Atomic structure of the eukaryotic intramembrane RAS methyltransferase ICMT

Diver, Melinda M.; Pedi, Leanne; Koide, Shohei; Long, Stephen B.

doi:10.1038/nature25439

Cited by 37 publications

(32 citation statements)

References 43 publications

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“…These findings illustrate one of the mechanisms induced by pancreatitis to drive pancreatic tumorigenesis and provide an in vivo rationale to develop strategies targeting the process of KRAS prenylation. Therefore, efforts aiming to interfere with KRAS prenylation and target the cell membrane must be maintained and encouraged [ 21 , 22 , 23 , 24 ].…”

Section: Discussionmentioning

confidence: 99%

A Novel KRAS Antibody Highlights a Regulation Mechanism of Post-Translational Modifications of KRAS during Tumorigenesis

Assi

Pirlot

Stroobant

et al. 2020

IJMS

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KRAS is a powerful oncogene responsible for the development of many cancers. Despite the great progress in understanding its function during the last decade, the study of KRAS expression, subcellular localization, and post-translational modifications remains technically challenging. Accordingly, many facets of KRAS biology are still unknown. Antibodies could be an effective and easy-to-use tool for in vitro and in vivo research on KRAS. Here, we generated a novel rabbit polyclonal antibody that allows immunolabeling of cells and tissues overexpressing KRAS. Cell transfection experiments with expression vectors for the members of the RAS family revealed a preferential specificity of this antibody for KRAS. In addition, KRAS was sensitively detected in a mouse tissue electroporated with an expression vector. Interestingly, our antibody was able to detect endogenous forms of unprenylated (immature) and prenylated (mature) KRAS in mouse organs. We found that KRAS prenylation was increased ex vivo and in vivo in a model of KRASG12D-driven tumorigenesis, which was concomitant with an induction of expression of essential KRAS prenylation enzymes. Therefore, our tool helped us to put the light on new regulations of KRAS activation during cancer initiation. The use of this tool by the RAS community could contribute to discovering novel aspects of KRAS biology.

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Section: Discussionmentioning

confidence: 99%

A Novel KRAS Antibody Highlights a Regulation Mechanism of Post-Translational Modifications of KRAS during Tumorigenesis

Assi

Pirlot

Stroobant

et al. 2020

IJMS

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“…The ligands of many membrane-integral enzymes and transporters are hydrophobic (or at least amphipathic), implying these ligands are most likely recognized (and released) laterally, from (and to) the membrane instead of through the aqueous phase. In particular membraneintegral enzymes with lipid-like ligands include many transferases (20)(21)(22)(23)(24), as well as some translocases (25), synthases (26), polymerases (27) and proteases (28). Little is known about how most of these proteins interact with the membrane, but the increasing availability of structural data will surely help advance our understanding.…”

Section: Discussionmentioning

confidence: 99%

DHHC20 palmitoyl-transferase reshapes the membrane to foster catalysis

Stix

Song

Banerjee

et al. 2019

Preprint

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Cysteine palmitoylation, a form of S-acylation, is a key post-translational modification in cellular signaling. This type of reversible lipidation is catalyzed by a family of integral membrane proteins known as DHHC acyltransferases. The first step in the S-acylation process is the recognition of free acyl-CoA from the lipid bilayer. The DHHC enzyme then becomes autoacylated, at a site defined by a conserved Asp-His-His-Cys motif. This reaction entails ionization of the catalytic Cys. Intriguingly, in known DHHC structures this catalytic Cys appears to be exposed to the hydrophobic interior of the lipid membrane, which would be highly unfavorable for a negatively charged nucleophile, thus hindering auto-acylation. Here, we use biochemical and computational methods to reconcile these seemingly contradicting facts. First, we experimentally demonstrate that human DHHC20 is active when reconstituted in POPC nanodiscs. Microsecond-long all-atom molecular dynamics simulations are then calculated for hDHHC20 and for different acyl-CoA forms, also in POPC. Strikingly, we observe that hDHHC20 induces a drastic deformation in the membrane, particularly on the cytoplasmic side where autoacylation occurs. As a result, the catalytic Cys becomes hydrated and optimally positioned to encounter the cleavage site in acyl-CoA. In summary, we hypothesize that DHHC enzymes locally reshape the membrane to foster a morphology that is specifically adapted for acyl-CoA recognition and auto-acylation.3 Significance StatementPalmitoylation, the most common form of S-acylation and the only reversible type of protein lipidation, is ubiquitous in eukaryotic cells. In humans, for example, it has been estimated that as much as ~10% of the proteome becomes palmitoylated, i.e. thousands of proteins. Accordingly, protein palmitoylation touches every important aspect of human physiology, both in health and disease. Despite its biological and biomedical importance, little is known about the molecular mechanism of the enzymes that catalyze this post-translational modification, known as DHHC acyltransferases. Here, we leverage the recently-determined atomic-resolution structure of human DHHC20 to gain novel insights into the mechanism of this class of enzymes, using both experimental and computational approaches.

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“…It will be interesting to see whether other SBPs can inhibit nucleotide exchange in similar ways. This work on Ras/Raf has provided important insights into Ras biology, which has recently been supplemented by the development of a monobody inhibitor of isoprenylcysteine carboxyl methyltransferase, the final protein involved in the maturation of Ras [48], demonstrating that SBPs represent useful tools for targeting intracellular proteins both in vitro and in vivo, and showing that intracellular modulation of Ras is not as intransigent a problem as previously thought.…”

Section: Mitogen-activated Protein Kinase Pathwaymentioning

confidence: 99%

“…Caspases are a homologous family of proteases that function as the intracellular effectors of apoptosis. They have been targeted by DARPin binders against the various caspases with the exception of caspase 4 [48]. However, not all of the binders were able to modulate caspase function, demonstrating that inhibition/activation is not a prerequisite of binding and emphasising the importance of performing functional assays before undertaking studies to examine SBPs' intracellular properties.…”

Section: Apoptosismentioning

confidence: 99%

Non-immunoglobulin scaffold proteins: Precision tools for studying protein-protein interactions in cancer

et al. 2018

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Cancer is frequently characterised by dysregulation of the cellular signalling processes that govern proliferation, survival and attachment. Understanding such dysregulation continues to present a challenge given the importance of protein-protein interactions in intracellular processes. Exploring this protein-protein interactome requires novel tools capable of discriminating between highly homologous proteins, individual domains and post-translational modifications. This review examines the potential of scaffold-based binding proteins to fulfil these requirements. It also explores protein-protein interactions in the context of intracellular signalling pathways and cancer, and demonstrates the uses of scaffold proteins as functional moderators, biosensors and imaging reagents. This review also highlights the timeliness and potential to develop international consortia to develop and validate highly specific "proteome" scaffold-based binding protein reagents with the ultimate aim of developing screening tools for studying the interactome.

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Atomic structure of the eukaryotic intramembrane RAS methyltransferase ICMT

Cited by 37 publications

References 43 publications

A Novel KRAS Antibody Highlights a Regulation Mechanism of Post-Translational Modifications of KRAS during Tumorigenesis

A Novel KRAS Antibody Highlights a Regulation Mechanism of Post-Translational Modifications of KRAS during Tumorigenesis

DHHC20 palmitoyl-transferase reshapes the membrane to foster catalysis

Non-immunoglobulin scaffold proteins: Precision tools for studying protein-protein interactions in cancer

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