A substance P (neurokinin-1) receptor mutant carboxyl-terminally truncated to resemble a naturally occurring receptor  isoform displays enhanced responsiveness and  resistance to desensitization

102

Section: Discussioncontrasting

confidence: 57%

Section: Discussionmentioning

confidence: 99%

mentioning

confidence: 99%

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Full-length and truncated neurokinin-1 receptor expression and function during monocyte/macrophage differentiation

Lai

Kilpatrick

et al. 2006

102

“…In addition, Lai et al (26) showed that upon ligand binding, tr-NK-1R, which lacks a C-terminal tail that binds and activates G q , cannot initiate calcium influx or activate PKC and NF-κB; however, the truncated receptor can activate ERK in a delayed manner. The tr-NK-1R has also been reported to be resistant to desensitization (27,28). Not only does the truncated receptor lack C-terminal residues that are important for desensitization, it is also incapable of activating PKC (26), a critical component of the feedback inhibition loop that causes desensitization of the full-length receptor (28).…”

Section: Discussionmentioning

confidence: 99%

Truncated neurokinin-1 receptor is increased in colonic epithelial cells from patients with colitis-associated cancer

Gillespie¹,

Leeman²,

Watts³

et al. 2011

Self Cite

Patients with chronic ulcerative colitis (UC) are at high risk for developing colorectal cancer. In this study, archival formalin-fixed paraffin-embedded colonic tissue from patients with UC who developed carcinoma (CA) or high-grade dysplasia (HGD) was examined for changes in expression of the proinflammatory and mitogenic neurokinin-1 receptor (NK-1R). Laser capture microscopy was used to microdissect epithelia from areas of colons that showed histologic evidence of CA, HGD, and epithelia that were not dysplastic or cancerous but did contain evidence of prior inflammation (quiescent colitis). mRNA was extracted from the dissected tissue, and PCR array analysis was performed on extracted mRNA. Two antibodies were necessary to separately estimate the protein levels of the truncated (tr-NK-1R) and full-length (fl-NK-1R) receptors by immunohistochemistry. mRNA expression of tr-NK-1R increased 14-fold (P = 0.02) when comparing the HGD and CA groups. In contrast, the fl-NK-1R transcript showed no significant differences among groups. The protein levels of the total NK-1R increased by 40% (P = 0.02) in HGD and 80% (P = 0.0007) in CA compared with quiescent colitis. There were no significant changes in protein levels of the fl-NK-1R. We conclude that the increase in total NK-1R protein in HGD and CA is attributable to an increase in tr-NK-1R, suggesting there may be a functional role for tr-NK-1R in malignant transformation in colitis-associated cancer. The tr-NK-1R could prove useful as a diagnostic marker to identify patients at risk for neoplasia and may serve as a useful therapeutic target in the treatment of colitisassociated cancer.colon cancer | receptor splice variants | substance P | IBD C hronic inflammation is associated with a higher rate of cancer development in various organs (1). More specifically, patients with ulcerative colitis (UC) are at high risk for developing colorectal cancer (2); both extent and duration of intestinal inflammation further increase risk (3, 4). These associations suggest that chronic intestinal inflammation is a causative factor in carcinogenesis in patients with UC, and that there is a causal link between chronic inflammation and increased risk of cancer. These observations raise the question of the signaling pathways by which long-standing inflammation might underlie the development of cancer.Substance P (SP) is a proinflammatory neuropeptide described by von Euler and Gaddum (5) and later isolated and characterized by Chang and Leeman (6). SP is synthesized by a variety of cells, most notably neurons and inflammatory cells such as macrophages (7). SP's primary receptor, the neurokinin-1 receptor (NK-1R), can mediate a variety of physiologic and pathophysiologic responses, including cell proliferation, migration, and inflammation (8). The NK-1R has been identified in epithelial cells in rodent models of colonic inflammation (9, 10) and in patients with UC as well as Crohn disease (11)(12)(13)(14). However, not all of these studies are in agreement regarding epithelial NK-1R e...

“…A naturally occurring truncated variant of the NK1R (NK1R␦325) exhibits impaired SP-induced desensitization and endocytosis, possibly because of an inability to interact with ␤-arrestin (11,12). Therefore, we also compared the ability of wild type and truncated NK1R to activate ERK1͞2.…”

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confidence: 99%

The proliferative and antiapoptotic effects of substance P are facilitated by formation of a β-arrestin-dependent scaffolding complex

DeFea

Vaughn

O'Bryan

et al. 2000

368

338

A requirement for scaffolding complexes containing internalized G protein-coupled receptors and ␤-arrestins in the activation and subcellular localization of extracellular signal-regulated kinases 1 and 2 (ERK1͞2) has recently been proposed. However, the composition of these complexes and the importance of this requirement for function of ERK1͞2 appear to differ between receptors. Here we report that substance P (SP) activation of neurokinin-1 receptor (NK1R) stimulates the formation of a scaffolding complex comprising internalized receptor, ␤-arrestin, src, and ERK1͞2 (detected by gel filtration, immunoprecipitation, and immunofluorescence). Inhibition of complex formation, by expression of dominant-negative ␤-arrestin or a truncated NK1R that fails to interact with ␤-arrestin, inhibits both SP-stimulated endocytosis of the NK1R and activation of ERK1͞2, which is required for the proliferative and antiapoptotic effects of SP. Thus, formation of a ␤-arrestin-containing complex facilitates the proliferative and antiapoptotic effects of SP, and these effects of SP could be diminished in cells expressing truncated NK1R corresponding to a naturally occurring variant.