The ATP-Releasing Maxi-Cl Channel: Its Identity, Molecular Partners, and Physiological/Pathophysiological Implications

Sabirov, Ravshan Z.; Islam, Md. Rafiqul; Okada, Toshiaki; Merzlyak, Petr G.; Kurbannazarova, Ranokhon Sh.; Tsiferova, Nargiza A.; Okada, Yasunobu

doi:10.3390/life11060509

Cited by 15 publications

(18 citation statements)

References 163 publications

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“…Electrophysiological properties of these three types of volume-related anion channels were directly studied by observing their channel currents using patch-clamp techniques, and those were described in detail so far in the review articles for VSOR/VRAC ( Strange et al, 1996 ; Nilius et al, 1997 ; Okada, 1997 ), Maxi-Cl ( Sabirov et al, 2016 , 2021 ), and ASOR/PAC ( Okada et al, 2021b ). The pharmacological properties of these three types of volume-related anion channels are different from each other, as recently summarized in our review article ( Okada et al, 2019b ).…”

Section: Functional Properties Of Volume-sensitive Outwardly Rectifying Anion Channel/volume-regulated Anion Channel Maxi-anion Channel Amentioning

confidence: 99%

Properties, Structures, and Physiological Roles of Three Types of Anion Channels Molecularly Identified in the 2010’s

et al. 2021

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Molecular identification was, at last, successfully accomplished for three types of anion channels that are all implicated in cell volume regulation/dysregulation. LRRC8A plus LRRC8C/D/E, SLCO2A1, and TMEM206 were shown to be the core or pore-forming molecules of the volume-sensitive outwardly rectifying anion channel (VSOR) also called the volume-regulated anion channel (VRAC), the large-conductance maxi-anion channel (Maxi-Cl), and the acid-sensitive outwardly rectifying anion channel (ASOR) also called the proton-activated anion channel (PAC) in 2014, 2017, and 2019, respectively. More recently in 2020 and 2021, we have identified the S100A10-annexin A2 complex and TRPM7 as the regulatory proteins for Maxi-Cl and VSOR/VRAC, respectively. In this review article, we summarize their biophysical and structural properties as well as their physiological roles by comparing with each other on the basis of their molecular insights. We also point out unsolved important issues to be elucidated soon in the future.

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Section: Functional Properties Of Volume-sensitive Outwardly Rectifying Anion Channel/volume-regulated Anion Channel Maxi-anion Channel Amentioning

confidence: 99%

Properties, Structures, and Physiological Roles of Three Types of Anion Channels Molecularly Identified in the 2010’s

et al. 2021

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“… * In situ hybridization, Northern Blot, RT-PCR were used to measure mRNA levels, * * western blot to detect protein and * * * immunohistochemistry, immunocytochemistry and immunofluorescence as well as cell fractions and vesicles were used to report localization of ion channels. # A complex with solute carrier organic anion transporter family member 2A1 as a core pore-forming component and two auxiliary regulatory proteins, annexin A2 and S100 calcium binding protein A10 [ 115 ]. CaV, voltage-gated calcium channel; CFTR, cystic fibrosis transmembrane conductance regulator (ATP-binding cassette sub-family C, member 7); CLC, chloride channel; Cx, connexin; K 2P , two-pore domain potassium channel; KCa, calcium-activated potassium channel; K ir , inwardly rectifying potassium channel; nAchR, nicotinic acetylcholine receptor; Na V , voltage-gated sodium channel; P2X, purinergic receptor P2X Px, pannexin; Ryr, ryanodine receptor; TRPM, transient receptor potential cation channel subfamily M; TRPP, transient receptor potential cation channel subfamily P; TRPV, transient receptor potential cation channel subfamily V; ZAC, zinc-activated channel.…”

Section: Placental Ion Channelsmentioning

confidence: 99%

Section: Placental Ion Channelsmentioning

confidence: 99%

“…However, the expression of these chloride channels is increased in placentae of pre-eclamptic (PE) and intra-uterine growth retardation pregnancies (IUGR), but it remains to be studied whether they contribute to pathological processes of these conditions [ 65 , 90 ]. Maxi-chloride channel is a complex with solute carrier organic anion transporter family member 2A1 (SLCO2A1) as pore-forming component and two auxiliary regulatory proteins, annexin 2 and S100 calcium binding protein A10 (S100A10) [ 115 ] Maxi-chloride channel has been shown to be regulated by arachidonic acid, fatty acids and steroid hormones [ 120 ]. In addition to chloride, the maxi-chloride channel is permeable to amino acids and it may have a role in placental volume regulation [ 121 ].…”

Section: Placental Ion Channelsmentioning

confidence: 99%

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Placental ion channels: potential target of chemical exposure

Zhao

Pasanen

Rysä

2022

Biology of Reproduction

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The placenta is an important organ for the exchange of substances between the fetus and the mother, hormone secretion and fetoplacental immunological defense. Placenta has organ-specific distribution of ion channels and trophoblasts, and placental vessels express a large number of ion channels. Several placental house-keeping activities and pregnancy complications are at least partly controlled by ion channels, which are playing an important role in regulating hormone secretion, trophoblastic homeostasis, ion transport, and vasomotor activity. The function of several placental ion channels (Na, Ca and Cl ion channels, cation channel, nicotinic acetylcholine receptors and aquaporin-1) are known to be influenced by chemical exposure i.e. their responses to different chemicals have been tested and confirmed in experimental models. Here we review the possibility that placental ion channels are targets of toxicological concern in terms of placental function, fetal growth and development.

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“…At this time, neither the identity nor the role of this channel was known. It now appears that its core component is the organic anion transporter SLCO2A1, which, in its resting (closed) state, functions as a prostaglandin transporter and in its active (open) state as a channel releasing mainly chloride and ATP [ 57 ]. This channel is thought to be involved in cell volume regulation and purinergic cell-to-cell signaling.…”

Section: Thiamine Triphosphate: Occurrence Synthesis Regulation and Rolementioning

confidence: 99%

Update on Thiamine Triphosphorylated Derivatives and Metabolizing Enzymatic Complexes

Bettendorff

2021

Biomolecules

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While the cellular functions of the coenzyme thiamine (vitamin B1) diphosphate (ThDP) are well characterized, the triphosphorylated thiamine derivatives, thiamine triphosphate (ThTP) and adenosine thiamine triphosphate (AThTP), still represent an intriguing mystery. They are present, generally in small amounts, in nearly all organisms, bacteria, fungi, plants, and animals. The synthesis of ThTP seems to require ATP synthase by a mechanism similar to ATP synthesis. In E. coli, ThTP is synthesized during amino acid starvation, while in plants, its synthesis is dependent on photosynthetic processes. In E. coli, ThTP synthesis probably requires oxidation of pyruvate and may play a role at the interface between energy and amino acid metabolism. In animal cells, no mechanism of regulation is known. Cytosolic ThTP levels are controlled by a highly specific cytosolic thiamine triphosphatase (ThTPase), coded by thtpa, and belonging to the ubiquitous family of the triphosphate tunnel metalloenzymes (TTMs). While members of this protein family are found in nearly all living organisms, where they bind organic and inorganic triphosphates, ThTPase activity seems to be restricted to animals. In mammals, THTPA is ubiquitously expressed with probable post-transcriptional regulation. Much less is known about the recently discovered AThTP. In E. coli, AThTP is synthesized by a high molecular weight protein complex from ThDP and ATP or ADP in response to energy stress. A better understanding of these two thiamine derivatives will require the use of transgenic models.

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The ATP-Releasing Maxi-Cl Channel: Its Identity, Molecular Partners, and Physiological/Pathophysiological Implications

Cited by 15 publications

References 163 publications

Properties, Structures, and Physiological Roles of Three Types of Anion Channels Molecularly Identified in the 2010’s

Properties, Structures, and Physiological Roles of Three Types of Anion Channels Molecularly Identified in the 2010’s

Placental ion channels: potential target of chemical exposure

Update on Thiamine Triphosphorylated Derivatives and Metabolizing Enzymatic Complexes

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