Rce1: mechanism and inhibition

Hampton, Shahienaz E.; Dore, Timothy M.; Schmidt, W.

doi:10.1080/10409238.2018.1431606

Cited by 41 publications

(34 citation statements)

References 117 publications

(193 reference statements)

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“…Manolaridis et al () and Hampton et al () have verified that Rce1 is an isoprenyl endopeptidase that localizes to the endoplasmic reticulum to remove the carboxyl‐terminal three amino acids via hydrolyzation of C15 or C20 isoprenylation of the cysteine in CAAX. Bergo et al () believe that suppression of Rce1 activity is associated with Ras mislocalization, diminished growth of Ras‐transformed fibroblasts in culture and in nude mice, and hypersensitivity to farnesyl and geranylgeranyl transferase inhibitors (FTIs).…”

Section: Discussionmentioning

confidence: 99%

Rce1 suppresses invasion and metastasis of hepatocellular carcinoma via epithelial‐mesenchymal transition induced by the TGF‐β1/H‐Ras signaling pathway

Yang

et al. 2019

Journal Cellular Physiology

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Ras converting enzyme 1 (Rce1) plays an important role in invasion and metastasis of malignancy. However, the mechanism has not yet been fully explored in hepatocellular carcinoma (HCC). Primarily, we investigated the expression of Rce1 and H-Ras influence on patient prognosis through the clinical data. Further, we analyzed the regulatory effects of Rce1/H-Ras signal pathway on the epithelial-mesenchymal transition (EMT) in vitro and in vivo. Finally, we screened out the protein which bonds with Rce1 by CO-IP experiment to discuss the mechanism of Rce1 in EMT of HCC. This research revealed a significantly decreased expression of Rce1 in HCC compared with noncancerous tissues (p < .05). In contrast, H-Ras expression was increased in the tumor. The expression of them was a close association with the differentiation and tumor-node-metastasis (TNM) stage of the tumor (p < .001; p = .035, respectively) and Rce1 was an independent prognostic indicator (95%Cl: 0.193-0.821; p = .013). Through targeted regulation of Rce1 by cDNA or small interfering RNA, results show that the lower expression of Rce1 facilitated EMT and promoted the invasion and metastasis of HCC (p < .05). Furthermore, the CO-IP experiment unfolded that Rce1 could bond with farnesyltransferase-β (FNTB) which mediated the expression of H-Ras. Conclusions: Rce1 inhibits EMT via target regulation H-Ras and suppress the early invasion and metastasis of HCC. It may be a potential therapeutic target and prognostic indicator for HCC. K E Y W O R D S epithelial-mesenchymal transition, hepatocellular carcinoma, invasion and metastasis, ras converting enzyme 1, signaling pathway

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Section: Discussionmentioning

confidence: 99%

Rce1 suppresses invasion and metastasis of hepatocellular carcinoma via epithelial‐mesenchymal transition induced by the TGF‐β1/H‐Ras signaling pathway

Yang

et al. 2019

Journal Cellular Physiology

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“…A specific RCE1 inhibitor would be required to determine whether targeting this enzyme pharmacologically could be useful in treating disorders of ZMPSTE24 deficiency—a strategy that would be relevant for MAD‐B and the extremely rare atypical form of HGPS, but not for RD as it is lethal at birth (Hampton, Dore, & Schmidt, 2018). However, such an inhibitor would not be required to completely inhibit RCE1 because 65% of reduced Rce1 expression was sufficient to double the median survival of Zmpste24 ‐deficient mice.…”

Section: Figurementioning

confidence: 99%

Targeting RAS‐converting enzyme 1 overcomes senescence and improves progeria‐like phenotypes of ZMPSTE24 deficiency

et al. 2020

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“…The AMR4 mutation identified in our screen (S347G) is near the active site of the gene’s only annotated domain, a CaaX protease and bacteriocin processing (CPBP) domain. Mutagenesis and structural studies of CPBP domains indicate a catalytic mechanism in which a conserved glutamate activates a nucleophilic water molecule for proteolysis ( 27 – 30 ). Mutation of this catalytic glutamate was shown to completely abolish protease function without disrupting the stability or conformation of the protein ( 29 ).…”

Section: Resultsmentioning

confidence: 99%

CaaX-Like Protease of Cyanobacterial Origin Is Required for Complex Plastid Biogenesis in Malaria Parasites

Meister

Tang

Pulkoski-Gross

et al. 2020

mBio

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Plasmodium parasites and related apicomplexans contain an essential “complex plastid” organelle of secondary endosymbiotic origin, the apicoplast. Biogenesis of this complex plastid poses a unique challenge requiring evolution of new cellular machinery. We previously conducted a mutagenesis screen for essential apicoplast biogenesis genes to discover organellar pathways with evolutionary and biomedical significance. Here we validate and characterize a gene candidate from our screen, Pf3D7_0913500. Using a conditional knockdown strain, we show that Pf3D7_0913500 depletion causes growth inhibition that is rescued by the sole essential product of the apicoplast, isopentenyl pyrophosphate (IPP), and results in apicoplast loss. Because Pf3D7_0913500 had no previous functional annotation, we name it apicoplast-minus IPP-rescued 4 (AMR4). AMR4 has an annotated CaaX protease and bacteriocin processing (CPBP) domain, which in eukaryotes typically indicates a role in CaaX postprenylation processing. Indeed, AMR4 is the only putative CaaX-like protease in Plasmodium parasites which are known to require protein prenylation, and we confirm that the conserved catalytic residue of AMR4 (E352) is required for its apicoplast function. However, we unexpectedly find that AMR4 does not act in a CaaX postprenylation processing pathway in Plasmodium falciparum. Instead, we find that AMR4 is imported into the apicoplast and is derived from a cyanobacterial CPBP gene which was retained through both primary and secondary endosymbiosis. Our findings suggest that AMR4 is not a true CaaX protease, but instead it performs a conserved, uncharacterized chloroplast function that has been retained for complex plastid biogenesis. IMPORTANCE Plasmodium parasites, which cause malaria, and related apicomplexans are important human and veterinary pathogens. These parasites represent a highly divergent and understudied branch of eukaryotes, and as such often defy the expectations set by model organisms. One striking example of unique apicomplexan biology is the apicoplast, an essential but nonphotosynthetic plastid derived from an unusual secondary (eukaryote-eukaryote) endosymbiosis. Endosymbioses are a major driver of cellular innovation, and apicoplast biogenesis pathways represent a hot spot for molecular evolution. We previously conducted an unbiased screen for apicoplast biogenesis genes in P. falciparum to uncover these essential and innovative pathways. Here, we validate a novel gene candidate from our screen and show that its role in apicoplast biogenesis does not match its functional annotation predicted by model eukaryotes. Our findings suggest that an uncharacterized chloroplast maintenance pathway has been reused for complex plastid biogenesis in this divergent branch of pathogens.

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Rce1: mechanism and inhibition

Cited by 41 publications

References 117 publications

Rce1 suppresses invasion and metastasis of hepatocellular carcinoma via epithelial‐mesenchymal transition induced by the TGF‐β1/H‐Ras signaling pathway

Rce1 suppresses invasion and metastasis of hepatocellular carcinoma via epithelial‐mesenchymal transition induced by the TGF‐β1/H‐Ras signaling pathway

Targeting RAS‐converting enzyme 1 overcomes senescence and improves progeria‐like phenotypes of ZMPSTE24 deficiency

CaaX-Like Protease of Cyanobacterial Origin Is Required for Complex Plastid Biogenesis in Malaria Parasites

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