 and increased sensitivity to an mTOR inhibitor which was further amplified by its combination with fluorouracil both in vitro and in vivo in PDXs.ConclusionsThe loss of ARID1A activates pS6 and SOX9 in GAC, which can be effectively targeted by an mTOR inhibitor. Therefore, our studies suggest a new therapeutic strategy of clinically targeting the mTOR pathway in patients with GAC with ARID1A deficiency.

Published

2021

9. Abstract 1612: Therapeutic co-targeting YAP1 and TAZ using antisense oligos (ASOs) suppress gastric cancer progression and peritoneal metastases

Author

Jingjing Wu, Ailing Scott, Yan Xu, Yuan Li, Yibo Fan, Ruiping Wang, Xiaodan Yao, Katsuhiro Yoshimura, Melissa Pool Pizzi, Kohei Yamashita, Shan Shao, Christopher Vellano, Linghua Wang, Alexey Revenko, Eric Dolinski, Jaffer A. Ajani, and Shumei Song

Subjects

Cancer Research, Oncology

Abstract

Gastric adenocarcinoma (GAC) is one of the most common malignancies worldwide and it is the fourth leading cause of cancer-related death. Peritoneal carcinomatosis (PC; malignant ascites or implants) in GAC patients is common and poses a challenge with short survival and lack of effective therapeutics. We and others have demonstrated that deregulation of the Hippo signaling pathway particularly with upregulation of its coactivators-YAP1 or TAZ drive cancer progression and metastases in gastroesophageal cancers suggesting YAP1 and TAZ are potential drug targets in solid tumors. However, discovery of effective drugs to target YAP1 or TAZ remains challenging due to the nuclear localization and lack of inhibitory pocket for YAP1 or TAZ. In this study, using scRNAseq and immunofluorescent staining, we observed that both YAP1, TAZ and their transcriptional factors-Tead1, Tead2, Tead3 and Tead4 are highly expressed in PC tumor cells and high expression of these proteins were associated with poorer prognosis. Further, we note that recently developed YAP or TAZ antisense oligonucleotides (ASO) can effectively and specifically suppress YAP or TAZ expression and transcription accompanied by decreased tumor cell invasion and tumor sphere formation. Further, we observed that YAP1 can interact with TAZ and both bind TEAD1,2,3 but not Tead4 transcriptional factors, while YAP1 ASO or TAZ ASO can decrease the interactions between YAP1 or TAZ with TEAD1,2,3 in GAC cells. Interestingly, inhibition of YAP1 or TAZ alone using the ASOs can complementarily increase the other at the protein and mRNA levels. Further, we revealed that YAP1 KO patient derived tumor cells (GA0518) are more sensitive to TAZ ASO than control cells and simultaneously inhibition of YAP1 and TAZ by ASOs reduces both YAP1and TAZ proteins and mRNA levels with significant decrease in cell proliferation and invasive capacity of YAP1 high tumor cells. Most importantly, co-targeting YAP and TAZ by the ASOs significantly attenuated progression and PC in the PDX model and sensitized to anti-PD1 immunotherapy in the KP-Luc syngeneic model. Taken together, our studies open a new avenue for developing novel therapeutic strategy by co-targeting both YAP1 and TAZ using the ASOs against GAC with PC. Keywords: Gastric Adenocarcinoma, YAP1, TAZ, Hippo pathway, Antisense Oligonucleotides (ASOs), Peritoneal Metastases, Targeted Therapy Citation Format: Jingjing Wu, Ailing Scott, Yan Xu, Yuan Li, Yibo Fan, Ruiping Wang, Xiaodan Yao, Katsuhiro Yoshimura, Melissa Pool Pizzi, Kohei Yamashita, Shan Shao, Christopher Vellano, Linghua Wang, Alexey Revenko, Eric Dolinski, Jaffer A. Ajani, Shumei Song. Therapeutic co-targeting YAP1 and TAZ using antisense oligos (ASOs) suppress gastric cancer progression and peritoneal metastases [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2023; Part 1 (Regular and Invited Abstracts); 2023 Apr 14-19; Orlando, FL. Philadelphia (PA): AACR; Cancer Res 2023;83(7_Suppl):Abstract nr 1612.

Published

2023

10. Epithelial SOX9 drives progression and metastases of gastric adenocarcinoma by promoting immunosuppressive tumour microenvironment.

Author

Yibo Fan, Yuan Li, Xiaodan Yao, Jiangkang Jin, Scott, Ailing, Liu, Bovey, Shan Wang, Longfei Huo, Ying Wang, Ruiping Wang, Pizzi, Melissa Pool, Lang Ma, Shan Shao, Sewastjanow-Silva, Matheus, Waters, Rebecca, Chatterjee, Deyali, Liu, Bin, Shanbhag, Namita, Guang Peng, and Calin, George Adrian

Subjects

XENOGRAFTS, SOX transcription factors, TUMOR microenvironment, PERITONEAL cancer, MACROPHAGE colony-stimulating factor, MONONUCLEAR leukocytes, PROSTATE cancer

Published

2023

11. Epithelial SOX9 drives progression and metastases of gastric adenocarcinoma by promoting immunosuppressive tumour microenvironment

Author

Yibo Fan, Yuan Li, Xiaodan Yao, Jiangkang Jin, Ailing Scott, Bovey Liu, Shan Wang, Longfei Huo, Ying Wang, Ruiping Wang, Melissa Pool Pizzi, Lang Ma, Shan Shao, Matheus Sewastjanow-Silva, Rebecca Waters, Deyali Chatterjee, Bin Liu, Namita Shanbhag, Guang Peng, George Adrian Calin, Pawel Karol Mazur, Samir M Hanash, Jo Ishizawa, Yuki Hirata, Osamu Nagano, Zhenning Wang, Linghua Wang, Wa Xian, Frank McKeon, Jaffer A Ajani, and Shumei Song

Subjects

Gastroenterology

Abstract

ObjectiveMany cancers engage embryonic genes for rapid growth and evading the immune system. SOX9 has been upregulated in many tumours, yet the role of SOX9 in mediating immunosuppressive tumour microenvironment is unclear. Here, we aim to dissect the role of SOX9-mediated cancer stemness attributes and immunosuppressive microenvironment in advanced gastric adenocarcinoma (GAC) for novel therapeutic discoveries.MethodsBulk RNAseq/scRNA-seq, patient-derived cells/models and extensive functional studies were used to identify the expression and functions of SOX9 and its target genes in vitro and in vivo. Immune responses were studied in PBMCs or CD45+immune cells cocultured with tumour cells with SOX9highor knockout and the KP-Luc2 syngeneic models were used for efficacy of combinations.ResultsSOX9 is one of the most upregulated SOX genes in GAC and highly expressed in primary and metastatic tissues and associated with poor prognosis. Depletion of SOX9 in patient-derived GAC cells significantly decreased cancer stemness attributes, tumour formation and metastases and consistently increased CD8+T cell responses when cocultured with PBMCs/CD45+cells from GAC patients. RNA sequencing identified the leukaemia inhibitory factor (LIF) as the top secreted molecule regulated by SOX9 in tumour cells and was enriched in malignant ascites and mediated SOX9-induced M2 macrophage repolarisation and inhibited T cell function.ConclusionEpithelial SOX9 is critical in suppressing CD8+T cell responses and modified macrophage function in GAC through the paracrine LIF factor. Cotargeting LIF/LIFR and CSF1R has great potential in targeting SOX9-mediated cancer stemness, T cell immunosuppression and metastases suggesting the novel combination therapy against advanced GAC.

Published

2021

12. Loss of ARID1A activates mTOR signaling and SOX9 in gastric adenocarcinoma-rationale for targeting

Author

Xiaochuan, Dong, Shumei, Song, Yuan, Li, Yibo, Fan, Lulu, Wang, Ruiping, Wang, Longfei, Huo, Ailing, Scott, Yan, Xu, Melissa Pool, Pizzi, Lang, Ma, Ying, Wang, Jiangkang, Jin, Wei, Zhao, Xiaodan, Yao, Randy L, Johnson, Linghua, Wang, Zhenning, Wang, Guang, Peng, and Jaffer A, Ajani

Subjects

DNA-Binding Proteins, Mice, Stomach Neoplasms, Cell Line, Tumor, TOR Serine-Threonine Kinases, Cell Culture Techniques, Animals, SOX9 Transcription Factor, Adenocarcinoma, Article, Cell Proliferation, Signal Transduction, Transcription Factors

Abstract

BACKGROUND: Gastric adenocarcinoma (GAC) is a lethal disease with limited therapeutic options. Genetic alterations in chromatin remodeling gene ARID1A and mTOR pathway activation occur frequently in GAC. Targeting the mTOR pathway in unselected patients has failed to show survival benefit. A deeper understanding of GAC might identify a subset that can benefit from mTOR pathway inhibition. METHODS: Genomic alterations in ARID1A were analyzed in GAC. Mouse gastric epithelial cells from CK19-Cre-Arid1A(−/−) and wild-type mice were used to determine the activation of oncogenic genes due to loss of Arid1A. Functional studies were performed to determine the significance of loss of ARID1A and the sensitivity of ARID1A-deficient cancer cells to mTOR inhibition in GAC. RESULTS: More than 30% of cases had alterations (mutations or deletions) of ARID1A and ARID1A expression was negatively associated with phosphorylation of S6 and SOX9 in GAC tissues and patient-derived xenografts (PDXs). Activation of mTOR signaling (increased pS6) and SOX9 nuclear expression were strongly increased in Arid1A(−/−) mouse gastric tissues which could be curtailed by RAD001, a mTOR inhibitor. Knockdown of ARID1A in GAC cell lines increased pS6 and nuclear SOX9 and increased sensitivity to an mTOR inhibitor which was further amplified by its combination with fluorouracil both in vitro and in vivo in PDXs. CONCLUSIONS: The loss of ARID1A activates pS6 and SOX9 in GAC, which can be effectively targeted by a mTOR inhibitor. Therefore, our studies suggest a new therapeutic strategy of clinically targeting the mTOR pathway in GAC patients with ARID1A deficiency.

Published

2020

13. Loss of ARID1A activates mTOR signaling and SOX9 in gastric adenocarcinoma—rationale for targeting ARID1A deficiency.

Author

Xiaochuan Dong, Shumei Song, Yuan Li, Yibo Fan, Lulu Wang, Ruiping Wang, Longfei Huo, Scott, Ailing, Yan Xu, Pizzi, Melissa Pool, Lang Ma, Ying Wang, Jiangkang Jin, Wei Zhao, Xiaodan Yao, Johnson, Randy L., Linghua Wang, Zhenning Wang, Guang Peng, and Ajani, Jaffer A.

Subjects

SOX transcription factors, HEARTBURN, ESOPHAGEAL cancer, HEPATITIS C

Published

2022

14. YAP1 mediates gastric adenocarcinoma peritoneal metastases that are attenuated by YAP1 inhibition

Author

Makoto Kobayashi, Samir M. Hanash, Ghia Tatlonghari, Longfei Huo, Ying Wang, Xiaodan Yao, Lang Ma, Jiankang Jin, Namita Shanbhag, Zhenning Wang, Guang Peng, Shumei Song, Randy L. Johnson, Jaffer A. Ajani, Yan Xu, Kazuto Harada, Ju Seog Lee, Ruiping Wang, Brian D. Badgwell, George A. Calin, Jeannelyn S. Estrella, Linghua Wang, Melissa Pool Pizzi, Jody Vykoukal, Yuan Li, Sinchita Roy-Chowdhuri, Wei Zhao, Xiaochuan Dong, and Ailing W. Scott

Subjects

0301 basic medicine, Cell, Cell Culture Techniques, Adenocarcinoma, Molecular oncology, 03 medical and health sciences, Mice, 0302 clinical medicine, Downregulation and upregulation, In vivo, Cancer stem cell, Stomach Neoplasms, medicine, Animals, Humans, Peritoneal Neoplasms, Adaptor Proteins, Signal Transducing, Oncogene, Chemistry, Gastroenterology, YAP-Signaling Proteins, Xenograft Model Antitumor Assays, In vitro, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Cancer research, Immunohistochemistry

Abstract

ObjectivePeritoneal carcinomatosis (PC; malignant ascites or implants) occurs in approximately 45% of advanced gastric adenocarcinoma (GAC) patients and associated with a poor survival. The molecular events leading to PC are unknown. The yes-associated protein 1 (YAP1) oncogene has emerged in many tumour types, but its clinical significance in PC is unclear. Here, we investigated the role of YAP1 in PC and its potential as a therapeutic target.MethodsPatient-derived PC cells, patient-derived xenograft (PDX) and patient-derived orthotopic (PDO) models were used to study the function of YAP1 in vitro and in vivo. Immunofluorescence and immunohistochemical staining, RNA sequencing (RNA-Seq) and single-cell RNA-Seq (sc-RNA-Seq) were used to elucidate the expression of YAP1 and PC cell heterogeneity. LentiCRISPR/Cas9 knockout of YAP1 and a YAP1 inhibitor were used to dissect its role in PC metastases.ResultsYAP1 was highly upregulated in PC tumour cells, conferred cancer stem cell (CSC) properties and appeared to be a metastatic driver. Dual staining of YAP1/EpCAM and sc-RNA-Seq revealed that PC tumour cells were highly heterogeneous, YAP1high PC cells had CSC-like properties and easily formed PDX/PDO tumours but also formed PC in mice, while genetic knockout YAP1 significantly slowed tumour growth and eliminated PC in PDO model. Additionally, pharmacologic inhibition of YAP1 specifically reduced CSC-like properties and suppressed tumour growth in YAP1high PC cells especially in combination with cytotoxics in vivo PDX model.ConclusionsYAP1 is essential for PC that is attenuated by YAP1 inhibition. Our data provide a strong rationale to target YAP1 in clinic for GAC patients with PC.

Published

2019

15. An improved strategy for CRISPR/Cas9 gene knockout and subsequent wildtype and mutant gene rescue

Author

Ying Wang, Ailing W. Scott, Jiankang Jin, Jaffer A. Ajani, Yuan Li, Longfei Huo, Melissa Pool Pizzi, Shumei Song, Yan Xu, Xiaodan Yao, and Lang Ma

Subjects

RHOA, Mutant, Artificial Gene Amplification and Extension, Tides, Biochemistry, Polymerase Chain Reaction, Transduction (genetics), Gene Knockout Techniques, Guide RNA, Database and Informatics Methods, 0302 clinical medicine, CRISPR, Clustered Regularly Interspaced Short Palindromic Repeats, Gene Editing, 0303 health sciences, Multidisciplinary, Physics, Gene Pool, Cell biology, Nucleic acids, Geophysics, 030220 oncology & carcinogenesis, Physical Sciences, Medicine, Genetic Engineering, Sequence Analysis, Plasmids, RNA, Guide, Kinetoplastida, Research Article, Bioinformatics, Science, Genetic Vectors, Nucleotide Sequencing, Biology, DNA construction, Research and Analysis Methods, 03 medical and health sciences, Cell Line, Tumor, Genetics, Humans, Molecular Biology Techniques, Sequencing Techniques, Gene, Molecular Biology, Gene knockout, 030304 developmental biology, Fluorescent Dyes, Evolutionary Biology, Biology and life sciences, Population Biology, Cas9, Lentivirus, Plasmid Construction, biology.protein, Earth Sciences, RNA, CRISPR-Cas Systems, Sequence Alignment, Population Genetics, Cloning

Abstract

A fluorescence marker mOrange was inserted to the popular pLentiCrispr-V2 to create pLentiCrispr-V2-mOrange (V2mO) that contained both a puromycin selection and a fluorescent marker, making viral production and target transduction visible. Lentiviruses packaged with this plasmid and appropriate guide RNAs (gRNAs) successfully knocked out the genes RhoA, Gli1, and Gal3 in human gastric cancer cell lines. Cas9-gRNA editing efficiency could be estimated directly from Sanger electropherograms of short polymerase chain reaction products around the gRNA regions in Cas9-gRNA transduced cells. Single cloning of transduced target cell pools must be performed to establish stable knockout clones. Rescue of wildtype (RhoA and Gal3) and mutant (RhoA.Y42C) genes into knockout cells was successful only when cDNAs, where gRNAs bind, were modified by three nucleotides while the amino acid sequences remained unchanged. Stringent on-target CRISPR/Cas9 editing was observed in Gal3 gene, but not in RhoA gene since RhoA.Y42C already presented a nucleotide change in gRNA5 binding site. In summary, our improved strategy added these advantages: adding visual marker to the popular lentiviral system, monitoring lentiviral production and transduction efficiencies, cell-sorting Cas9+ cells in target cells by fluorescence-activated cell sorting, direct estimation of gene editing efficiency of target cell pools by short PCR electropherograms around gRNA binding sites, and successful rescue of wildtype and mutant genes in knockout cells, overcoming Cas9 editing by modifying cDNAs.

Published

2019

16. Molecular biology and immunology of gastric cancer peritoneal metastasis

Author

Xiaodan Yao, Shumei Song, and Jaffer A. Ajani

Subjects

0301 basic medicine, Cellular immunity, Peritoneal metastasis, Hepatology, business.industry, medicine.medical_treatment, Gastroenterology, Treatment options, Cancer, Review Article, Immunotherapy, medicine.disease, Molecular biology, Targeted therapy, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, 030220 oncology & carcinogenesis, medicine, Overall survival, Signal transduction, business

Abstract

Peritoneal metastases occur in 55-60% of patients with gastric cancer (GC) and are associated with a 2% 5-year overall survival rate. There are limited treatment options for these patients, and no targeted therapy or immunotherapy is available. Rational therapeutic targets remain to be found. In this review, we present the published literature and our own recent experience in molecular biology to identify important molecules and signaling pathways as well as cellular immunity involved in the peritoneal metastasis of GC. We also suggest potential novel strategies for improving the outcomes of GC patients with peritoneal metastasis.

Published

2020

17. Idiopathic IgA Nephropathy with Diffuse Crescent Formation

Author

Huiping Chen, Leishi Li, Zhihong Liu, Yusheng Yu, Qingwen Wang, Xiaodan Yao, Zheng Tang, Wei-xing Hu, and Yan Wu

Subjects

Adult, Male, Pathology, medicine.medical_specialty, Nephrotic Syndrome, CD8 Antigens, Antigens, Differentiation, Myelomonocytic, urologic and male genital diseases, Nephropathy, Pathogenesis, Glomerulonephritis, Antigens, CD, Immunopathology, medicine, Humans, Hematuria, urogenital system, business.industry, Follow up studies, food and beverages, Glomerulonephritis, IGA, medicine.disease, female genital diseases and pregnancy complications, Immunoglobulin A, Immunoglobulin M, Nephrology, Creatinine, CD4 Antigens, Hypertension, Clinicopathological features, Female, Creatinine blood, business, Follow-Up Studies, Kidney disease

Abstract

Objective: To investigate the clinicopathological features and outcome of idiopathic IgA nephropathy with diffuse crescent formation in Chinese patients. Methods: Twenty-five patients with diffuse crescentic IgA nephropathy (DCIgAN), 15 males and 10 females with median age of 28.5, and median disease duration of 5.1 months, were studied. Their clinical, laboratory and pathological features and outcome were investigated. Twenty-one were administered pulse immunosuppressive therapy, and 15 were followed up for more than 6 months. Results: 1.14% had total IgA nephropathy, and 16.4% total diffuse crescentic glomerulonephritis. Clinically, most of patients (88%) showed rapidly progressive glomerulonephritis associated with a high level of serum creatinine (418 ± 264 µmol/l). Gross hematuria was noted in 72%, hypertension in 64%, and nephrotic syndrome in 48%. Pathologically, except for diffuse crescent formation (a median 65% and range 50–95%), we observed segmental necrosis of glomerular capillaries in 60%, glomerular infiltrating cells in 48%, endothelial cells proliferation in 32%, and rupture of Bowmans’ capsule in 24%. Severe tubular interstitial damage was also found, tubular atrophy in 64%, interstitial fibrosis in 60%, diffuse interstitial infiltrating cells in 74%, and interstitial vasculitis in 40%. Immunopathologically, four phenotypes were observed; however, IgA associated with IgM deposition was higher than that in patients with general IgA nephropathy (IgAN). In addition, the infiltrating CD4+, CD8+, CD68+ and PCNA+ cells in renal tissue were significantly high compared with that in controls. In a follow-up study, 66.7% of patients had life-sustaining renal function, 4 of them had normal range of serum creatinine (Conclusions: The patients with crescentic IgA nephropathy mostly show rapidly progressive nephritis associated with more severe pathological changes including glomerular, tubular interstitial and vascular lesions than in patients with general IgAN. The infiltrates in glomeruli may contribute to the crescentic formation, and the intensive immune suppressing treatment is useful to improve renal damage in patients with DCIgAN.

Published

2002

18. Molecular Genetics and Gene Therapy Aspects of Phenylalanine Hydroxylase (PAH) Related Hyperphenylalaninemias

Author

Youming Zhang and Xiaodan Yao

Subjects

chemistry.chemical_classification, congenital, hereditary, and neonatal diseases and abnormalities, medicine.medical_specialty, integumentary system, Phenylalanine hydroxylase, Genetic enhancement, Phenylalanine, Biology, Prescription drug abuse, eye diseases, Amino acid, Biochemistry, chemistry, Molecular genetics, Liver enzyme, otorhinolaryngologic diseases, medicine, biology.protein, Tyrosine

Abstract

Hyperphenylalaninemias (HPAs; OMIM 261600) are related to phenylalanine hydroxylase (PAH; OMIM *612349) deficiency; a hepatic enzyme, and are characterized by moderate and/or high levels of the amino acid phenylalanine and reduction of tyrosine. High levels of phenylalanine and low of tyrosine characterize phenylketonuria (PKU; OMIM 261600) disease whereas moderately increased levels of phenylalanine and/or reduced or normal levels of tyrosine are usually

Published

2014

19. The clinical and pathological characteristics of Chinese patients with pauci‐immune crescentic glomerulonephritis

Author

Xiaodan Yao, Weixin Hu, Leishi Li, Zheng Tang, Huiping Chen, and Yan Wu

Subjects

HBsAg, medicine.medical_specialty, business.industry, Crescentic glomerulonephritis, MEDLINE, General Medicine, Hepatitis C, medicine.disease, Hiv risk, Nephrology, Accidental, Pauci-immune, Immunology, medicine, medicine.symptom, Intensive care medicine, business, Pathological

Abstract

The search for quality in the health service cannot lead aside the safety of its operators and users, subject to the well defined parameters of Law 626. This study makes a preliminary examination of the accidents occurring in our Health District which comprises three hospitals, 600 beds and 1,800 employees. A total of 172 accidents have been reported. The percentages can be broken down between the various sectors: 73% of accidents involve nurses, 9% involve doctors and 1% administrative personnel. The greatest risk in hemodialysis is the biological factor (through accidental cuts or pricks which account for 67% of the accidents reported) and involves humans (both patients and personnel), monitors and environments as the sources of pathogens. The most frequently isolated germs are E. coli and Pseudomonas. It has been shown that prevention is above all based on the accuracy with which procedures are followed. The risk of hepatitis C has not yet been resolved, as is affinned in a review reported in the study. The HIV risk gives the greatest cause for concern, even if only 0.2% after exposure compared to 15-36 for HbsAg. Compliance with universal rules for prevention and post-exposure procedures provides an adequate guarantee for prevention.

Published

2000

20. Cyclosporine A in treatment of membranous lupus nephropathy

Author

Weixin, Hu, Zhihong, Liu, Shuqiong, Shen, Shijun, Li, Xiaodan, Yao, Huiping, Chen, and Leishi, Li

Subjects

Adult, Male, Treatment Outcome, Adolescent, Cyclosporine, Humans, Prednisone, Female, Glomerulonephritis, Membranous, Lupus Nephritis, Retrospective Studies

Abstract

To investigate retrospectively the efficacy of cyclosporine A (CsA) in the treatment of membranous lupus nephropathy (MLN).Twenty-four patients with systemic lupus erythematosus (SLE) and biopsy-proven MLN were treated with CsA in combination with prednisone. CsA was given at a starting dosage of 5 mg x kg(-1) x d(-1) for 3 months, with a 1 mg x kg(-1) x d(-1) reduction every month and then maintained at a dosage of 2 mg x kg(-1) x d(-1). The dosage of oral prednisone differed from person to person according to levels of extra-renal activity. Clinical efficacy and adverse reactions were retrospectively analyzed. Complete remission was defined as having a urinary proteinuria level (Upr) of0.4 g/d, and normal serum albumin and serum creatinine (SCr) levels, without SLE activity. Partial remission was defined as having a UPr decrement50% of baseline value and a serum albumin value of 30 - 35 g/L, without SLE activity. No response was defined as having a Upr decrement50% of baseline value and2.0 g/d, or as a deterioration of renal function, or as having active SLE.One patient could no longer undergo follow-up, and the other 23 patients were treated with CsA and followed up for 6 - 36 months (mean 16.8 +/- 8.4 months). The mean starting dosage of CsA was 4.7 +/- 0.5) mg x kg(-1) x d(-1) and the trough level of the whole blood CsA was 248 +/- 110) micro g/L. Twelve patients (52.2%) achieved complete remission, 10 patients (43.3%) achieved partial remission after CsA treatment, and one patient showed no response. At different CsA treatment timepoint, the complete remission rates were 17.4% (3rd month), 21.7% (6th month), 40% (12th month), 88.9% (18th month) and 100% (24th month) respectively. SCr elevation, when within a normal limit was not observed in most patients during early CsA administration, and at the end of the follow-up all the patients had a normal SCr. Relapse occurred in 33.3% of the patients after withdrawing CsA for 4 - 24 months. No chronic CsA renal toxicity was observed in 4 patients who had a repeat renal biopsy after CsA treatment for 6 - 24 months.CsA could be regarded as an effective therapy for patients with membranous lupus nephropathy, but its adverse effects, especially its nephrotoxicity, should be carefully monitored during CsA treatment.

Published

2003

21. Clinical spectrum of diffuse crescentic glomerulonephritis in Chinese patients

Author

Zheng, Tang, Yan, Wu, Qingwen, Wang, Caihong, Zeng, Xiaodan, Yao, Weixin, Hu, Huiping, Chen, Zhihong, Liu, and Leishi, Li

Subjects

Adult, Male, China, Glomerulonephritis, Adolescent, Humans, Female, Middle Aged, Child, Aged

Abstract

To investigate retrospectively the incidence, distribution of primary disease and clinicopathologic characteristics of diffuse crescentic glomerulonephritis (DCGN) in Chinese patients.One hundred and seventy-two consecutive patients diagnosed as having DCGN out of 9828 cases of non-transplanting renal biopsies over sixteen years, were studied. DCGN is categorized into three types according to immunopathologic characteristics. The incidence of this disease, its primary diseases, clinical characteristics and serum antineutrophil cytoplasmic antibodies (ANCAs) were analyzed.The distribution of patients among the three classifications was 8.7% type I, 68.6% type II and 22.7% type III. Clinically, the majority of patients (69.8%) presented rapidly progressive glomerulonephritis (RPGN), but 30.2% manifested a chronic nephritic syndrome or chronic renal failure. In terms of related conditions, 93% were anemic, 61.6% had hypertension, 50.6% oliguria, 45.3% nephrotic syndrome, 43% uremic syndrome and 39.5% displayed gross hematuria. Those patients who were positive in serum for ANCAs had predominantly type III DCGN. Two cases with anti-GBM-antibody crescentic glomerulonephritis and three with lupus nephritis were also positive for ANCAs in serum.DCGN is not rare in Chinese patients. A majority of patients in our study presented with RPGN, but 30.2% manifested a chronic renal failure. Lupus patients with DCGN that were positive for ANCAs had more severe vasculitic lesions.

Published

2003

22. Pathological demography of native patients in a nephrology center in China

Author

Huiping, Chen, Zheng, Tang, Caihong, Zeng, Weixin, Hu, Qingwen, Wang, Yushen, Yu, Xiaodan, Yao, Jianping, Wang, Maoyan, Zhu, Hong, Zhou, Hong, Liu, Zhihong, Liu, and Leishi, Li

Subjects

Adult, Male, Adolescent, Japan, Child, Preschool, Prevalence, Humans, Infant, Female, Kidney Diseases, Middle Aged, Child, Aged

Abstract

To analysis the pathological demography in Chinese patients undergoing renal biopsy from our nephrology center.Between January 1979 and October 2000 in Jinling Hospital, Nanjing, China, 10,002 attempts of percutaneous renal were performed in patients with renal disease from 33 provinces of China. The pathological classifications were made according to the WHO criteria of 1982 for renal pathology or the modified WHO criteria of 1995 by a panel of pathologists and nephrologists during routine clinical-pathological rounds. The pathological demography between those specimens collected from 1979 - 1989 and those from 1990 - 1999 was compared.The mean age of the 10,002 subjects undergoing renal biopsy was 31.4 +/- 13.0 years (ranging from 1 to 78 years), with a male to female ratio of 1.3:1; for the 592 renal transplant recipients, the mean age was 37.5 +/- 9.1 years (ranging from 16 to 66 years), with a male to female ratio of 2.36:1. Primary glomerular diseases (PGD) accounted for 71% of the total patients undergoing renal biopsies, secondary glomerular nephritis (SGN) 23%, tubular-interstitial diseases 3.2%, unclassified renal diseases 1.3%, hereditary and congenital renal diseases 1.0%, end stage renal diseases 0.96%, and recently realized or rare renal diseases 0.15%. IgA nephropathy (IgAN) was the most frequent pathological pattern (40%) of PGD, followed by mesangial proliferative lesion (MsPL) (30%), membranous nephropathy (MN) (10%), and focal segmental glomerulosclerosis (FSGS) (6%). Lupus nephritis (LN) was the most pathology common seen (74%) in SGN. During the 22 years of the study period, there was a steady increase in patients with SGN discovered during pathological evaluation of renal disorders. A rise in prevalence was found in IgA nephropathy, MN (both P0.001), crescentic glomerulonephritis (P0.0001), anti-GBM disease, and hemolytic-uremic syndrome/thrombotic thrombocytopenic purpura related renal damages (both P0.001). There was a decrease in endocapillary proliferative glomerulonephritis (P0.001) and IgM nephropathy (IgMN) (P0.01) from 1990 - 1999 as compared to 1979 - 1989. Infrequent renal pathological entities were also diagnosed in this group, including Niemann Pick disease, Fabry's disease, POEMS syndrome, and lipoprotein glomerulonephropathy.This is the largest series of renal biopsy data in China, and therefore may reflect the demographic picture of renal diseases in this country. Changes in prevalence of renal pathological entities were reflected in this group of patients over the last 22 years. In primary glomerular diseases, IgA nephropathy is still the most frequently observed pathological pattern. In SGN, LN appeared the most often. Increased prevalence was found in anti-GBM nephritis and HUS/TTP.

Published

2003

23. Challenge in pathologic diagnosis of Alport syndrome: evidence from correction of previous misdiagnosis

Author

Xin Chen, Huiping Chen, Caihong Zeng, Weixin Hu, Shutian Xu, Daxi Ji, Zheng Tang, Yang-lin Hu, Zhihong Liu, Yan-ting Yu, Qingwen Wang, Gao-yuan Huang, and Xiaodan Yao

Subjects

Male, medicine.medical_specialty, Adolescent, lcsh:Medicine, Nephritis, Hereditary, Young Adult, Immunohistology, Glomerulonephritis, Internal medicine, Diagnosis, medicine, Humans, Genetics(clinical), Pharmacology (medical), Alport syndrome, Young adult, Genetics (clinical), Medicine(all), medicine.diagnostic_test, Glomerulosclerosis, Focal Segmental, business.industry, Research, lcsh:R, Case-control study, Glomerulosclerosis, General Medicine, medicine.disease, Dermatology, Endocrinology, Case-Control Studies, Mesangial proliferative glomerulonephritis, Female, Renal biopsy, business, Nephritis

Abstract

Background Pathologic studies play an important role in evaluating patients with Alport syndrome besides genotyping. Difficulties still exist in diagnosing Alport syndrome (AS), and misdiagnosis is a not-so-rare event, even in adult patient evaluated with renal biopsy. Methods We used nested case–control study to investigate 52 patients previously misdiagnosed and 52 patients initially diagnosed in the China Alport Syndrome Treatments and Outcomes Registry e-system. Results We found mesangial proliferative glomerulonephritis (MsPGN, 26.9%) and focal and segmental glomerulosclerosis (FSGS, 19.2%) were the most common misdiagnosis. FSGS was the most frequent misdiagnosis in female X-linked AS (fXLAS) patients (34.8%), and MsPGN in male X-linked AS (mXLAS) patients (41.2%). Previous misdiagnosed mXLAS patients (13/17, 76.5%) and autosomal recessive AS (ARAS) patients (8/12, 66.7%) were corrected after a second renal biopsy. While misdiagnosed fXLAS patients (18/23, 78.3%) were corrected after a family member diagnosed (34.8%) or after rechecking electronic microscopy and/or collagen-IV alpha-chains immunofluresence study (COL-IF) (43.5%) during follow-up. With COL-IF as an additional criterion for AS diagnosis, we found that patients with less than 3 criteria reached have increased risk of misdiagnosis (3.29-fold for all misdiagnosed AS patients and 3.90-fold for fXLAS patients). Conclusion We emphasize timely and careful study of electronic microscopy and COL-IF in pathologic evaluation of AS patients. With renal and/or skin COL-IF as additional criterion, 3 diagnosis criteria reached are the cutoff for diagnosing AS pathologically.

Published

2012