Lipid-targeting pleckstrin homology domain turns its autoinhibitory face toward the TEC kinases

Amatya, Neha; Wales, Thomas E.; Kwon, Annie; Yeung, Wayland; Joseph, Rajiv; Fulton, D. Bruce; Kannan, Natarajan; Engen, John R.; Andreotti, Amy H.

doi:10.1073/pnas.1907566116

Cited by 22 publications

(31 citation statements)

References 56 publications

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“…Previous work has established that the regulatory SH3 and SH2 domains of BTK assemble into a compact autoinhibitory conformation on the ‘distal’ surface of the kinase domain, similar to the autoinhibited SRC kinases ( Figure 1b ; Joseph et al, 2017 ; Wang et al, 2015 ). Solution data support an additional autoinhibitory interface on the activation loop face of the kinase domain occupied by the PHTH domain ( Figure 1b ; Amatya et al, 2019 ; Devkota et al, 2017 ). Upon receptor-mediated activation, the regulatory domains of BTK bind their activating ligands, which releases the catalytic domain from its intramolecular interactions, thereby permitting activation loop phosphorylation and a conformational shift of the catalytic machinery from the inactive to active state.…”

Section: Introductionmentioning

confidence: 74%

“…Solution data support an additional autoinhibitory interface on the activation loop face of the kinase domain occupied by the PHTH domain ( Fig. 1b) (12,13). Upon receptor mediated activation, the regulatory domains of BTK bind their activating ligands, which releases the catalytic domain from its intramolecular interactions, thereby permitting activation loop phosphorylation and a conformational shift of the catalytic machinery from the inactive to active state.…”

Section: Introductionmentioning

confidence: 79%

“…PHTH, Pleckstrin homology-Tec homology domain; PRR, proline-rich region; SH3, Src homology three domain; SH2, Src homology two domain; L, SH2-kinase linker; FL, full-length; 32LKD, SH3-SH2-linker-kinase domain; and LKD, linker-kinase domain. ( b ) Domain arrangement of BTK full-length (FL) in the autoinhibited conformation (left) based on the crystal structure of the BTK SH3-SH2-kinase (32LKD) fragment (PDB ID: 4XI2) and solution data supporting an autoinhibitory interaction between the PHTH domain and the activation loop face of the kinase domain ( Amatya et al, 2019 ; Devkota et al, 2017 ). The location of T316 in the SH2 domain is indicated with a black circle.…”

Section: Introductionmentioning

confidence: 99%

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Differential impact of BTK active site inhibitors on the conformational state of full-length BTK

Joseph

Amatya

Fulton

et al. 2020

eLife

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Bruton's tyrosine kinase (BTK) is targeted in the treatment of B-cell disorders including leukemias and lymphomas. Currently approved BTK inhibitors, including Ibrutinib, a first-in-class covalent inhibitor of BTK, bind directly to the kinase active site. While effective at blocking the catalytic activity of BTK, consequences of drug binding on the global conformation of full-length BTK are unknown. Here we uncover a range of conformational effects in full-length BTK induced by a panel of active site inhibitors, including large-scale shifts in the conformational equilibria of the regulatory domains. Additionally, we find that a remote Ibrutinib resistance mutation, T316A in the BTK SH2 domain, drives spurious BTK activity by destabilizing the compact autoinhibitory conformation of full-length BTK, shifting the conformational ensemble away from the autoinhibited form. Future development of BTK inhibitors will need to consider long-range allosteric consequences of inhibitor binding, including the emerging application of these BTK inhibitors in treating COVID-19.

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Section: Introductionmentioning

confidence: 74%

Section: Introductionmentioning

confidence: 79%

Section: Introductionmentioning

confidence: 99%

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Differential impact of BTK active site inhibitors on the conformational state of full-length BTK

Joseph

Amatya

Fulton

et al. 2020

eLife

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“…The BTK PHTH domain in Pose 2 (Figure 4) blocks access of substrate to the kinase domain active site (Amatya et al, 2019) and the residues of the PHTH domain that mediate this autoinhibitory interaction (Y42 and D43) (Devkota et al, 2017;Joseph et al, 2017) are the same residues that mediate the Saraste dimer interface suggesting that this autoinhibitory pose is likely mutually exclusive with the active BTK dimer. The (D) Once PIP 3 levels in the membrane surpass the required threshold, BTK engages PIP 3 via the canonical and peripheral binding sites in PHTH and BTK dimerization at the membrane is stabilized.…”

Section: A Defining Feature Of Btk and The Tec Family Kinases The Phth Domainmentioning

confidence: 99%

Reining in BTK: Interdomain Interactions and Their Importance in the Regulatory Control of BTK

Kueffer

Joseph

Andreotti

2021

Front. Cell Dev. Biol.

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Since Dr. Ogden Bruton’s 1952 paper describing the first human primary immunodeficiency disease, the peripheral membrane binding signaling protein, aptly named Bruton’s tyrosine kinase (BTK), has been the target of intense study. Dr. Bruton’s description of agammaglobulinemia set the stage for ultimately understanding key signaling steps emanating from the B cell receptor. BTK is a multidomain tyrosine kinase and in the decades since Dr. Bruton’s discovery it has become clear that genetic defects in the regulatory domains or the catalytic domain can lead to immunodeficiency. This finding underscores the intricate regulatory mechanisms within the BTK protein that maintain appropriate levels of signaling both in the resting B cell and during an immune challenge. In recent decades, BTK has become a target for clinical intervention in treating B cell malignancies. The survival reliance of B cell malignancies on B cell receptor signaling has allowed small molecules that target BTK to become essential tools in treating patients with hematological malignancies. The first-in-class Ibrutinib and more selective second-generation inhibitors all target the active site of the multidomain BTK protein. Therapeutic interventions targeting BTK have been successful but are plagued by resistance mutations that render drug treatment ineffective for some patients. This review will examine the molecular mechanisms that drive drug resistance, the long-range conformational effects of active site inhibitors on the BTK regulatory apparatus, and emerging opportunities to allosterically target the BTK kinase to improve therapeutic interventions using combination therapies.

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“…Bruton ‘s tyrosine kinase (Btk) and Interleukin-2-inducible T cell kinase (Itk) are known to play a key role in B cell and T cell receptor signaling, respectively [ 77 ]. Both Btk and Itk are localized in the cytoplasm in resting cells and translocate to the plasma membrane upon receptor activation through binding of their PH domains to PtdIns(3,4,5) P 3 [ 78 ]. Small compounds targeting the interaction between Btk PH domain and PtdIns(3,4,5) P 3 have been developed [ 79 ].…”

Section: Targeting Ph Domains Of Signaling Proteins: Beyond Aktmentioning

confidence: 99%

Inositol Polyphosphate-Based Compounds as Inhibitors of Phosphoinositide 3-Kinase-Dependent Signaling

Maffucci

Falasca

2020

IJMS

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Signaling pathways regulated by the phosphoinositide 3-kinase (PI3K) enzymes have a well-established role in cancer development and progression. Over the past 30 years, the therapeutic potential of targeting this pathway has been well recognized, and this has led to the development of a multitude of drugs, some of which have progressed into clinical trials, with few of them currently approved for use in specific cancer settings. While many inhibitors compete with ATP, hence preventing the catalytic activity of the kinases directly, a deep understanding of the mechanisms of PI3K-dependent activation of its downstream effectors led to the development of additional strategies to prevent the initiation of this signaling pathway. This review summarizes previously published studies that led to the identification of inositol polyphosphates as promising parent molecules to design novel inhibitors of PI3K-dependent signals. We focus our attention on the inhibition of protein–membrane interactions mediated by binding of pleckstrin homology domains and phosphoinositides that we proposed 20 years ago as a novel therapeutic strategy.

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Lipid-targeting pleckstrin homology domain turns its autoinhibitory face toward the TEC kinases

Cited by 22 publications

References 56 publications

Differential impact of BTK active site inhibitors on the conformational state of full-length BTK

Differential impact of BTK active site inhibitors on the conformational state of full-length BTK

Reining in BTK: Interdomain Interactions and Their Importance in the Regulatory Control of BTK

Inositol Polyphosphate-Based Compounds as Inhibitors of Phosphoinositide 3-Kinase-Dependent Signaling

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