2015
DOI: 10.1128/mcb.00143-15
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Loss of ADAM17-Mediated Tumor Necrosis Factor Alpha Signaling in Intestinal Cells Attenuates Mucosal Atrophy in a Mouse Model of Parenteral Nutrition

Abstract: e Total parenteral nutrition (TPN) is commonly used clinically to sustain patients; however, TPN is associated with profound mucosal atrophy, which may adversely affect clinical outcomes. Using a mouse TPN model, removing enteral nutrition leads to decreased crypt proliferation, increased intestinal epithelial cell (IEC) apoptosis and increased mucosal tumor necrosis factor alpha (TNF-␣) expression that ultimately produces mucosal atrophy. Upregulation of TNF-␣ signaling plays a central role in mediating TPN-i… Show more

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Cited by 22 publications
(34 citation statements)
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References 65 publications
(113 reference statements)
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“…It is likely that the increased proinflammatory expression of TNF-␣ may have prevented the TPN-associated increase in IEC apoptosis, since this is very tightly linked to the TPN-associated IEC apoptosis (14). We have previously shown a critical link to this proinflammatory response and a loss of EBF (15,16). Thus, it is quite possible that the persistent loss of EBF in the refeeding group was due to the increase in the expression of this proinflammatory response.…”
Section: Discussionmentioning
confidence: 97%
“…It is likely that the increased proinflammatory expression of TNF-␣ may have prevented the TPN-associated increase in IEC apoptosis, since this is very tightly linked to the TPN-associated IEC apoptosis (14). We have previously shown a critical link to this proinflammatory response and a loss of EBF (15,16). Thus, it is quite possible that the persistent loss of EBF in the refeeding group was due to the increase in the expression of this proinflammatory response.…”
Section: Discussionmentioning
confidence: 97%
“…These results also highlight that no other ADAM can compensate for ADAM10 loss required for Notch signaling in development and normal adult crypt homeostasis [56]. For example, no Notch phenotype is observed in the ADAM17-deficient intestine[71]. …”
Section: Adam10 and Intestinal Homeostasismentioning
confidence: 94%
“…While activating mutations of the NOTCH-1 NRR that result in ligand-independent proteolysis are found frequently in human leukemia, illustrating the importance for tight control of metalloprotease access to the S2 site[70], it is currently unclear whether such ligand-independent Notch activation plays a role in mammalian development and normal tissue homeostasis. Indeed, as will be discussed later, the ADAM17-deficient intestine has no overt intestinal phenotype under normal physiological conditions[71]. …”
Section: Adam10 and Intestinal Homeostasismentioning
confidence: 99%
“…A slight increase in proinflammatory cytokine expression has been observed in the colonic mucosa of Adam17 ex/ex mice, which suggests sensitization to inflammatory stimuli (79, 80). Similarly, IEC-Adam17 KO mice on a C57BL/6J background do not have an intestinal phenotype (81, 82) (Table 2). No defects in the development and number of Peyer’s patches, in small intestinal barrier function, or in cytokine gene signatures have been observed (81, 82).…”
Section: Adams and The Gastrointestinal Tractmentioning
confidence: 96%
“…Similarly, IEC-Adam17 KO mice on a C57BL/6J background do not have an intestinal phenotype (81, 82) (Table 2). No defects in the development and number of Peyer’s patches, in small intestinal barrier function, or in cytokine gene signatures have been observed (81, 82). The normal intestinal secretory differentiation in hypomorphic Adam17 mice and IEC-Adam17 KO mice indicates that ADAM17 is not required for Notch signaling in the crypt compartment (50).…”
Section: Adams and The Gastrointestinal Tractmentioning
confidence: 96%