Novel KCNQ4 variants in different functional domains confer genotype- and mechanism-based therapeutics in patients with nonsyndromic hearing loss

Sang Yeon Lee; Hyun Been Choi; Mina Park; Il Soon Choi; Jieun An; Ami Kim; Eunku Kim; Nahyun Kim; Jin Hee Han; Min young Kim; Seung min Lee; Doo Yi Oh; Bong Jik Kim; Nayoung Yi; Nayoung, K.D. Kim; Chung Lee; Woong Yang Park; Young Ik Koh; Heon Yung Gee; Hyun Sung Cho; Tong Mook Kang; Byung Yoon Choi

doi:10.1038/s12276-021-00653-4

Novel KCNQ4 variants in different functional domains confer genotype- and mechanism-based therapeutics in patients with nonsyndromic hearing loss

Sang Yeon Lee, Hyun Been Choi, Mina Park, Il Soon Choi, Jieun An, Ami Kim, Eunku Kim, Nahyun Kim, Jin Hee Han, Min young Kim, Seung min Lee, Doo Yi Oh, Bong Jik Kim, Nayoung Yi, Nayoung, K.D. Kim, Chung Lee, Woong Yang Park, Young Ik Koh, Heon Yung Gee, Hyun Sung ChoTong Mook Kang, Byung Yoon Choi

Department of Pharmacology

Research output: Contribution to journal › Article › peer-review

18 Citations (Scopus)

Abstract

Loss-of-function variant in the gene encoding the KCNQ4 potassium channel causes autosomal dominant nonsyndromic hearing loss (DFNA2), and no effective pharmacotherapeutics have been developed to reverse channel activity impairment. Phosphatidylinositol 4,5-bisphosphate (PIP₂), an obligatory phospholipid for maintaining KCNQ channel activity, confers differential pharmacological sensitivity of channels to KCNQ openers. Through whole-exome sequencing of DFNA2 families, we identified three novel KCNQ4 variants related to diverse auditory phenotypes in the proximal C-terminus (p.Arg331Gln), the C-terminus of the S6 segment (p.Gly319Asp), and the pore region (p.Ala271_Asp272del). Potassium currents in HEK293T cells expressing each KCNQ4 variant were recorded by patch-clamp, and functional recovery by PIP₂ expression or KCNQ openers was examined. In the homomeric expression setting, the three novel KCNQ4 mutant proteins lost conductance and were unresponsive to KCNQ openers or PIP₂ expression. Loss of p.Arg331Gln conductance was slightly restored by a tandem concatemer channel (WT-p.R331Q), and increased PIP₂ expression further increased the concatemer current to the level of the WT channel. Strikingly, an impaired homomeric p.Gly319Asp channel exhibited hyperactivity when a concatemer (WT-p.G319D), with a negative shift in the voltage dependence of activation. Correspondingly, a KCNQ inhibitor and chelation of PIP₂ effectively downregulated the hyperactive WT-p.G319D concatemer channel. Conversely, the pore-region variant (p.Ala271_Asp272del) was nonrescuable under any condition. Collectively, these novel KCNQ4 variants may constitute therapeutic targets that can be manipulated by the PIP₂ level and KCNQ-regulating drugs under the physiological context of heterozygous expression. Our research contributes to the establishment of a genotype/mechanism-based therapeutic portfolio for DFNA2.

Original language	English
Pages (from-to)	1192-1204
Number of pages	13
Journal	Experimental and Molecular Medicine
Volume	53
Issue number	7
DOIs	https://doi.org/10.1038/s12276-021-00653-4
Publication status	Published - 2021 Jul

Bibliographical note

Publisher Copyright:
© 2021, The Author(s).

All Science Journal Classification (ASJC) codes

Biochemistry
Molecular Medicine
Molecular Biology
Clinical Biochemistry

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10.1038/s12276-021-00653-4

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Lee, S. Y., Choi, H. B., Park, M., Choi, I. S., An, J., Kim, A., Kim, E., Kim, N., Han, J. H., Kim, M. Y., Lee, S. M., Oh, D. Y., Kim, B. J., Yi, N., Kim, N. K. D., Lee, C., Park, W. Y., Koh, Y. I., Gee, H. Y., ... Choi, B. Y. (2021). Novel KCNQ4 variants in different functional domains confer genotype- and mechanism-based therapeutics in patients with nonsyndromic hearing loss. Experimental and Molecular Medicine, 53(7), 1192-1204. https://doi.org/10.1038/s12276-021-00653-4

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title = "Novel KCNQ4 variants in different functional domains confer genotype- and mechanism-based therapeutics in patients with nonsyndromic hearing loss",

abstract = "Loss-of-function variant in the gene encoding the KCNQ4 potassium channel causes autosomal dominant nonsyndromic hearing loss (DFNA2), and no effective pharmacotherapeutics have been developed to reverse channel activity impairment. Phosphatidylinositol 4,5-bisphosphate (PIP2), an obligatory phospholipid for maintaining KCNQ channel activity, confers differential pharmacological sensitivity of channels to KCNQ openers. Through whole-exome sequencing of DFNA2 families, we identified three novel KCNQ4 variants related to diverse auditory phenotypes in the proximal C-terminus (p.Arg331Gln), the C-terminus of the S6 segment (p.Gly319Asp), and the pore region (p.Ala271_Asp272del). Potassium currents in HEK293T cells expressing each KCNQ4 variant were recorded by patch-clamp, and functional recovery by PIP2 expression or KCNQ openers was examined. In the homomeric expression setting, the three novel KCNQ4 mutant proteins lost conductance and were unresponsive to KCNQ openers or PIP2 expression. Loss of p.Arg331Gln conductance was slightly restored by a tandem concatemer channel (WT-p.R331Q), and increased PIP2 expression further increased the concatemer current to the level of the WT channel. Strikingly, an impaired homomeric p.Gly319Asp channel exhibited hyperactivity when a concatemer (WT-p.G319D), with a negative shift in the voltage dependence of activation. Correspondingly, a KCNQ inhibitor and chelation of PIP2 effectively downregulated the hyperactive WT-p.G319D concatemer channel. Conversely, the pore-region variant (p.Ala271_Asp272del) was nonrescuable under any condition. Collectively, these novel KCNQ4 variants may constitute therapeutic targets that can be manipulated by the PIP2 level and KCNQ-regulating drugs under the physiological context of heterozygous expression. Our research contributes to the establishment of a genotype/mechanism-based therapeutic portfolio for DFNA2.",

author = "Lee, {Sang Yeon} and Choi, {Hyun Been} and Mina Park and Choi, {Il Soon} and Jieun An and Ami Kim and Eunku Kim and Nahyun Kim and Han, {Jin Hee} and Kim, {Min young} and Lee, {Seung min} and Oh, {Doo Yi} and Kim, {Bong Jik} and Nayoung Yi and Kim, {Nayoung, K.D.} and Chung Lee and Park, {Woong Yang} and Koh, {Young Ik} and Gee, {Heon Yung} and Cho, {Hyun Sung} and Kang, {Tong Mook} and Choi, {Byung Yoon}",

note = "Publisher Copyright: {\textcopyright} 2021, The Author(s).",

year = "2021",

month = jul,

doi = "10.1038/s12276-021-00653-4",

language = "English",

volume = "53",

pages = "1192--1204",

journal = "Experimental and Molecular Medicine",

issn = "1226-3613",

publisher = "Springer Nature",

number = "7",

}

Lee, SY, Choi, HB, Park, M, Choi, IS, An, J, Kim, A, Kim, E, Kim, N, Han, JH, Kim, MY, Lee, SM, Oh, DY, Kim, BJ, Yi, N, Kim, NKD, Lee, C, Park, WY, Koh, YI, Gee, HY, Cho, HS, Kang, TM & Choi, BY 2021, 'Novel KCNQ4 variants in different functional domains confer genotype- and mechanism-based therapeutics in patients with nonsyndromic hearing loss', Experimental and Molecular Medicine, vol. 53, no. 7, pp. 1192-1204. https://doi.org/10.1038/s12276-021-00653-4

TY - JOUR

T1 - Novel KCNQ4 variants in different functional domains confer genotype- and mechanism-based therapeutics in patients with nonsyndromic hearing loss

AU - Lee, Sang Yeon

AU - Choi, Hyun Been

AU - Park, Mina

AU - Choi, Il Soon

AU - An, Jieun

AU - Kim, Ami

AU - Kim, Eunku

AU - Kim, Nahyun

AU - Han, Jin Hee

AU - Kim, Min young

AU - Lee, Seung min

AU - Oh, Doo Yi

AU - Kim, Bong Jik

AU - Yi, Nayoung

AU - Kim, Nayoung, K.D.

AU - Lee, Chung

AU - Park, Woong Yang

AU - Koh, Young Ik

AU - Gee, Heon Yung

AU - Cho, Hyun Sung

AU - Kang, Tong Mook

AU - Choi, Byung Yoon

PY - 2021/7

Y1 - 2021/7

N2 - Loss-of-function variant in the gene encoding the KCNQ4 potassium channel causes autosomal dominant nonsyndromic hearing loss (DFNA2), and no effective pharmacotherapeutics have been developed to reverse channel activity impairment. Phosphatidylinositol 4,5-bisphosphate (PIP2), an obligatory phospholipid for maintaining KCNQ channel activity, confers differential pharmacological sensitivity of channels to KCNQ openers. Through whole-exome sequencing of DFNA2 families, we identified three novel KCNQ4 variants related to diverse auditory phenotypes in the proximal C-terminus (p.Arg331Gln), the C-terminus of the S6 segment (p.Gly319Asp), and the pore region (p.Ala271_Asp272del). Potassium currents in HEK293T cells expressing each KCNQ4 variant were recorded by patch-clamp, and functional recovery by PIP2 expression or KCNQ openers was examined. In the homomeric expression setting, the three novel KCNQ4 mutant proteins lost conductance and were unresponsive to KCNQ openers or PIP2 expression. Loss of p.Arg331Gln conductance was slightly restored by a tandem concatemer channel (WT-p.R331Q), and increased PIP2 expression further increased the concatemer current to the level of the WT channel. Strikingly, an impaired homomeric p.Gly319Asp channel exhibited hyperactivity when a concatemer (WT-p.G319D), with a negative shift in the voltage dependence of activation. Correspondingly, a KCNQ inhibitor and chelation of PIP2 effectively downregulated the hyperactive WT-p.G319D concatemer channel. Conversely, the pore-region variant (p.Ala271_Asp272del) was nonrescuable under any condition. Collectively, these novel KCNQ4 variants may constitute therapeutic targets that can be manipulated by the PIP2 level and KCNQ-regulating drugs under the physiological context of heterozygous expression. Our research contributes to the establishment of a genotype/mechanism-based therapeutic portfolio for DFNA2.

AB - Loss-of-function variant in the gene encoding the KCNQ4 potassium channel causes autosomal dominant nonsyndromic hearing loss (DFNA2), and no effective pharmacotherapeutics have been developed to reverse channel activity impairment. Phosphatidylinositol 4,5-bisphosphate (PIP2), an obligatory phospholipid for maintaining KCNQ channel activity, confers differential pharmacological sensitivity of channels to KCNQ openers. Through whole-exome sequencing of DFNA2 families, we identified three novel KCNQ4 variants related to diverse auditory phenotypes in the proximal C-terminus (p.Arg331Gln), the C-terminus of the S6 segment (p.Gly319Asp), and the pore region (p.Ala271_Asp272del). Potassium currents in HEK293T cells expressing each KCNQ4 variant were recorded by patch-clamp, and functional recovery by PIP2 expression or KCNQ openers was examined. In the homomeric expression setting, the three novel KCNQ4 mutant proteins lost conductance and were unresponsive to KCNQ openers or PIP2 expression. Loss of p.Arg331Gln conductance was slightly restored by a tandem concatemer channel (WT-p.R331Q), and increased PIP2 expression further increased the concatemer current to the level of the WT channel. Strikingly, an impaired homomeric p.Gly319Asp channel exhibited hyperactivity when a concatemer (WT-p.G319D), with a negative shift in the voltage dependence of activation. Correspondingly, a KCNQ inhibitor and chelation of PIP2 effectively downregulated the hyperactive WT-p.G319D concatemer channel. Conversely, the pore-region variant (p.Ala271_Asp272del) was nonrescuable under any condition. Collectively, these novel KCNQ4 variants may constitute therapeutic targets that can be manipulated by the PIP2 level and KCNQ-regulating drugs under the physiological context of heterozygous expression. Our research contributes to the establishment of a genotype/mechanism-based therapeutic portfolio for DFNA2.

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Novel KCNQ4 variants in different functional domains confer genotype- and mechanism-based therapeutics in patients with nonsyndromic hearing loss

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