In silico analysis of SIGMAR1 variant (rs4879809) segregating in a consanguineous Pakistani family showing amyotrophic lateral sclerosis without frontotemporal lobar dementia

Ullah, Muhammad Ikram; Ahmad, Arsalan; Raza, Syed M.; Amar, Ali; Ali, Amjad; Bhatti, Attya; John, Peter; Mohyuddin, Aisha; Ahmad, Wasim; Hassan, Muhammad Jawad

doi:10.1007/s10048-015-0453-1

Cited by 38 publications

(29 citation statements)

References 25 publications

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“…5 Homozygous SIGMAR1 mutations cause juvenile or young-onset ALS with no cognitive deficit. [6][7][8] Here, we identified a novel SIG-MAR1 mutation together with a common, but damaging, singlenucleotide polymorphism in an ALS patient with the oldest-old onset.…”

Section: Dear Editormentioning

confidence: 99%

“…However, one of these families was subsequently identified as positive for the C9orf72 mutation, suggesting that the SIGMAR1 mutation does not exclusively explain the etiology at least in this family . Homozygous SIGMAR1 mutations cause juvenile or young‐onset ALS with no cognitive deficit . Here, we identified a novel SIGMAR1 mutation together with a common, but damaging, single‐nucleotide polymorphism in an ALS patient with the oldest‐old onset.…”

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confidence: 98%

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Compound heterozygote mutations in the SIGMAR1 gene in an oldest‐old patient with amyotrophic lateral sclerosis

Izumi

Morino

Miyamoto

et al. 2018

Geriatrics Gerontology Int

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Section: Dear Editormentioning

confidence: 99%

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confidence: 98%

Compound heterozygote mutations in the SIGMAR1 gene in an oldest‐old patient with amyotrophic lateral sclerosis

Izumi

Morino

Miyamoto

et al. 2018

Geriatrics Gerontology Int

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“…Instead, its nearest homolog is the yeast Δ8-Δ7 sterol isomerase, ERG2p, although the σ 1 receptor itself has no detectable isomerase activity 11 . Human genetic data have linked point mutants in σ 1 receptor to inherited motor neuron diseases [12][13][14] , and animal models implicate the receptor in Parkinson's disease 15 , addiction 16 , and pain 17 . A σ 1 receptor antagonist is currently in clinical trials for the treatment of neuropathic pain 7 , and agonists are in clinical trials for Alzheimer's disease 5 and ischemic stroke 6 .…”

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confidence: 99%

Structural basis for σ₁ receptor ligand recognition

Schmidt

Betz

Dror

et al. 2018

Preprint

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The σ 1 receptor is a poorly understood integral membrane protein expressed in most cells and tissues in the human body. It has been shown to modulate the activity of other membrane proteins such as ion channels and G protein-coupled receptors 1-4 , and ligands targeting the σ 1 receptor are currently in clinical trials for treatment of Alzheimer's disease 5 , ischemic stroke 6 , and neuropathic pain 7 . Despite its importance, relatively little is known regarding σ 1 receptor function at the molecular level. Here, we present crystal structures of the human σ 1 receptor bound to the classical antagonists haloperidol and NE-100, as well as the agonist (+)-pentazocine, at crystallographic resolutions of 3.1 Å, 2.9 Å, and 3.1 Å respectively. These structures reveal a unique binding pose for the agonist. The structures and accompanying molecular dynamics (MD) simulations demonstrate that the agonist induces subtle structural rearrangements in the receptor. In addition, we show that ligand binding and dissociation from σ 1 is a multistep process, with extraordinarily slow kinetics limited by receptor conformational change. We use MD simulations to reconstruct a ligand binding pathway that requires two major conformational changes. Taken together, these data provide a framework for understanding the molecular basis for agonist action at σ 1 .Discovered in 1976 8 , the σ 1 receptor has attracted interest because it binds a host of structurally dissimilar pharmacologically active compounds with high affinity (Fig. 1a). These include benzomorphans, antipsychotics, psychosis-inducing drugs, the antifungal agent fenpropimorph, sterols such as progesterone, and numerous other compounds 9 . These molecules contain few shared features, although most include a basic nitrogen atom flanked on two sides by longer hydrophobic moieties (typically

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“…σ1R is highly expressed in motor neurons [ 1 , 27 ], and autosomal recessive loss-of-function mutations in σ1R are primarily associated with distal hereditary motor neuropathy [ 10 , 46 , 47 ], and ALS/FTLD [ 23 , 48 ]. In vitro studies have revealed aberrant subcellular distribution of σ1R E102Q in NSC34 cells and have shown that cells expressing the mutant protein are more prone to apoptosis induced by ER stress than those expressing the WT protein [ 25 ].…”

Section: Discussionmentioning

confidence: 99%

The ALS-Related σ1R E102Q Mutant Eludes Ligand Control and Exhibits Anomalous Response to Calcium

Rodríguez-Muñoz

Cortés-Montero

Garzón

et al. 2020

IJMS

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Sigma receptor type 1 (σ1R) is a transmembrane protein expressed throughout the central nervous system and in certain peripheral tissues. The human σ1R E102Q mutation causes juvenile amyotrophic lateral sclerosis (ALS), likely by inducing a series of alterations in calcium efflux from the endoplasmic reticulum (ER) to mitochondria that affects calcium homeostasis and cellular survival. Here, we report the influence of calcium on σ1R E102Q associations with glutamate N-methyl-D-aspartate receptors (NMDARs), binding immunoglobulin protein (BiP), and transient receptor potential calcium channels A1, V1, and M8. The mutant protein inhibited the binding of calmodulin to these calcium channels and interacted less with BiP than wild-type σ1R, thereby contributing to calcium homeostasis dysfunction. Mutant σ1R, but not wild-type σ1R, strongly bound to histidine triad nucleotide binding protein 1, which regulates neuromuscular synaptic organization and target selection through teneurin 1. While ligands regulated the association of σ1R wild-type with NMDARs and BiP, they failed to modulate the interaction between these proteins and the σ1R E102Q mutant. Thus, the σ1R E102Q mutant exhibited an anomalous response to cytosolic calcium levels, altered affinity for target proteins, and a loss of response to regulatory ligands. We believe that these modifications may contribute to the onset of juvenile ALS.

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In silico analysis of SIGMAR1 variant (rs4879809) segregating in a consanguineous Pakistani family showing amyotrophic lateral sclerosis without frontotemporal lobar dementia

Cited by 38 publications

References 25 publications

Compound heterozygote mutations in the SIGMAR1 gene in an oldest‐old patient with amyotrophic lateral sclerosis

Compound heterozygote mutations in the SIGMAR1 gene in an oldest‐old patient with amyotrophic lateral sclerosis

Structural basis for σ₁ receptor ligand recognition

The ALS-Related σ1R E102Q Mutant Eludes Ligand Control and Exhibits Anomalous Response to Calcium

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In silico analysis of SIGMAR1 variant (rs4879809) segregating in a consanguineous Pakistani family showing amyotrophic lateral sclerosis without frontotemporal lobar dementia

Cited by 38 publications

References 25 publications

Compound heterozygote mutations in the SIGMAR1 gene in an oldest‐old patient with amyotrophic lateral sclerosis

Compound heterozygote mutations in the SIGMAR1 gene in an oldest‐old patient with amyotrophic lateral sclerosis

Structural basis for σ1 receptor ligand recognition

The ALS-Related σ1R E102Q Mutant Eludes Ligand Control and Exhibits Anomalous Response to Calcium

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Product

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Structural basis for σ₁ receptor ligand recognition