Esophageal Cancer Related Gene-4 Is a Choroid Plexus-Derived Injury Response Gene: Evidence for a Biphasic Response in Early and Late Brain Injury

Podvin, Sonia; González, Ana-Maria; Miller, Miles C.; Dang, Xitong; Botfield, Hannah; Donahue, John E.; Kurabi, Arwa; Boissaud-Cooke, Matthew; Rossi, Ryan; Leadbeater, Wendy; Johanson, Conrad E.; Coimbra, Raúl; Stopa, Edward G.; Eliceiri, Brian P.; Baird, Andrew

doi:10.1371/journal.pone.0024609

Cited by 41 publications

(78 citation statements)

References 36 publications

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“…Likewise, we performed qRT-PCR and demonstrated elevated ECRG4 lung expression (lane 1) in comparison to heart (lane 2) and skin (lane 3) (Figure 1B). Immunoblotting of mouse lung with the anti-ECRG4 antibody [27, 46] revealed the presence of a single 14 kDa peptide that corresponded to the molecular weight of the predicted precursor product, amino acids 31–148, of ECRG4 (Figure 1C). …”

Section: Resultsmentioning

confidence: 99%

“…Several recent studies suggest that ECRG4 plays a role in injury homeostasis because its downregulation after injury/inflammation allows for dysinhibition of cell proliferation in vivo [27, 29, 46, 50, 51]. Its epigenetic regulation, however, suggests that the return of basal gene expression after injury could depend on epigenetic factors determined by environment, diet, and age.…”

Section: Introductionmentioning

confidence: 99%

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Pulmonary preconditioning, injury, and inflammation modulate expression of the candidate tumor suppressor geneECRG4in lung

Kao

Shaterian

Cauvi

et al. 2014

Experimental Lung Research

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Purpose The human c2orf40 gene encodes a candidate tumor suppressor called Esophageal Cancer-Related Gene-4 (ECRG4) that is a cytokine-like epigenetically-regulated protein that is characteristically downregulated in cancer, injury, inflammation, and infection. Here, we asked whether ECRG4 gene expression is detectable in lung epithelial cells and if its expression changes with inflammation, infection, and/or protective preconditioning. Materials and Methods We used immunoblotting, PCR, and quantitative PCR to measure ECRG4 and either inhalation anesthesia preconditioning, lipopolysaccharide injection, or laparotomy to modulate lung inflammation. Results Immunoblotting establishes the presence of the full-length 14 kDa ECRG4 peptide in mouse lung. Immunohistochemistry localizes ECRG4 to type l alveolar epithelial cells. Basal ECRG4 mRNA is greater than TNF-α, IL-1β, and IL-6 but following inflammatory lung injury, TNF-α, IL-1β, IL-6, and IL-10 are upregulated while ECRG4 gene expression is decreased. Similar findings are observed after an intravenous administration of lipopolysaccharide. In contrast, lung preconditioning with isoflurane anesthesia increases lung ECRG4 gene expression. Over-expression of ECRG4 in human lung epithelial cells in vitro decreases cell proliferation implying that a loss of ECRG4 in vivo would be permissive to cell growth. Conclusions This study supports the hypothesis that ECRG4 acts as a sentinel growth inhibitor in lung alveolar epithelial cells. Its downregulation by injury, infection, and inflammation and upregulation by preconditioning supports a role for ECRG4 in regulating the alveolar epithelium response to injury and inflammation. By extension, the findings support a functional consequence to its inhibition by promoter hypermethylation (i.e. lung cancer) and suggest potential benefits to its upregulation.

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Section: Resultsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Pulmonary preconditioning, injury, and inflammation modulate expression of the candidate tumor suppressor geneECRG4in lung

Kao

Shaterian

Cauvi

et al. 2014

Experimental Lung Research

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“…The C2ORF40 gene is important in processes associated with physiological functional regulation, including inflammation, injury, senescence, the neuroendocrines environment, differentiation and apoptosis (5)(6)(7)(8)(9)(10)(11)(12)(13). Notably, previous studies have indicated that C2ORF40 is a candidate tumor suppressor gene associated with prognosis in a variety of tumors (4,(14)(15)(16)(17)(18)(19)(20)(21)(22).…”

Section: Introductionmentioning

confidence: 99%

Soluble purified recombinant C2ORF40 protein inhibits tumor cell growth in vivo by decreasing telomerase activity in esophageal squamous cell carcinoma

Wang

et al. 2016

Oncology Letters

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Abstract.The chromosome 2 open reading frame 40 (C2ORF40) gene is a candidate tumor suppressor gene for a variety of tumors. Previous results by the present authors revealed that the C2ORF40 protein is a secreted protein.However, the exact biological function of secreted C2ORF40 protein in carcinogenesis has not been thoroughly investigated. In the present study, the signal peptide sequence of the C2ORF40 cDNA was initially removed to produce secreted recombinant human C2ORF40 protein (rhC2ORF40). Soluble rhC2ORF40 was successfully expressed and purified, which was evaluated for the first time, to the best of our knowledge, for tumor-suppressing function in vivo in esophageal cancer. The present results revealed that soluble purified rhC2ORF40 was concentrated with a purity of >95%. Furthermore, rhC2ORF40 inhibited esophageal cancer cell growth in vivo in a dose-dependent manner compared with a control group (P<0.05). In addition, the present study demonstrated for the first time that rhC2ORF40 decreased telomerase activity using telomeric repeat amplification protocol-enzyme-linked immunosorbent assay (P<0.05), without affecting the expression levels of telomerase-component RNA (P>0.05), as shown with polymerase chain reaction. Overall, the present results demonstrated that soluble rhC2ORF40 inhibited tumor cell growth in vivo by decreasing telomerase activity in esophageal squamous cell carcinoma. Therefore, soluble rhC2ORF40 with a high purity and biological activity may be a potential biological therapy drug for esophageal cancer.

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“…We have focused on the potential for esophageal cancer related gene-4 (ECRG4) to serve as a sentinel factor on immune cells that may regulate the immune set point based on its expression on the surface of leukocytes, its release from the cell surface after inflammatory stimuli, and its epigenetic regulation that may explain differences in Ecrg4 expression between individuals [6][7][8][9]. Esophageal cancer related gene-4 encodes a 148 amino acid precursor protein that is tethered to the cell surface but shed on activation [6,10].…”

mentioning

confidence: 99%

“…Esophageal cancer related gene-4 encodes a 148 amino acid precursor protein that is tethered to the cell surface but shed on activation [6,10]. We have demonstrated previously that ECRG4 is present on the surface of polymorphonuclear leukocytes (PMNs) and, on ex vivo activation by agonists such as lipopolysaccharide (LPS), ECRG4 is released and can be detected by immunoblotting and proteomic analyses of biologic fluids including conditioned media, cerebrospinal fluid, and serum [6,7,[10][11][12]. We have also demonstrated that ECRG4 interacts with the human innate immunity receptor complex (TLR4-CD14-MD2) supporting further an important role in responding to inflammatory insults such as severe injury [13].…”

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confidence: 99%

Monitoring Neutrophil-Expressed Cell Surface Esophageal Cancer Related Gene-4 after Severe Burn Injury

Costantini

Coimbra

Lopez

et al. 2015

Surgical Infections

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Background: We identified recently esophageal cancer related gene-4 (ECRG4) as a candidate cytokine that is expressed on the surface of quiescent polymorphonuclear leukocytes (PMNs) and shed in response to ex vivo treatment with lipopolysaccharide. To investigate the potential biologic relevance of changes in cell surface ECRG4 in human samples, we performed a pilot study to examine a population of burn patients in whom blood could be analyzed prospectively. We hypothesized that cutaneous burn injury would alter cell surface expression of ECRG4 on PMNs. Methods: Patients admitted with more than 20% total burn surface area (TBSA) (n = 10) had blood collected at the time of admission and weekly thereafter. For comparison, blood was obtained from a control group of healthy human volunteers (n = 4). We used flow cytometry to measure changes in ECRG4 + PMNs from patients during recovery from injury. Esophageal cancer related gene-4 expression at each time point was compared with the patient's clinical status based on a Multiple Organ Dysfunction (MOD) score. Results: Esophageal cancer related gene-4 was detected on the PMN surface of cells collected from healthy volunteers, however, within 48 h of admission after burn injury (n = 10 patients), the number of PMNs with cell surface ECRG4 was decreased. Esophageal cancer related gene-4 expression in PMNs was re-established over the course of patient recovery, unless complications occurred. In this case, the decrease in cell surface ECRG4 + PMNs preceded the clinical diagnosis of infectious complications and was reflected by increased organ injury scores. Conclusion: From a small sample set, we were able to determine that PMN cell surface ECRG4 expression was decreased after burn injury and returned to baseline during recovery from injury. Although larger studies are needed to define the role of ECRG4 in human PMNs further, this report is the first assessment of cell surface ECRG4 protein in a patient population to support analogous findings in animal studies.

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Esophageal Cancer Related Gene-4 Is a Choroid Plexus-Derived Injury Response Gene: Evidence for a Biphasic Response in Early and Late Brain Injury

Cited by 41 publications

References 36 publications

Pulmonary preconditioning, injury, and inflammation modulate expression of the candidate tumor suppressor geneECRG4in lung

Pulmonary preconditioning, injury, and inflammation modulate expression of the candidate tumor suppressor geneECRG4in lung

Soluble purified recombinant C2ORF40 protein inhibits tumor cell growth in vivo by decreasing telomerase activity in esophageal squamous cell carcinoma

Monitoring Neutrophil-Expressed Cell Surface Esophageal Cancer Related Gene-4 after Severe Burn Injury

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