Structural basis of recognition of farnesylated and methylated KRAS4b by PDEδ

Dharmaiah, Srisathiyanarayanan; Bindu, Lakshman; Tran, Timothy H.; Gillette, William; Frank, Peter; Ghirlando, Rodolfo; Nissley, Dwight V.; Esposito, Dominic; McCormick, Frank; Stephen, Andrew; Simanshu, Dhirendra K.

doi:10.1073/pnas.1615316113

Cited by 146 publications

(210 citation statements)

References 62 publications

(73 reference statements)

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“…However, it is still unclear to what extent designing drugs to inhibit the interaction of K-Ras4B with PDEδ would accomplish this goal. The recent structure [82] coupled with earlier observations [83] and modeling suggest that PDEδ may be able to bind other depalmitoylated isoforms, and geranyl-geranylated K-Ras is also a PDEδ substrate; not only farnesylated K-Ras. CaM’s interaction with K-Ras4B and its role in KRAS -driven cancers have long been considered an option [5].…”

Section: Discussionmentioning

confidence: 99%

Calmodulin and PI3K Signaling in KRAS Cancers

et al. 2017

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Calmodulin (CaM) uniquely promotes signaling of oncogenic K-Ras; but not N-Ras or H-Ras. How CaM interacts with K-Ras and how this stimulates cell proliferation are among the most challenging questions in KRAS-driven cancers. Earlier data pointed to formation of a ternary complex consisting of K-Ras, PI3Kα and CaM. Recent data point to phosphorylated CaM binding to the SH2 domains of the p85 subunit of PI3Kα and activating it. Modeling suggests that the high affinity interaction between the phosphorylated CaM tyrosine motif and PI3Kα, can promote full PI3Kα activation by oncogenic K-Ras. Our up-to-date review discusses CaM’s role in PI3K signaling at the membrane in KRAS-driven cancers. This is significant since it may help development of K-Ras-specific pharmacology.

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Section: Discussionmentioning

confidence: 99%

Calmodulin and PI3K Signaling in KRAS Cancers

et al. 2017

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“…Full Length KRas4b was solvated and equilibrated for 20 ns using NAMD 2.11 molecular Dynamics software package [17] and was later found to be nearly identical to the recently published full-length structure of KRas4b. [18]…”

Section: Methodsmentioning

confidence: 99%

Interaction of KRas4b with anionic membranes: A special role for PIP 2

Gregory

McLean

Sligar

2017

Biochemical and Biophysical Research Communications

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KRas4b is a small G-protein whose constitutively active oncogenic mutants are present in 90% of pancreatic cancers. Using fully post-translationally modified KRAS4b, we investigated the role of lipid identity in the recruitment of KRas4b to a membrane surface of defined composition. Application of a newly developed single frequency fluorescence anisotropy decay experiment to this system revealed that KRas4b has a significant binding preference for Nanodisc bilayers containing PIP2. We conducted molecular dynamics simulations to look for an origin of this specificity. In the case of membranes containing PIP2 the protein formed long-lived salt bridges with PIP2 head groups but not the monovalent DMPS, explaining the experimentally observed lipid specificity. Additionally, we report that PIP2 forms key contacts with Helix-4 on the catalytic domain of KRas4b that orient the protein in a manner expected to facilitate association with upstream and downstream signaling partners.

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“…Our structural work on full-length KRAS4b in complex with PDEδ showed that unlike Rho and Rab GDIs that interact with both prenylated lipid and switch regions of G-domain, PDEδ only interacts with the C-terminal amino acids together with the farnesylated and methylated C185 of KRAS4b (Dharmaiah et al, 2016). Structure-based sequence analysis identified a 5-amino acid long sequence motif (Lys-Ser-Lys-Thr-Lys) in KRAS4b that may enable PDEδ to bind to both farnesylated as well as geranylgeranylated KRAS4b.…”

Section: Ras Proteins In the Membranementioning

confidence: 99%

RAS Proteins and Their Regulators in Human Disease

Simanshu

Nissley

McCormick

2017

Cell

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1,316

1,350

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RAS proteins are binary switches, cycling between ON and OFF states during signal transduction. These switches are normally tightly controlled, but in RAS-related diseases, such as cancer, RASopathies, and many psychiatric disorders, mutations in the RAS genes or their regulators render RAS proteins persistently active. The structural basis of the switch and many of the pathways that RAS controls are well known, but the precise mechanisms by which RAS proteins function are less clear. All RAS biology occurs in membranes: a precise understanding of RAS’ interaction with membranes is essential to understand RAS action and to intervene in RAS-driven diseases.

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Structural basis of recognition of farnesylated and methylated KRAS4b by PDEδ

Cited by 146 publications

References 62 publications

Calmodulin and PI3K Signaling in KRAS Cancers

Calmodulin and PI3K Signaling in KRAS Cancers

Interaction of KRas4b with anionic membranes: A special role for PIP 2

RAS Proteins and Their Regulators in Human Disease

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