Prestin

Protein-coding gene in the species Homo sapiens

More reference expression dataBioGPS

n/a

Gene ontology
Molecular function	spectrin binding protein homodimerization activity sulfate transmembrane transporter activity secondary active sulfate transmembrane transporter activity bicarbonate transmembrane transporter activity oxalate transmembrane transporter activity chloride channel activity transcription factor binding chloride transmembrane transporter activity
Cellular component	cytoplasm integral component of membrane lateral plasma membrane membrane plasma membrane integral component of plasma membrane basolateral plasma membrane
Biological process	cochlea development response to potassium ion positive regulation of cell motility sulfate transport regulation of membrane potential response to thyroid hormone regulation of intracellular pH chloride transmembrane transport sensory perception of sound protein tetramerization negative regulation of ion transmembrane transport bicarbonate transport ion transmembrane transport response to ischemia anion transmembrane transport response to salt transmembrane transport positive regulation of cell size regulation of cell shape response to auditory stimulus response to salicylic acid fructose transmembrane transport oxalate transport sulfate transmembrane transport
Sources:Amigo / QuickGO

Orthologs

Species

Human

Mouse

Entrez


375611


80979

Ensembl


ENSG00000170615


ENSMUSG00000029015

UniProt


P58743


Q99NH7

RefSeq (mRNA)

NM_001167962 NM_198999 NM_206883 NM_206884 NM_206885
NM_001321787


NM_030727 NM_001289787 NM_001289788

RefSeq (protein)

NP_001161434 NP_001308716 NP_945350 NP_996766 NP_996767
NP_996768


NP_001276716 NP_001276717 NP_109652

Location (UCSC)

Chr 7: 103.35 – 103.45 Mb

Chr 5: 22.02 – 22.07 Mb

PubMed search

^[3]

^[4]

Wikidata

View/Edit Human

View/Edit Mouse

Prestin is a protein that is critical to sensitive hearing in mammals. It is encoded by the SLC26A5 (solute carrier anion transporter family 26, member 5) gene.^[5]^[6]

Prestin is the motor protein of the outer hair cells of the inner ear of the mammalian cochlea.^[5] It is highly expressed in the outer hair cells, and is not expressed in the nonmotile inner hair cells. Immunolocalization shows prestin is expressed in the lateral plasma membrane of the outer hair cells, the region where electromotility occurs. The expression pattern correlates with the appearance of outer hair cell electromotility.

Function

Prestin is essential in auditory processing. It is specifically expressed in the lateral membrane of outer hair cells (OHCs) of the cochlea. There is no significant difference between prestin density in high-frequency and low-frequency regions of the cochlea in fully developed mammals.^[7] There is good evidence that prestin has undergone adaptive evolution in mammals ^[8] associated with acquisition of high frequency hearing in mammals.^[9] The prestin protein shows several parallel amino acid replacements in bats, whales, and dolphins that have independently evolved ultrasonic hearing and echolocation, and these represent rare cases of convergent evolution at the sequence level.^[10]^[11]

Prestin (mol. wt. 80 kDa) is a member of a distinct family of anion transporters, SLC26. Members of this family are structurally well conserved and can mediate the electroneutral exchange of chloride and carbonate across the plasma membrane of mammalian cells, two anions found to be essential for outer hair cell motility. Unlike the classical, enzymatically driven motors, this new type of motor is based on direct voltage-to-displacement conversion and acts several orders of magnitude faster than other cellular motor proteins. A targeted gene disruption strategy of prestin showed a >100-fold (or 40 dB) loss of auditory sensitivity.^[12]

Prestin is a transmembrane protein that mechanically contracts and elongates leading to electromotility of outer hair cells (OHC). Electromotility is the driving force behind the somatic motor of the cochlear amplifier, which is a mammalian evolution that increases sensitivity to incoming sound wave frequencies and, thus, amplifies the signal. Previous research has suggested that this modulation takes place via an extrinsic voltage-sensor (partial anion transporter model), whereby chloride binds to the intracellular side of prestin and enters a defunct transporter, causing prestin elongation.^[13] However, there is new evidence that prestin acts through an intrinsic voltage-sensor (IVS) in which intracellular chloride binds allosterically to prestin to modify shape.^[14]^[15]

Intrinsic voltage sensing

In this model of intrinsic voltage-sensing, the movement of ions generates a nonlinear capacitance (NLC). Based upon the generated voltage and the depolarized or hyperpolarized state of the cell, prestin will transition through two distinct steps, representing the three-state model of prestin modulation.^[16] Experiments show that with increasing depolarizing stimuli, prestin transitions from an elongated state to an intermediate state to a contracted state, increasing its NLC. Under hyperpolarizing conditions, NLC decreases and prestin transitions back to its elongated state. Of significance, increased membrane tension as characterized by prestin elongation decreases the chloride allosteric binding site affinity for chloride, perhaps playing a role in regulation of prestin modulation. The total estimated displacement of prestin upon modulation from elongated to contracted state is 3–4 nm².^[16] A recent study supports the IVS model showing that mutations of 12 residues that span the intracellular side of prestin's core membrane resulted in significant decrease in NLC. Eight of the 12 residues were positively charged and are hypothesized to make up the allosteric chloride binding site of prestin.^[14]

Anion transport

Although previously thought to be absent, anion transport has also been shown to be an important aspect of prestin's ability to drive electromotility of hair cells.^[14]^[15] This mechanism is independent of prestin's voltage-sensing capabilities based upon mutagenesis experiments showing that different mutations lead to effects in either anion-uptake or NLC, but not both.^[14] It is suggested that prestin contains an intrinsic anion-uptake mechanism based upon research showing concentration dependent [¹⁴C]formate uptake in Chinese hamster ovary (CHO) cells. These results could not be reproduced in oocytes. Therefore, prestin may require an associated cofactor for anion uptake in oocytes; however, this hypothesis is still under question. Experiments have shown that various anions can compete for prestin uptake including malate, chloride, and alkylsulfonic anions.^[14]^[17]

Discovery

Prestin was discovered by Peter Dallos's group in 2000 and named from the musical notation presto because of the speed of the protein.^[5]

The prestin molecule was patented by its discoverers in 2003.^[18]

Clinical significance

Mutations in the SLC26A5 gene have been associated with non-syndromic hearing loss.^[6]

Blockers

Electromotile function of mammalian prestin is blocked by the amphiphilic anion salicylate at millimolar concentrations. Application of salicylate blocks prestin function in a dose-dependent and readily reversible manner.^[13]

References

^ ^a ^b ^c GRCh38: Ensembl release 89: ENSG00000170615 – Ensembl, May 2017
^ ^a ^b ^c GRCm38: Ensembl release 89: ENSMUSG00000029015 – Ensembl, May 2017
^ "Human PubMed Reference:". National Center for Biotechnology Information, U.S. National Library of Medicine.
^ "Mouse PubMed Reference:". National Center for Biotechnology Information, U.S. National Library of Medicine.
^ ^a ^b ^c Zheng J, Shen W, He DZ, Long KB, Madison LD, Dallos P (Jun 2000). "Prestin is the motor protein of cochlear outer hair cells". Nature. 405 (6783): 149–55. Bibcode:2000Natur.405..149Z. doi:10.1038/35012009. PMID 10821263. S2CID 4409772.
^ ^a ^b "Entrez Gene: SLC26A5 solute carrier family 26, member 5 (prestin)".
^ Mahendrasingam S, Beurg M, Fettiplace R, Hackney CM (2010). "The ultrastructural distribution of prestin in outer hair cells: A post-embedding immunogold investigation of low and high frequency regions of the rat cochlea". European Journal of Neuroscience. 31 (9): 1595–1605. doi:10.1111/j.1460-9568.2010.07182.x. PMC 2925464. PMID 20525072.
^ Franchini LF, Elgoyhen AB (Dec 2006). "Adaptive evolution in mammalian proteins involved in cochlear outer hair cell electromotility". Molecular Phylogenetics and Evolution. 41 (3): 622–635. doi:10.1016/j.ympev.2006.05.042. hdl:11336/79650. PMID 16854604.
^ Rossiter SJ, Zhang S, Liu Y (2011). "Prestin and high frequency hearing in mammals". Commun Integr Biol. 4 (2): 236–9. doi:10.4161/cib.4.2.14647. PMC 3104589. PMID 21655450.
^ Liu Y, Rossiter SJ, Han X, Cotton JA, Zhang S (2010). "Cetaceans on a molecular fast track to ultrasonic hearing". Curr. Biol. 20 (20): 1834–9. Bibcode:2010CBio...20.1834L. doi:10.1016/j.cub.2010.09.008. PMID 20933423.
^ Li Y, Liu Z, Shi P, Zhang P (2010). "The hearing gene Prestin unites echolocating bats and whales". Curr. Biol. 20 (2): R55–R56. Bibcode:2010CBio...20..R55L. doi:10.1016/j.cub.2009.11.042. PMID 20129037. S2CID 7367035.
^ Liberman MC, Gao J, He DZ, Wu X, Jia S, Zuo J (September 2002). "Prestin is required for electromotility of the outer hair cell and for the cochlear amplifier". Nature. 419 (6904): 300–4. Bibcode:2002Natur.419..300L. doi:10.1038/nature01059. PMID 12239568. S2CID 4412381.
^ ^a ^b Oliver D, He DZ, Klöcker N, Ludwig J, Schulte U, Waldegger S, Ruppersberg JP, Dallos P, Fakler B (2001). "Intracellular Anions as the Voltage Sensor of Prestin, the Outer Hair Cell Motor Protein". Science. 292 (5525): 2340–2343. doi:10.1126/science.1060939. PMID 11423665. S2CID 23864514.
^ ^a ^b ^c ^d ^e Bai JP, Surguchev A, Montoya S, Aronson PS, Santos-Sacchi J, Navaratnam D (2009). "Prestin's Anion Transport and Voltage-Sensing Capabilities Are Independent". Biophysical Journal. 96 (8): 3179–3186. Bibcode:2009BpJ....96.3179B. doi:10.1016/j.bpj.2008.12.3948. PMC 2718310. PMID 19383462.
^ ^a ^b Song L, Santos-Sacchi J (2010). "Conformational State-Dependent Anion Binding in Prestin: Evidence for Allosteric Modulation". Biophysical Journal. 98 (3): 371–376. Bibcode:2010BpJ....98Q.371S. doi:10.1016/j.bpj.2009.10.027. PMC 2814207. PMID 20141749.
^ ^a ^b Homma K, Dallos P (2010). "Evidence That Prestin Has at Least Two Voltage-dependent Steps". Journal of Biological Chemistry. 286 (3): 2297–2307. doi:10.1074/jbc.M110.185694. PMC 3023524. PMID 21071769.
^ Rybalchenko V, Santos-Sacchi J (2008). "Anion Control of Voltage Sensing by the Motor Protein Prestin in Outer Hair Cells". Biophysical Journal. 95 (9): 4439–4447. Bibcode:2008BpJ....95.4439R. doi:10.1529/biophysj.108.134197. PMC 2567960. PMID 18658219.
^ US granted 6602992, Dallos P, Zheng J, Madison LD, "Mammalian prestin polynucleotides", published 2003-08-05

Markovich D (2001). "Physiological roles and regulation of mammalian sulfate transporters". Physiol. Rev. 81 (4): 1499–533. doi:10.1152/physrev.2001.81.4.1499. PMID 11581495. S2CID 30942862.
Dallos P, Fakler B (2002). "Prestin, a new type of motor protein". Nat. Rev. Mol. Cell Biol. 3 (2): 104–11. doi:10.1038/nrm730. PMID 11836512. S2CID 7333228.
Dallos P, Zheng J, Cheatham MA (2006). "Prestin and the cochlear amplifier". J. Physiol. 576 (Pt 1): 37–42. doi:10.1113/jphysiol.2006.114652. PMC 1995634. PMID 16873410.
Sanger Centre T, Washington University Genome Sequencing Cente T (1999). "Toward a complete human genome sequence". Genome Res. 8 (11): 1097–108. doi:10.1101/gr.8.11.1097. PMID 9847074.
Lohi H, Kujala M, Kerkelä E, Saarialho-Kere U, Kestilä M, Kere J (2001). "Mapping of five new putative anion transporter genes in human and characterization of SLC26A6, a candidate gene for pancreatic anion exchanger". Genomics. 70 (1): 102–12. doi:10.1006/geno.2000.6355. PMID 11087667.
Weber T, Zimmermann U, Winter H, Mack A, Köpschall I, Rohbock K, Zenner HP, Knipper M (2002). "Thyroid hormone is a critical determinant for the regulation of the cochlear motor protein prestin". Proc. Natl. Acad. Sci. U.S.A. 99 (5): 2901–6. Bibcode:2002PNAS...99.2901W. doi:10.1073/pnas.052609899. PMC 122445. PMID 11867734.
Liberman MC, Gao J, He DZ, Wu X, Jia S, Zuo J (2002). "Prestin is required for electromotility of the outer hair cell and for the cochlear amplifier". Nature. 419 (6904): 300–4. Bibcode:2002Natur.419..300L. doi:10.1038/nature01059. PMID 12239568. S2CID 4412381.
Liu XZ, Ouyang XM, Xia XJ, Zheng J, Pandya A, Li F, Du LL, Welch KO, Petit C, Smith RJ, Webb BT, Yan D, Arnos KS, Corey D, Dallos P, Nance WE, Chen ZY (2004). "Prestin, a cochlear motor protein, is defective in non-syndromic hearing loss". Hum. Mol. Genet. 12 (10): 1155–62. doi:10.1093/hmg/ddg127. PMID 12719379.
Dong XX, Iwasa KH (2004). "Tension sensitivity of prestin: comparison with the membrane motor in outer hair cells". Biophys. J. 86 (2): 1201–8. Bibcode:2004BpJ....86.1201D. doi:10.1016/S0006-3495(04)74194-6. PMC 1303912. PMID 14747354.
Matsuda K, Zheng J, Du GG, Klöcker N, Madison LD, Dallos P (2004). "N-linked glycosylation sites of the motor protein prestin: effects on membrane targeting and electrophysiological function". J. Neurochem. 89 (4): 928–38. doi:10.1111/j.1471-4159.2004.02377.x. PMID 15140192. S2CID 24400032.
Chambard JM, Ashmore JF (2005). "Regulation of the voltage-gated potassium channel KCNQ4 in the auditory pathway". Pflügers Arch. 450 (1): 34–44. doi:10.1007/s00424-004-1366-2. PMID 15660259. S2CID 21570482.
Rajagopalan L, Patel N, Madabushi S, Goddard JA, Anjan V, Lin F, Shope C, Farrell B, Lichtarge O, Davidson AL, Brownell WE, Pereira FA (2006). "Essential helix interactions in the anion transporter domain of prestin revealed by evolutionary trace analysis". J. Neurosci. 26 (49): 12727–34. doi:10.1523/JNEUROSCI.2734-06.2006. PMC 2675645. PMID 17151276.
Toth T, Deak L, Fazakas F, Zheng J, Muszbek L, Sziklai I (2007). "A new mutation in the human pres gene and its effect on prestin function". Int. J. Mol. Med. 20 (4): 545–50. doi:10.3892/ijmm.20.4.545. hdl:2437/4636. PMID 17786286.

This article incorporates text from the United States National Library of Medicine, which is in the public domain.

Membrane proteins, carrier proteins: membrane transport proteins solute carrier (TC 2A)

By group

SLC1–10

(1):	high affinity glutamate and neutral amino-acid transporter SLC1A1 2 3 4 5 6 7
(2):	facilitative GLUT transporter SLC2A1 2 3 4 5 6 7 8 9 10 11 12 13 14
(3):	heavy subunits of heterodimeric amino-acid transporters SLC3A1 2
(4):	bicarbonate transporter SLC4A1 2 3 4 5 6 7 8 9 10 11
(5):	sodium glucose cotransporter SLC5A1 2 3 4 5 6 7 8 9 10 11 12
(6):	sodium- and chloride- dependent sodium:neurotransmitter symporters SLC6A1 SLC6A2 SLC6A3 SLC6A4 SLC6A5 SLC6A6 SLC6A7 SLC6A8 SLC6A9 SLC6A10 SLC6A11 SLC6A12 SLC6A13 SLC6A14 SLC6A15 SLC6A16 SLC6A17 SLC6A18 SLC6A19 SLC6A20
(7):	cationic amino-acid transporter/glycoprotein-associated SLC7A1 SLC7A2 SLC7A3 SLC7A4 glycoprotein-associated/light or catalytic subunits of heterodimeric amino-acid transporters SLC7A5 SLC7A6 SLC7A7 SLC7A8 SLC7A9 SLC7A10 SLC7A11 SLC7A13 SLC7A14
(8):	Na⁺/Ca²⁺ exchanger SLC8A1 SLC8A2 SLC8A3
(9):	Na⁺/H⁺ exchanger SLC9A1 SLC9A2 SLC9A3 SLC9A4 SLC9A5 SLC9A6 SLC9A7 SLC9A8 SLC9A9 SLC9A10 SLC9A11
(10):	sodium bile salt cotransport SLC10A1 SLC10A2 SLC10A3 SLC10A4 SLC10A5 SLC10A6 SLC10A7 10A1 10A2 10A3 10A7

SLC11–20

(11):	proton coupled metal ion transporter SLC11A1 SLC11A2 11A3
(12):	electroneutral cation-Cl cotransporter SLC12A1 SLC12A2 SLC12A3 SLC12A4 SLC12A5 SLC12A6 SLC12A7 SLC12A8 SLC12A9
(13):	human Na⁺-sulfate/carboxylate cotransporter SLC13A1 SLC13A2 SLC13A3 SLC13A4 SLC13A5
(14):	urea transporter SLC14A1 SLC14A2
(15):	proton oligopeptide cotransporter SLC15A1 SLC15A2 SLC15A3 SLC15A4
(16):	monocarboxylate transporter SLC16A1 SLC16A2 SLC16A3 SLC16A4 SLC16A5 SLC16A6 SLC16A7 SLC16A8 SLC16A9 SLC16A10 SLC16A11 SLC16A12 SLC16A13 SLC16A14
(17):	Vesicular glutamate transporter 1 SLC17A1 SLC17A2 SLC17A3 SLC17A4 SLC17A5 SLC17A6 SLC17A7 SLC17A8 SLC17A9
(18):	vesicular monoamine transporter SLC18A1 SLC18A2 SLC18A3
(19):	folate/thiamine transporter SLC19A1 SLC19A2 SLC19A3
(20):	type III Na⁺-phosphate cotransporter SLC20A1 SLC20A2

SLC21–30

(21):	Organic anion-transporting polypeptide SLCO1A2 SLCO1B1 SLCO1B3 SLCO1B4 SLCO1C1 SLCO2A1 SLCO2B1 SLCO3A1 SLCO4A1 SLCO4C1 SLCO5A1(SLCO6A1)
(22):	organic cation/anion/zwitterion transporter SLC22A1 SLC22A2 SLC22A3 SLC22A4 SLC22A5 SLC22A6 SLC22A7 SLC22A8 SLC22A9 SLC22A10 SLC22A11 SLC22A12 SLC22A13 SLC22A14 SLC22A15 SLC22A16 SLC22A17 SLC22A18 SLC22A19 SLC22A20
(23):	Na+-dependent ascorbic acid transporter SLC23A1 SLC23A2 SLC23A3 SLC23A4
(24):	Na⁺/(Ca²⁺-K⁺) exchanger SLC24A1 SLC24A2 SLC24A3 SLC24A4 SLC24A5 SLC24A6
(25):	mitochondrial carrier SLC25A1 SLC25A2 SLC25A3 SLC25A4 SLC25A5 SLC25A6 SLC25A7 SLC25A8 SLC25A9 SLC25A10 SLC25A11 SLC25A12 SLC25A13 SLC25A14 SLC25A15 SLC25A16 SLC25A17 SLC25A18 SLC25A19 SLC25A20 SLC25A21 SLC25A22 SLC25A23 SLC25A24 SLC25A25 SLC25A26 SLC25A27 SLC25A28 SLC25A29 SLC25A30 SLC25A31 SLC25A32 SLC25A33 SLC25A34 SLC25A35 SLC25A36 SLC25A37 SLC25A38 SLC25A39 SLC25A40 SLC25A41 SLC25A42 SLC25A43 SLC25A44 SLC25A45 SLC25A46
(26):	multifunctional anion exchanger SLC26A1 SLC26A2 SLC26A3 SLC26A4 SLC26A5 SLC26A6 SLC26A7 SLC26A8 SLC26A9 SLC26A10 SLC26A11
(27):	fatty acid transport proteins SLC27A1 SLC27A2 SLC27A3 SLC27A4 SLC27A5 SLC27A6
(28):	Na⁺-coupled nucleoside transport (SLC28A1 SLC28A2 SLC28A3
(29):	facilitative nucleoside transporter SLC29A1 SLC29A2 SLC29A3 SLC29A4
(30):	zinc efflux SLC30A1 SLC30A2 SLC30A3 SLC30A4 SLC30A5 SLC30A6 SLC30A7 SLC30A8 SLC30A9 SLC30A10

SLC31–40

(31):	copper transporter SLC31A1
(32):	Vesicular glutamate transporter 1 SLC32A1
(33):	Acetyl-CoA transporter SLC33A1
(34):	type II Na⁺-phosphate cotransporter SLC34A1 SLC34A2 SLC34A3
(35):	nucleoside-sugar transporter SLC35A1 SLC35A2 SLC35A3 SLC35A4 SLC35A5 SLC35B1 SLC35B2 SLC35B3 SLC35B4 SLC35C1 SLC35C2 SLC35D1 SLC35D2 SLC35D3 SLC35E1 SLC35E2 SLC35E3 SLC35E4
(36):	proton-coupled amino-acid transporter SLC36A1 SLC36A2 SLC36A3 SLC36A436A2
(37):	sugar-phosphate/phosphate exchanger SLC37A1 SLC37A2 SLC37A3 SLC37A4
(38):	System A & N, sodium-coupled neutral amino-acid transporter SLC38A1 SLC38A2 SLC38A3 SLC38A4 SLC38A5 SLC38A6 SLC38A10
(39):	metal ion transporter SLC39A1 SLC39A2 SLC39A3 SLC39A4 SLC39A5 SLC39A6 SLC39A7 SLC39A8 SLC39A9 SLC39A10 SLC39A11 SLC39A12 SLC39A13 SLC39A14
(40):	basolateral iron transporter SLC40A1

SLC41–48

(41):	Magnesium transporter E SLC41A1 SLC41A2 SLC41A3
(42):	Ammonia transporter RhAG RhBG RhCG
(43):	Na⁺-independent, system-L like amino-acid transporter SLC43A1 SLC43A2 SLC43A3
(44):	Choline-like transporter SLC44A1 SLC44A2 SLC44A3 SLC44A4 SLC44A5
(45):	Putative sugar transporter SLC45A1 SLC45A2 SLC54A3 SLC45A4
(46):	Folate transporter SLC46A1 SLC46A2
(47):	multidrug and toxin extrusion SLC47A1 SLC47A2
(48):	Heme transporter

SLCO1–4
O1A2 O1B1 O1B3 O2B1 O431 O4A1

Ion pumps

Symporter, Cotransporter	Na⁺/K⁺,Cl⁻ Na⁺/P_i3 Na⁺/Cl⁻ Na⁺/glucose Na⁺/I⁻ Cl⁻/K⁺ 4 5
Antiporter (exchanger)	Na⁺/H⁺ Na⁺/Ca²⁺ Na⁺/(Ca²⁺-K⁺) - Cl⁻/HCO⁻ ₃ (Band 3) Cl⁻-formate Cl⁻-oxalate