The Inflammatory Feed-Forward Loop Triggered by the Complement Component C3 as a Potential Target in Endometriosis

Agostinis, Chiara; Zorzet, Sonia; Balduit, Andrea; Zito, Gabriella; Mangogna, Alessandro; Macor, Paolo; Romano, Federico; Toffoli, Miriam; Belmonte, Beatrice; Morello, Gaia; Martorana, Annamaria; Borelli, Violetta; Ricci, Giuseppe; Kishore, Uday; Bulla, Roberta

doi:10.3389/fimmu.2021.693118

Cited by 12 publications

(12 citation statements)

References 61 publications

(79 reference statements)

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“…Previous studies have shown that the TLR4-C3 axis can regulate intestinal immune responses during chronic colitis ( 41 ). Research byAgostinis C identified the inflammatory feed-foward loop triggered by complement component C3 may serve as a potential therapeutic target for endometriosis ( 42 ). Rijcken E et al.…”

Section: Discussionmentioning

confidence: 99%

Potential shared pathogenic mechanisms between endometriosis and inflammatory bowel disease indicate a strong initial effect of immune factors

Zhang,

Mo,

Wang

et al. 2024

Front. Immunol.

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IntroductionOver the past decades, immune dysregulation has been consistently demonstrated being common charactoristics of endometriosis (EM) and Inflammatory Bowel Disease (IBD) in numerous studies. However, the underlying pathological mechanisms remain unknown. In this study, bioinformatics techniques were used to screen large-scale gene expression data for plausible correlations at the molecular level in order to identify common pathogenic pathways between EM and IBD.MethodsBased on the EM transcriptomic datasets GSE7305 and GSE23339, as well as the IBD transcriptomic datasets GSE87466 and GSE126124, differential gene analysis was performed using the limma package in the R environment. Co-expressed differentially expressed genes were identified, and a protein-protein interaction (PPI) network for the differentially expressed genes was constructed using the 11.5 version of the STRING database. The MCODE tool in Cytoscape facilitated filtering out protein interaction subnetworks. Key genes in the PPI network were identified through two topological analysis algorithms (MCC and Degree) from the CytoHubba plugin. Upset was used for visualization of these key genes. The diagnostic value of gene expression levels for these key genes was assessed using the Receiver Operating Characteristic (ROC) curve and Area Under the Curve (AUC) The CIBERSORT algorithm determined the infiltration status of 22 immune cell subtypes, exploring differences between EM and IBD patients in both control and disease groups. Finally, different gene expression trends shared by EM and IBD were input into CMap to identify small molecule compounds with potential therapeutic effects.Results113 differentially expressed genes (DEGs) that were co-expressed in EM and IBD have been identified, comprising 28 down-regulated genes and 86 up-regulated genes. The co-expression differential gene of EM and IBD in the functional enrichment analyses focused on immune response activation, circulating immunoglobulin-mediated humoral immune response and humoral immune response. Five hub genes (SERPING1、VCAM1、CLU、C3、CD55) were identified through the Protein-protein Interaction network and MCODE.High Area Under the Curve (AUC) values of Receiver Operating Characteristic (ROC) curves for 5hub genes indicate the predictive ability for disease occurrence.These hub genes could be used as potential biomarkers for the development of EM and IBD. Furthermore, the CMap database identified a total of 9 small molecule compounds (TTNPB、CAY-10577、PD-0325901 etc.) targeting therapeutic genes for EM and IBD.DiscussionOur research revealed common pathogenic mechanisms between EM and IBD, particularly emphasizing immune regulation and cell signalling, indicating the significance of immune factors in the occurence and progression of both diseases. By elucidating shared mechanisms, our study provides novel avenues for the prevention and treatment of EM and IBD.

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Section: Discussionmentioning

confidence: 99%

Potential shared pathogenic mechanisms between endometriosis and inflammatory bowel disease indicate a strong initial effect of immune factors

Zhang,

Mo,

Wang

et al. 2024

Front. Immunol.

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“…ROC analysis revealed that four IRGs can be used as potential biomarkers of endometriosis, which also demonstrated the feasibility in terms of the AUC, a signal for endometriosis occurrence. Recently, C3 was considered a candidate diagnostic biomarker of endometrosis, and its expression was correlated with the engraftment of the endometriotic cysts [ 45 ]. The overexpression of VCAM-1 on the peritoneum of endometriosis had been revealed by Schutt et al [ 46 ].…”

Section: Discussionmentioning

confidence: 99%

“…The TF-IRG network could be used to present novel prospective molecular mechanisms underlying the development of tumors [ 45 ]. However, studies of the regulatory mechanisms underlying TFs and IRGs in endometriosis are still in progress.…”

Section: Discussionmentioning

confidence: 99%

Identification and Analysis of Potential Immune-Related Biomarkers in Endometriosis

et al. 2023

Journal of Immunology Research

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Background. Endometriosis is an inflammatory gynecological disease leading to deep pelvic pain, dyspareunia, and infertility. The pathophysiology of endometriosis is complex and depends on a variety of biological processes and pathways. Therefore, there is an urgent need to identify reliable biomarkers for early detection and accurate diagnosis to predict clinical outcomes and aid in the early intervention of endometriosis. We screened transcription factor- (TF-) immune-related gene (IRG) regulatory networks as potential biomarkers to reveal new molecular subgroups for the early diagnosis of endometriosis. Methods. To explore potential therapeutic targets for endometriosis, the Gene Expression Omnibus (GEO), Immunology Database and Analysis Portal (ImmPort), and TF databases were used to obtain data related to the recognition of differentially expressed genes (DEGs), differentially expressed IRGs (DEIRGs), and differentially expressed TFs (DETFs). Gene Ontology (GO) and Kyoto Encyclopedia of Genes and Genomes (KEGG) pathway enrichment analyses were performed on the DETFs and DEIRGs. Then, DETFs and DEIRGs were further validated in the external datasets of GSE51981 and GSE1230103. Then, we used quantitative real-time polymerase chain reaction (qRT-PCR) to verify the hub genes. Simultaneously, the Pearson correlation analysis and protein-protein interaction (PPI) analyses were used to indicate the potential mechanisms of TF-IRGs at the molecular level and obtain hub IRGs. Finally, the receiver operating characteristic (ROC) curve analysis was used to assess the diagnostic value of the hub IRGs. Results. We screened a total of 94 DETFs and 121 DEIRGs in endometriosis. Most downregulated DETFs showed decreased expression in the endometria of moderate/severe endometriosis patients. The top-ranked upregulated DEIRGs were upregulated in the endometra of infertile women. Functional analysis showed that DETFs and DEIRGs may be involved in the biological behaviors and pathways of endometriosis. The TF-IRG PPI network was successfully constructed. Compared with the control group, high C3, VCAM1, ITGB2, and C3AR1 expression had statistical significance in endometriosis among the hub DEIRGs. They also showed higher sensitivity and specificity by ROC analysis for the diagnosis of endometriosis. Finally, compared with controls, C3 and VCAM1 were highly expressed in endometriosis tissue samples. In addition, they also showed high specificity and sensitivity for diagnosing endometriosis. Conclusion. Overall, we discovered the TF-IRG regulatory network and analyzed 4 hub IRGs that were closely related to endometriosis, which contributes to the diagnosis of endometriosis. Additionally, we verified that DETFs or DEIRGs were associated with the clinicopathological features of endometriosis, and external datasets also confirmed the hub IRGs. Finally, C3 and VCAM1 were highly expressed in endometriosis tissue samples compared with controls and may be potential biomarkers of endometriosis, which are helpful for the early diagnosis of endometriosis.

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“…The key step for activating the complement system by recognizing non self-molecules is to activate the central C3 component through the classical pathway (antibody mediated), lectin pathway or alternative pathway ( 91 ). C3 is also present in the epithelial cells of the endometrium ( 92 ). Activation of C3 on the cell surface can stimulate the formation of membrane attack complexes on NEUs and target cells, resulting in cell damage and cell lysis, but other host cells are protected by membrane binding regulatory molecules such as CD46, CD55 and CD59 ( 93 ).…”

Section: Reciprocal Interactions Between Immunity Endometrium and Mic...mentioning

confidence: 99%

“Iron triangle” of regulating the uterine microecology: Endometrial microbiota, immunity and endometrium

Zhu

Yang

et al. 2022

Front. Immunol.

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The uterus is the core place for breeding new life. The balance and imbalance of uterine microecology can directly affect or even dominate the female reproductive health. Emerging data demonstrate that endometrial microbiota, endometrium and immunity play an irreplaceable role in regulating uterine microecology, forming a dynamic iron triangle relationship. Up to nowadays, it remains unclear how the three factors affect and interact with each other, which is also a frontier topic in the emerging field of reproductive tract microecology. From this new perspective, we aim to clarify the relationship and mechanism of the interaction of these three factors, especially their pairwise interactions. Finally, the limitations and future perspectives of the current studies are summarized. In general, these three factors have a dynamic relationship of mutual dependence, promotion and restriction under the physiological or pathological conditions of uterus, among which the regulatory mechanism of microbiota and immunity plays a role of bridge. These findings can provide new insights and measures for the regulation of uterine microecology, the prevention and treatment of endometrial diseases, and the further multi-disciplinary integration between microbiology, immunology and reproductive medicine.

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The Inflammatory Feed-Forward Loop Triggered by the Complement Component C3 as a Potential Target in Endometriosis

Cited by 12 publications

References 61 publications

Potential shared pathogenic mechanisms between endometriosis and inflammatory bowel disease indicate a strong initial effect of immune factors

Potential shared pathogenic mechanisms between endometriosis and inflammatory bowel disease indicate a strong initial effect of immune factors

Identification and Analysis of Potential Immune-Related Biomarkers in Endometriosis

“Iron triangle” of regulating the uterine microecology: Endometrial microbiota, immunity and endometrium

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