Elucidating the fundamental fibrotic processes driving abdominal adhesion formation

Foster, Deshka S.; Marshall, Clement D.; Gulati, Gunsagar S.; Chinta, Malini; Nguyen, Alan; Salhotra, Ankit; Jones, Ruth Ellen; Burcham, Austin; Lerbs, Tristan; Cui, Lü; King, Megan E.; Titan, Ashley L.; Ransom, Ryan C.; Manjunath, Anoop; Hu, Michael S.; Blackshear, Charles P.; Mascharak, Shamik; Moore, Alessandra L.; Norton, Jeffrey A.; Kin, Cindy; Shelton, Andrew; Januszyk, Michael; Gurtner, Geoffrey C.; Wernig, Gerlinde; Longaker, Michael T.

doi:10.1038/s41467-020-17883-1

Cited by 55 publications

(41 citation statements)

References 51 publications

(50 reference statements)

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“…Human gene PDGFRA encodes platelet-derived growth factor receptor α, both a deficit and excess of which worsen reproductive potential through skeletal defects in newborns [ 75 ] and predisposition to infertility after infections [ 76 ] ( Table 4 ).…”

Section: Resultsmentioning

confidence: 99%

A Bioinformatics Model of Human Diseases on the Basis of Differentially Expressed Genes (of Domestic Versus Wild Animals) That Are Orthologs of Human Genes Associated with Reproductive-Potential Changes

Vasiliev

Chadaeva

Рассказов

et al. 2021

IJMS

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Earlier, after our bioinformatic analysis of single-nucleotide polymorphisms of TATA-binding protein-binding sites within gene promoters on the human Y chromosome, we suggested that human reproductive potential diminishes during self-domestication. Here, we implemented bioinformatics models of human diseases using animal in vivo genome-wide RNA-Seq data to compare the effect of co-directed changes in the expression of orthologous genes on human reproductive potential and during the divergence of domestic and wild animals from their nearest common ancestor (NCA). For example, serotonin receptor 3A (HTR3A) deficiency contributes to sudden death in pregnancy, consistently with Htr3a underexpression in guinea pigs (Cavia porcellus) during their divergence from their NCA with cavy (C. aperea). Overall, 25 and three differentially expressed genes (hereinafter, DEGs) in domestic animals versus 11 and 17 DEGs in wild animals show the direction consistent with human orthologous gene-markers of reduced and increased reproductive potential. This indicates a reliable association between DEGs in domestic animals and human orthologous genes reducing reproductive potential (Pearson’s χ2 test p < 0.001, Fisher’s exact test p < 0.05, binomial distribution p < 0.0001), whereas DEGs in wild animals uniformly match human orthologous genes decreasing and increasing human reproductive potential (p > 0.1; binomial distribution), thus enforcing the norm (wild type).

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Section: Resultsmentioning

confidence: 99%

A Bioinformatics Model of Human Diseases on the Basis of Differentially Expressed Genes (of Domestic Versus Wild Animals) That Are Orthologs of Human Genes Associated with Reproductive-Potential Changes

Vasiliev

Chadaeva

Рассказов

et al. 2021

IJMS

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“…Mechanically, MSLN + MCs is the important subpopulation of MCs involved in the development of adhesion. Foster et al 41 recently found that JUN expression was strongly induced and correlated with prominent MSLN expression, and inhibition of JUN significantly minimizes adhesion formation.…”

Section: Cellular Mechanisms Of Pamentioning

confidence: 99%

A review of physiological and cellular mechanisms underlying fibrotic postoperative adhesion

Xia

Kang

et al. 2021

Int. J. Biol. Sci.

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Postoperative adhesions (PA) are fibrotic tissues that are the most common driver of long-term morbidity after abdominal and pelvic surgery. The optimal drug or material to prevent adhesion formation has not yet been discovered. Comprehensive understanding of cellular and molecular mechanisms of adhesion process stimulates the design of future anti-adhesive strategies. Recently, disruption of peritoneal mesothelial cells were suggested as the 'motor' of PA formation, followed by a cascade of events (coagulation, inflammation, fibrinolysis) and influx of various immune cells, ultimately leading to a fibrous exudate. We showed that a variety of immune cells were recruited into adhesive peritoneal tissues in patients with small bowel obstruction caused by PA. The interactions among various types of immune cells contribute to PA development following peritoneal trauma. Our review focuses on the specific role of different immune cells in cellular and humoral mechanisms underpinning adhesion development.

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“…Of importance, Foster et al analysed adhesions from patients and mouse models to elucidate the heterogeneity and source of fibrogenic cells. Fibroblasts within adhesions were found to express platelet derived growth factor receptor alpha (PDGFRA), a transmembrane receptor tyrosine kinase, as well as fibroblast markers, such as αSMA, vimentin, and collagen 1 (COL1) [ 92 ]. In murine ischaemic tissue-induced adhesions, fibroblasts expressed JUN (proto-oncogene, named after viral homolog v-jun in avian sarcoma virus 17), which is a transcriptional master regulator of fibrogenesis, and a portion of these cells were also positive for the mesothelial marker mesothelin (MSLN).…”

Section: Serosal Repair and Adhesion Formationmentioning

confidence: 99%

“…Analysis of these clusters in relation to their timepoints revealed that early JUN activation promoted a profibrotic state as reflected in the expression profiles. Moreover, inhibition of the highly expressed Jun/Jak/Stat pathway was found to reduce adhesion formation and was proposed as a novel preventative strategy [ 92 ].…”

Section: Serosal Repair and Adhesion Formationmentioning

confidence: 99%

“…Mesothelial cells have been proposed as another important source of fibrogenic cells that mediate adhesion formation through a process of MMT. Using human adhesion samples, Foster and colleagues demonstrated that a small portion of JUN+ fibroblasts also expressed the mesothelial marker MSLN and the EMT pathway was one of the most significantly upregulated molecular profiles in cultured adhesion fibroblasts [ 92 ]. Sandoval and colleagues also analysed human adhesions and showed co-localisation of the epithelial marker, cytokeratin and the mesenchymal marker, αSMA, in spindle-like cells in the subserosa strongly implicating that mesothelial cells had transitioned to become myofibroblasts [ 97 ], a feature commonly found in biopsy samples from peritoneal dialysis patients [ 54 ].…”

Section: Serosal Repair and Adhesion Formationmentioning

confidence: 99%

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Post-Surgical Peritoneal Scarring and Key Molecular Mechanisms

Herrick

Wilm

2021

Biomolecules

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Post-surgical adhesions are internal scar tissue and a major health and economic burden. Adhesions affect and involve the peritoneal lining of the abdominal cavity, which consists of a continuous mesothelial covering of the cavity wall and majority of internal organs. Our understanding of the full pathophysiology of adhesion formation is limited by the fact that the mechanisms regulating normal serosal repair and regeneration of the mesothelial layer are still being elucidated. Emerging evidence suggests that mesothelial cells do not simply form a passive barrier but perform a wide range of important regulatory functions including maintaining a healthy peritoneal homeostasis as well as orchestrating events leading to normal repair or pathological outcomes following injury. Here, we summarise recent advances in our understanding of serosal repair and adhesion formation with an emphasis on molecular mechanisms and novel gene expression signatures associated with these processes. We discuss changes in mesothelial biomolecular marker expression during peritoneal development, which may help, in part, to explain findings in adults from lineage tracing studies using experimental adhesion models. Lastly, we highlight examples of where local tissue specialisation may determine a particular response of peritoneal cells to injury.

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Elucidating the fundamental fibrotic processes driving abdominal adhesion formation

Cited by 55 publications

References 51 publications

A Bioinformatics Model of Human Diseases on the Basis of Differentially Expressed Genes (of Domestic Versus Wild Animals) That Are Orthologs of Human Genes Associated with Reproductive-Potential Changes

A Bioinformatics Model of Human Diseases on the Basis of Differentially Expressed Genes (of Domestic Versus Wild Animals) That Are Orthologs of Human Genes Associated with Reproductive-Potential Changes

A review of physiological and cellular mechanisms underlying fibrotic postoperative adhesion

Post-Surgical Peritoneal Scarring and Key Molecular Mechanisms

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