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Latest revision as of 17:37, 13 June 2018

Hexokinase-1 (HK1) is an enzyme that in humans is encoded by the HK1 gene on chromosome 10. Hexokinases phosphorylate glucose to produce glucose-6-phosphate (G6P), the first step in most glucose metabolism pathways. This gene encodes a ubiquitous form of hexokinase which localizes to the outer membrane of mitochondria. Mutations in this gene have been associated with hemolytic anemia due to hexokinase deficiency. Alternative splicing of this gene results in five transcript variants which encode different isoforms, some of which are tissue-specific. Each isoform has a distinct N-terminus; the remainder of the protein is identical among all the isoforms. A sixth transcript variant has been described, but due to the presence of several stop codons, it is not thought to encode a protein. [provided by RefSeq, Apr 2009]^[1]

Structure

HK1 is one of four highly homologous hexokinase isoforms in mammalian cells.^[2]^[3]

Gene

The HK1 gene spans approximately 131 kb and consists of 25 exons. Alternative splicing of its 5’ exons produces different transcripts in different cell types: exons 1-5 and exon 8 (exons T1-6) are testis-specific exons; exon 6, located approximately 15 kb downstream of the testis-specific exons, is the erythroid-specific exon (exon R); and exon 7, located approximately 2.85 kb downstream of exon R, is the first 5’ exon for the ubiquitously expressed HK1 isoform. Moreover, exon 7 encodes the porin-binding domain (PBD) conserved in mammalian HK1 genes. Meanwhile, the remaining 17 exons are shared among all HK1 isoforms.

In addition to exon R, a stretch of the proximal promoter that contains a GATA element, an SP1 site, CCAAT, and an Ets-binding motif is necessary for expression of HK-R in erythroid cells.^[2]

Protein

This gene encodes a 100 kDa homodimer with a regulatory N-terminal domain (1-475), catalytic C-terminal domain (residues 476-917), and an alpha-helix connecting its two subunits.^[2]^[4]^[5]^[6] Both terminal domains are composed of a large subdomain and a small subdomain. The flexible region of the C-terminal large subdomain (residues 766–810) can adopt various positions and is proposed to interact with the base of ATP. Moreover, glucose and G6P bind in close proximity at the N- and C-terminal domains and stabilize a common conformational state of the C-terminal domain.^[4]^[5] According to one model, G6P acts as an allosteric inhibitor which binds the N-terminal domain to stabilize its closed conformation, which then stabilizes a conformation of the C-terminal flexible subdomain that blocks ATP. A second model posits that G6P acts as an active inhibitor that stabilizes the closed conformation and competes with ATP for the C-terminal binding site.^[4] Results from several studies suggest that the C-terminal is capable of both catalytic and regulatory action.^[7] Meanwhile, the hydrophobic N-terminal lacks enzymatic activity by itself but contains the G6P regulatory site and the PBD, which is responsible for the protein’s stability and binding to the outer mitochondrial membrane (OMM).^[2]^[8]^[6]^[9]

Function

As one of two mitochondrial isoforms of hexokinase and a member of the sugar kinase family, HK1 catalyzes the rate-limiting and first obligatory step of glucose metabolism, which is the ATP-dependent phosphorylation of glucose to G6P.^[4]^[3]^[6]^[10] Physiological levels of G6P can regulate this process by inhibiting HK1 as negative feedback, though inorganic phosphate (P_i) can relieve G6P inhibition.^[4]^[8]^[6] However, unlike HK2 and HK3, HK1 itself is not directly regulated by P_i, which better suits its ubiquitous catabolic role.^[3] By phosphorylating glucose, HK1 effectively prevents glucose from leaving the cell and, thus, commits glucose to energy metabolism.^[4]^[9]^[8]^[6] Moreover, its localization and attachment to the OMM promotes the coupling of glycolysis to mitochondrial oxidative phosphorylation, which greatly enhances ATP production by direct recycling of mitochondrial ATP/ADP to meet the cell’s energy demands.^[10]^[6]^[11] Specifically, OMM-bound HK1 binds VDAC1 to trigger opening of the mitochondrial permeability transition pore and release mitochondrial ATP to further fuel the glycolytic process.^[6]^[3]

Another critical function for OMM-bound HK1 is cell survival and protection against oxidative damage.^[10]^[3] Activation of Akt kinase is mediated by HK1-VDAC1 coupling as part of the growth factor-mediated phosphatidyl inositol 3-kinase (PI3)/Akt cell survival intracellular signaling pathway, thus preventing cytochrome c release and subsequent apoptosis.^[10]^[2]^[6]^[3] In fact, there is evidence that VDAC binding by the anti-apoptotic HK1 and by the pro-apoptotic creatine kinase are mutually exclusive, indicating that the absence of HK1 allows creatine kinase to bind and open VDAC.^[3] Furthermore, HK1 has demonstrated anti-apoptotic activity by antagonizing Bcl-2 proteins located at the OMM, which then inhibits TNF-induced apoptosis.^[2]^[9]

In the prefrontal cortex, HK1 putatively forms a protein complex with EAAT2, Na+/K+ ATPase, and aconitase, which functions to remove glutamate from the perisynaptic space and maintain low basal levels in the synaptic cleft.^[11]

In particular, HK1 is the most ubiquitously expressed isoform out of the four hexokinases, and constitutively expressed in most tissues, though it is majorly found in brain, kidney, and red blood cells (RBCs).^[2]^[4]^[9]^[3]^[11]^[6]^[12] Its high abundance in the retina, specifically the photoreceptor inner segment, outer plexiform layer, inner nuclear layer, inner plexiform layer, and ganglion cell layer, attests to its crucial metabolic purpose.^[13] It is also expressed in cells derived from hematopoietic stem cells, such as RBCs, leukocytes, and platelets, as well as from erythroid-progenitor cells.^[2] Of note, HK1 is the sole hexokinase isoform found in the cells and tissues which rely most heavily on glucose metabolism for their function, including brain, erythrocytes, platelets, leukocytes, and fibroblasts.^[14] In rats, it is also the predominant hexokinase in fetal tissues, likely due to their constitutive glucose utilization.^[8]^[12]

Clinical significance

Mutations in this gene are associated with type 4H of Charcot–Marie–Tooth disease, also known as Russe-type hereditary motor and sensory neuropathy (HMSNR).^[15] Due to the crucial role of HK1 in glycolysis, hexokinase deficiency has been identified as a cause of erythroenzymopathies associated with hereditary non-spherocytic hemolytic anemia (HNSHA). Likewise, HK1 deficiency has resulted in cerebral white matter injury, malformations, and psychomotor retardation, as well as latent diabetes mellitus and panmyelopathy.^[2] Meanwhile, HK1 is highly expressed in cancers, and its anti-apoptotic effects have been observed in highly glycolytic hepatoma cells.^[9]^[2]

Neurodegenerative disorders

HK1 may be causally linked to mood and psychotic disorders, including unipolar depression (UPD), bipolar disorder (BPD), and schizophrenia via both its roles in energy metabolism and cell survival. For instance, the accumulation of lactate in the brains of BPD and SCHZ patients potentially results from the decoupling of HK1 from the OMM, and by extension, glycolysis from mitochondrial oxidative, phosphorylation. In the case of SCHZ, decreasing HK1 attachment to the OMM in the parietal cortex resulted in decreased glutamate reuptake capacity and, thus, glutamate spillover from the synapses. The released glutamate activates extrasynaptic glutamate receptors, leading to altered structure and function of glutamate circuits, synaptic plasticity, frontal cortical dysfunction, and ultimately, the cognitive deficits characteristic of SCHZ.^[11] Similarly, Hk1 mitochondrial detachment has been associated with hypothyroidism, which involves abnormal brain development and increased risk for depression, while its attachment leads to neural growth.^[10] In Parkinson’s disease, HK1 detachment from VDAC via Parkin-mediated ubiquitylation and degradation disrupts the MPTP on depolarized mitochondria, consequently blocking mitochondrial localization of Parkin and halting glycolysis.^[3] Further research is required to determine the relative HK1 detachment needed in various cell types for different psychiatric disorders. This research can also contribute to developing therapies to target causes of the detachment, from gene mutations to interference by factors such as beta-amyloid peptide and insulin.^[10]

Retinitis pigmentosa

A heterozygous missense mutation in the HK1 gene (a change at position 847 from glutamate to lysine) has been linked to retinitis pigmentosa.^[16]^[13] Since this substitution mutation is located far from known functional sites and does not impair the enzyme’s glycolytic activity, it is likely that the mutation acts through another biological mechanism unique to the retina.^[16] Notably, studies in mouse retina reveal interactions between Hk1, the mitochondrial metallochaperone Cox11, and the chaperone protein Ranbp2, which serve to maintain normal metabolism and function in the retina. Thus, the mutation may disrupt these interactions and lead to retinal degradation.^[13] Alternatively, this mutation may act through the enzyme’s anti-apoptotic function, as disrupting the regulation of the hexokinase-mitochondria association by insulin receptors could trigger photoreceptor apoptosis and retinal degeneration.^[16]^[13] In this case, treatments that preserve the hexokinase–mitochondria association may serve as a potential therapeutic approach.^[13]

Interactions

HK1 is known to interact with:

Interactive pathway map

Click on genes, proteins and metabolites below to link to respective articles. ^{[§ 1]}

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|{{{bSize}}}px|alt=Glycolysis and Gluconeogenesis edit]]

Glycolysis and Gluconeogenesis edit

↑ The interactive pathway map can be edited at WikiPathways: "GlycolysisGluconeogenesis_WP534".

References

↑ "Entrez Gene: HK1 hexokinase 1".
↑ ^2.0 ^2.1 ^2.2 ^2.3 ^2.4 ^2.5 ^2.6 ^2.7 ^2.8 ^2.9 Murakami K, Kanno H, Tancabelic J, Fujii H (2002). "Gene expression and biological significance of hexokinase in erythroid cells". Acta Haematologica. 108 (4): 204–9. doi:10.1159/000065656. PMID 12432216.
↑ ^3.00 ^3.01 ^3.02 ^3.03 ^3.04 ^3.05 ^3.06 ^3.07 ^3.08 ^3.09 ^3.10 Okatsu K, Iemura S, Koyano F, Go E, Kimura M, Natsume T, Tanaka K, Matsuda N (Nov 2012). "Mitochondrial hexokinase HKI is a novel substrate of the Parkin ubiquitin ligase". Biochemical and Biophysical Research Communications. 428 (1): 197–202. doi:10.1016/j.bbrc.2012.10.041. PMID 23068103.
↑ ^4.0 ^4.1 ^4.2 ^4.3 ^4.4 ^4.5 ^4.6 Aleshin AE, Zeng C, Bourenkov GP, Bartunik HD, Fromm HJ, Honzatko RB (Jan 1998). "The mechanism of regulation of hexokinase: new insights from the crystal structure of recombinant human brain hexokinase complexed with glucose and glucose-6-phosphate". Structure. 6 (1): 39–50. doi:10.1016/s0969-2126(98)00006-9. PMID 9493266.
↑ ^5.0 ^5.1 Aleshin AE, Kirby C, Liu X, Bourenkov GP, Bartunik HD, Fromm HJ, Honzatko RB (Mar 2000). "Crystal structures of mutant monomeric hexokinase I reveal multiple ADP binding sites and conformational changes relevant to allosteric regulation". Journal of Molecular Biology. 296 (4): 1001–15. doi:10.1006/jmbi.1999.3494. PMID 10686099.
↑ ^6.0 ^6.1 ^6.2 ^6.3 ^6.4 ^6.5 ^6.6 ^6.7 ^6.8 Robey RB, Hay N (Aug 2006). "Mitochondrial hexokinases, novel mediators of the antiapoptotic effects of growth factors and Akt". Oncogene. 25 (34): 4683–96. doi:10.1038/sj.onc.1209595. PMID 16892082.
↑ Cárdenas, ML; Cornish-Bowden, A; Ureta, T (5 March 1998). "Evolution and regulatory role of the hexokinases". Biochimica et Biophysica Acta. 1401 (3): 242–64. doi:10.1016/s0167-4889(97)00150-x. PMID 9540816.
↑ ^8.0 ^8.1 ^8.2 ^8.3 Printz RL, Osawa H, Ardehali H, Koch S, Granner DK (Feb 1997). "Hexokinase II gene: structure, regulation and promoter organization". Biochemical Society Transactions. 25 (1): 107–12. doi:10.1042/bst0250107. PMID 9056853.
↑ ^9.0 ^9.1 ^9.2 ^9.3 ^9.4 Schindler A, Foley E (Dec 2013). "Hexokinase 1 blocks apoptotic signals at the mitochondria". Cellular Signalling. 25 (12): 2685–92. doi:10.1016/j.cellsig.2013.08.035. PMID 24018046.
↑ ^10.0 ^10.1 ^10.2 ^10.3 ^10.4 ^10.5 Regenold WT, Pratt M, Nekkalapu S, Shapiro PS, Kristian T, Fiskum G (Jan 2012). "Mitochondrial detachment of hexokinase 1 in mood and psychotic disorders: implications for brain energy metabolism and neurotrophic signaling". Journal of Psychiatric Research. 46 (1): 95–104. doi:10.1016/j.jpsychires.2011.09.018. PMID 22018957.
↑ ^11.0 ^11.1 ^11.2 ^11.3 ^11.4 ^11.5 ^11.6 Shan D, Mount D, Moore S, Haroutunian V, Meador-Woodruff JH, McCullumsmith RE (Apr 2014). "Abnormal partitioning of hexokinase 1 suggests disruption of a glutamate transport protein complex in schizophrenia". Schizophrenia Research. 154 (1–3): 1–13. doi:10.1016/j.schres.2014.01.028. PMC 4151500. PMID 24560881.
↑ ^12.0 ^12.1 Reid, S; Masters, C (1985). "On the developmental properties and tissue interactions of hexokinase". Mechanisms of ageing and development. 31 (2): 197–212. doi:10.1016/s0047-6374(85)80030-0. PMID 4058069.
↑ ^13.0 ^13.1 ^13.2 ^13.3 ^13.4 Wang F, Wang Y, Zhang B, Zhao L, Lyubasyuk V, Wang K, Xu M, Li Y, Wu F, Wen C, Bernstein PS, Lin D, Zhu S, Wang H, Zhang K, Chen R (Nov 2014). "A missense mutation in HK1 leads to autosomal dominant retinitis pigmentosa". Investigative Ophthalmology & Visual Science. 55 (11): 7159–64. doi:10.1167/iovs.14-15520. PMC 4224578. PMID 25316723.
↑ Gjesing AP, Nielsen AA, Brandslund I, Christensen C, Sandbæk A, Jørgensen T, Witte D, Bonnefond A, Froguel P, Hansen T, Pedersen O (25 July 2011). "Studies of a genetic variant in HK1 in relation to quantitative metabolic traits and to the prevalence of type 2 diabetes". BMC Medical Genetics. 12: 99. doi:10.1186/1471-2350-12-99. PMC 3161933. PMID 21781351.
↑ Online Mendelian Inheritance in Man (OMIM) 605285
↑ ^16.0 ^16.1 ^16.2 Sullivan LS, Koboldt DC, Bowne SJ, Lang S, Blanton SH, Cadena E, Avery CE, Lewis RA, Webb-Jones K, Wheaton DH, Birch DG, Coussa R, Ren H, Lopez I, Chakarova C, Koenekoop RK, Garcia CA, Fulton RS, Wilson RK, Weinstock GM, Daiger SP (Nov 2014). "A dominant mutation in hexokinase 1 (HK1) causes retinitis pigmentosa". Investigative Ophthalmology & Visual Science. 55 (11): 7147–58. doi:10.1167/iovs.14-15419. PMC 4224580. PMID 25190649.

Daniele A, Altruda F, Ferrone M, Silengo L, Romeo G, Archidiacono N, Rocchi M (1992). "Mapping of human hexokinase 1 gene to 10q11----qter". Human Heredity. 42 (2): 107–10. doi:10.1159/000154049. PMID 1572668.
Magnani M, Bianchi M, Casabianca A, Stocchi V, Daniele A, Altruda F, Ferrone M, Silengo L (Jul 1992). "A recombinant human 'mini'-hexokinase is catalytically active and regulated by hexose 6-phosphates". The Biochemical Journal. 285 (1): 193–9. doi:10.1042/bj2850193. PMC 1132765. PMID 1637300.
Magnani M, Serafini G, Bianchi M, Casabianca A, Stocchi V (Jan 1991). "Human hexokinase type I microheterogeneity is due to different amino-terminal sequences". The Journal of Biological Chemistry. 266 (1): 502–5. PMID 1985912.
Adams V, Griffin LD, Gelb BD, McCabe ER (Jun 1991). "Protein kinase activity of rat brain hexokinase". Biochemical and Biophysical Research Communications. 177 (3): 1101–6. doi:10.1016/0006-291X(91)90652-N. PMID 2059200.
Murakami K, Blei F, Tilton W, Seaman C, Piomelli S (Feb 1990). "An isozyme of hexokinase specific for the human red blood cell (HKR)". Blood. 75 (3): 770–5. PMID 2297576.
Nishi S, Seino S, Bell GI (Dec 1988). "Human hexokinase: sequences of amino- and carboxyl-terminal halves are homologous". Biochemical and Biophysical Research Communications. 157 (3): 937–43. doi:10.1016/S0006-291X(88)80964-1. PMID 3207429.
Rijksen G, Akkerman JW, van den Wall Bake AW, Hofstede DP, Staal GE (Jan 1983). "Generalized hexokinase deficiency in the blood cells of a patient with nonspherocytic hemolytic anemia". Blood. 61 (1): 12–8. PMID 6848140.
Bianchi M, Magnani M (1995). "Hexokinase mutations that produce nonspherocytic hemolytic anemia". Blood Cells, Molecules & Diseases. 21 (1): 2–8. doi:10.1006/bcmd.1995.0002. PMID 7655856.
Blachly-Dyson E, Zambronicz EB, Yu WH, Adams V, McCabe ER, Adelman J, Colombini M, Forte M (Jan 1993). "Cloning and functional expression in yeast of two human isoforms of the outer mitochondrial membrane channel, the voltage-dependent anion channel". The Journal of Biological Chemistry. 268 (3): 1835–41. PMID 8420959.
Aleshin AE, Zeng C, Fromm HJ, Honzatko RB (Aug 1996). "Crystallization and preliminary X-ray analysis of human brain hexokinase". FEBS Letters. 391 (1–2): 9–10. doi:10.1016/0014-5793(96)00688-6. PMID 8706938.
Visconti PE, Olds-Clarke P, Moss SB, Kalab P, Travis AJ, de las Heras M, Kopf GS (Jan 1996). "Properties and localization of a tyrosine phosphorylated form of hexokinase in mouse sperm". Molecular Reproduction and Development. 43 (1): 82–93. doi:10.1002/(SICI)1098-2795(199601)43:1<82::AID-MRD11>3.0.CO;2-6. PMID 8720117.
Mori C, Nakamura N, Welch JE, Shiota K, Eddy EM (May 1996). "Testis-specific expression of mRNAs for a unique human type 1 hexokinase lacking the porin-binding domain". Molecular Reproduction and Development. 44 (1): 14–22. doi:10.1002/(SICI)1098-2795(199605)44:1<14::AID-MRD2>3.0.CO;2-W. PMID 8722688.
Murakami K, Piomelli S (Feb 1997). "Identification of the cDNA for human red blood cell-specific hexokinase isozyme". Blood. 89 (3): 762–6. PMID 9028305.
Ruzzo A, Andreoni F, Magnani M (Jan 1998). "An erythroid-specific exon is present in the human hexokinase gene". Blood. 91 (1): 363–4. PMID 9414310.
Travis AJ, Foster JA, Rosenbaum NA, Visconti PE, Gerton GL, Kopf GS, Moss SB (Feb 1998). "Targeting of a germ cell-specific type 1 hexokinase lacking a porin-binding domain to the mitochondria as well as to the head and fibrous sheath of murine spermatozoa". Molecular Biology of the Cell. 9 (2): 263–76. doi:10.1091/mbc.9.2.263. PMC 25249. PMID 9450953.
Aleshin AE, Zeng C, Bourenkov GP, Bartunik HD, Fromm HJ, Honzatko RB (Jan 1998). "The mechanism of regulation of hexokinase: new insights from the crystal structure of recombinant human brain hexokinase complexed with glucose and glucose-6-phosphate". Structure. 6 (1): 39–50. doi:10.1016/S0969-2126(98)00006-9. PMID 9493266.
Ruzzo A, Andreoni F, Magnani M (Apr 1998). "Structure of the human hexokinase type I gene and nucleotide sequence of the 5' flanking region". The Biochemical Journal. 331 (2): 607–13. doi:10.1042/bj3310607. PMC 1219395. PMID 9531504.
Aleshin AE, Zeng C, Bartunik HD, Fromm HJ, Honzatko RB (Sep 1998). "Regulation of hexokinase I: crystal structure of recombinant human brain hexokinase complexed with glucose and phosphate". Journal of Molecular Biology. 282 (2): 345–57. doi:10.1006/jmbi.1998.2017. PMID 9735292.
Murakami K, Kanno H, Miwa S, Piomelli S (Jun 1999). "Human HKR isozyme: organization of the hexokinase I gene, the erythroid-specific promoter, and transcription initiation site". Molecular Genetics and Metabolism. 67 (2): 118–30. doi:10.1006/mgme.1999.2842. PMID 10356311.

[WikiPathways-17] The interactive pathway map can be edited at WikiPathways: "GlycolysisGluconeogenesis_WP534".

[entrez-1] "Entrez Gene: HK1 hexokinase 1".

[pmid12432216-2] 2.0 ^2.1 ^2.2 ^2.3 ^2.4 ^2.5 ^2.6 ^2.7 ^2.8 ^2.9 Murakami K, Kanno H, Tancabelic J, Fujii H (2002). "Gene expression and biological significance of hexokinase in erythroid cells". Acta Haematologica. 108 (4): 204–9. doi:10.1159/000065656. PMID 12432216.

[pmid23068103-3] 3.00 ^3.01 ^3.02 ^3.03 ^3.04 ^3.05 ^3.06 ^3.07 ^3.08 ^3.09 ^3.10 Okatsu K, Iemura S, Koyano F, Go E, Kimura M, Natsume T, Tanaka K, Matsuda N (Nov 2012). "Mitochondrial hexokinase HKI is a novel substrate of the Parkin ubiquitin ligase". Biochemical and Biophysical Research Communications. 428 (1): 197–202. doi:10.1016/j.bbrc.2012.10.041. PMID 23068103.

[pmid9493266-4] 4.0 ^4.1 ^4.2 ^4.3 ^4.4 ^4.5 ^4.6 Aleshin AE, Zeng C, Bourenkov GP, Bartunik HD, Fromm HJ, Honzatko RB (Jan 1998). "The mechanism of regulation of hexokinase: new insights from the crystal structure of recombinant human brain hexokinase complexed with glucose and glucose-6-phosphate". Structure. 6 (1): 39–50. doi:10.1016/s0969-2126(98)00006-9. PMID 9493266.

[pmid10686099-5] 5.0 ^5.1 Aleshin AE, Kirby C, Liu X, Bourenkov GP, Bartunik HD, Fromm HJ, Honzatko RB (Mar 2000). "Crystal structures of mutant monomeric hexokinase I reveal multiple ADP binding sites and conformational changes relevant to allosteric regulation". Journal of Molecular Biology. 296 (4): 1001–15. doi:10.1006/jmbi.1999.3494. PMID 10686099.

[pmid16892082-6] 6.0 ^6.1 ^6.2 ^6.3 ^6.4 ^6.5 ^6.6 ^6.7 ^6.8 Robey RB, Hay N (Aug 2006). "Mitochondrial hexokinases, novel mediators of the antiapoptotic effects of growth factors and Akt". Oncogene. 25 (34): 4683–96. doi:10.1038/sj.onc.1209595. PMID 16892082.

[pmid9540816-7] Cárdenas, ML; Cornish-Bowden, A; Ureta, T (5 March 1998). "Evolution and regulatory role of the hexokinases". Biochimica et Biophysica Acta. 1401 (3): 242–64. doi:10.1016/s0167-4889(97)00150-x. PMID 9540816.

[pmid9056853-8] 8.0 ^8.1 ^8.2 ^8.3 Printz RL, Osawa H, Ardehali H, Koch S, Granner DK (Feb 1997). "Hexokinase II gene: structure, regulation and promoter organization". Biochemical Society Transactions. 25 (1): 107–12. doi:10.1042/bst0250107. PMID 9056853.

[pmid24018046-9] 9.0 ^9.1 ^9.2 ^9.3 ^9.4 Schindler A, Foley E (Dec 2013). "Hexokinase 1 blocks apoptotic signals at the mitochondria". Cellular Signalling. 25 (12): 2685–92. doi:10.1016/j.cellsig.2013.08.035. PMID 24018046.

[pmid22018957-10] 10.0 ^10.1 ^10.2 ^10.3 ^10.4 ^10.5 Regenold WT, Pratt M, Nekkalapu S, Shapiro PS, Kristian T, Fiskum G (Jan 2012). "Mitochondrial detachment of hexokinase 1 in mood and psychotic disorders: implications for brain energy metabolism and neurotrophic signaling". Journal of Psychiatric Research. 46 (1): 95–104. doi:10.1016/j.jpsychires.2011.09.018. PMID 22018957.

[pmid24560881-11] 11.0 ^11.1 ^11.2 ^11.3 ^11.4 ^11.5 ^11.6 Shan D, Mount D, Moore S, Haroutunian V, Meador-Woodruff JH, McCullumsmith RE (Apr 2014). "Abnormal partitioning of hexokinase 1 suggests disruption of a glutamate transport protein complex in schizophrenia". Schizophrenia Research. 154 (1–3): 1–13. doi:10.1016/j.schres.2014.01.028. PMC 4151500. PMID 24560881.

[pmid4058069-12] 12.0 ^12.1 Reid, S; Masters, C (1985). "On the developmental properties and tissue interactions of hexokinase". Mechanisms of ageing and development. 31 (2): 197–212. doi:10.1016/s0047-6374(85)80030-0. PMID 4058069.

[pmid25316723-13] 13.0 ^13.1 ^13.2 ^13.3 ^13.4 Wang F, Wang Y, Zhang B, Zhao L, Lyubasyuk V, Wang K, Xu M, Li Y, Wu F, Wen C, Bernstein PS, Lin D, Zhu S, Wang H, Zhang K, Chen R (Nov 2014). "A missense mutation in HK1 leads to autosomal dominant retinitis pigmentosa". Investigative Ophthalmology & Visual Science. 55 (11): 7159–64. doi:10.1167/iovs.14-15520. PMC 4224578. PMID 25316723.

[pmid21781351-14] Gjesing AP, Nielsen AA, Brandslund I, Christensen C, Sandbæk A, Jørgensen T, Witte D, Bonnefond A, Froguel P, Hansen T, Pedersen O (25 July 2011). "Studies of a genetic variant in HK1 in relation to quantitative metabolic traits and to the prevalence of type 2 diabetes". BMC Medical Genetics. 12: 99. doi:10.1186/1471-2350-12-99. PMC 3161933. PMID 21781351.

[15] Online Mendelian Inheritance in Man (OMIM) 605285

[pmid25190649-16] 16.0 ^16.1 ^16.2 Sullivan LS, Koboldt DC, Bowne SJ, Lang S, Blanton SH, Cadena E, Avery CE, Lewis RA, Webb-Jones K, Wheaton DH, Birch DG, Coussa R, Ren H, Lopez I, Chakarova C, Koenekoop RK, Garcia CA, Fulton RS, Wilson RK, Weinstock GM, Daiger SP (Nov 2014). "A dominant mutation in hexokinase 1 (HK1) causes retinitis pigmentosa". Investigative Ophthalmology & Visual Science. 55 (11): 7147–58. doi:10.1167/iovs.14-15419. PMC 4224580. PMID 25190649.

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[§ 1]

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+{{Infobox_gene}}
-{{SI}}
+'''Hexokinase-1''' (HK1) is an [[enzyme]] that in humans is encoded by the ''HK1'' [[gene]] on chromosome 10. [[Hexokinase]]s [[phosphorylate]] [[glucose]] to produce [[glucose-6-phosphate]] (G6P), the first step in most glucose metabolism pathways. This gene encodes a ubiquitous form of hexokinase which localizes to the [[outer mitochondrial membrane|outer membrane of mitochondria]]. Mutations in this gene have been associated with [[hemolytic anemia]] due to hexokinase deficiency. [[Alternative splicing]] of this gene results in five transcript variants which encode different [[isoform]]s, some of which are tissue-specific. Each isoform has a distinct [[N-terminal|N-terminus]]; the remainder of the protein is identical among all the isoforms. A sixth transcript variant has been described, but due to the presence of several [[stop codon]]s, it is not thought to encode a protein. [provided by RefSeq, Apr 2009]<ref name="entrez">{{cite web | title = Entrez Gene: HK1 hexokinase 1| url = https://www.ncbi.nlm.nih.gov/sites/entrez?Db=gene&Cmd=ShowDetailView&TermToSearch=3098| accessdate = }}</ref>
-{{EH}}
+== Structure ==
-'''Hexokinase 1''', also known as '''HK1''', is a human [[gene]].
+HK1 is one of four highly homologous hexokinase isoforms in mammalian cells.<ref name=pmid12432216>{{cite journal | vauthors = Murakami K, Kanno H, Tancabelic J, Fujii H | title = Gene expression and biological significance of hexokinase in erythroid cells | journal = Acta Haematologica | volume = 108 | issue = 4 | pages = 204–9 | date = 2002 | pmid = 12432216 | doi = 10.1159/000065656 }}</ref><ref name=pmid23068103>{{cite journal | vauthors = Okatsu K, Iemura S, Koyano F, Go E, Kimura M, Natsume T, Tanaka K, Matsuda N | title = Mitochondrial hexokinase HKI is a novel substrate of the Parkin ubiquitin ligase | journal = Biochemical and Biophysical Research Communications | volume = 428 | issue = 1 | pages = 197–202 | date = Nov 2012 | pmid = 23068103 | doi = 10.1016/j.bbrc.2012.10.041 }}</ref>
-<!-- The PBB_Summary template is automatically maintained by Protein Box Bot.  See Template:PBB_Controls to Stop updates. -->
-{{PBB_Summary
-| section_title =
-| summary_text = Hexokinases phosphorylate glucose to produce glucose-6-phosphate, thus committing glucose to the glycolytic pathway. This gene encodes a ubiquitous form of hexokinase which localizes to the outer membrane of mitochondria. Mutations in this gene have been associated with hemolytic anemia due to hexokinase deficiency. Alternative splicing of this gene results in five transcript variants which encode different isoforms, some of which are tissue-specific. Each isoform has a distinct N-terminus; the remainder of the protein is identical among all the isoforms. A sixth transcript variant has been described, but due to the presence of several stop codons, it is not thought to encode a protein.<ref name="entrez">{{cite web | title = Entrez Gene: HK1 hexokinase 1| url = http://www.ncbi.nlm.nih.gov/sites/entrez?Db=gene&Cmd=ShowDetailView&TermToSearch=3098| accessdate = }}</ref>
-}}
-==References==
+=== Gene ===
-{{reflist}}
-==Further reading==
+The ''HK1'' gene spans approximately 131 [[kilobase|kb]] and consists of 25 [[exon]]s. [[Alternative splicing]] of its 5’ exons produces different transcripts in different cell types: exons 1-5 and exon 8 (exons T1-6) are testis-specific exons; exon 6, located approximately 15 kb downstream of the testis-specific exons, is the [[erythroid]]-specific exon (exon R); and exon 7, located approximately 2.85 kb downstream of exon R, is the first 5’ exon for the ubiquitously expressed HK1 isoform. Moreover, exon 7 encodes the porin-binding domain (PBD) conserved in mammalian ''HK1'' genes. Meanwhile, the remaining 17 exons are shared among all HK1 isoforms.
-{{refbegin | 2}}
-{{PBB_Further_reading
+In addition to exon R, a stretch of the proximal [[promoter (genetics)|promoter]] that contains a GATA element, an SP1 site, CCAAT, and an Ets-binding motif is necessary for expression of HK-R in erythroid cells.<ref name=pmid12432216/>
-| citations =
-*{{cite journal  | author=Murakami K, Kanno H, Tancabelic J, Fujii H |title=Gene expression and biological significance of hexokinase in erythroid cells. |journal=Acta Haematol. |volume=108 |issue= 4 |pages= 204–9 |year= 2003 |pmid= 12432216 |doi=  }}
+=== Protein ===
-*{{cite journal  | author=Daniele A, Altruda F, Ferrone M, ''et al.'' |title=Mapping of human hexokinase 1 gene to 10q11----qter. |journal=Hum. Hered. |volume=42 |issue= 2 |pages= 107–10 |year= 1992 |pmid= 1572668 |doi=  }}
-*{{cite journal  | author=Magnani M, Bianchi M, Casabianca A, ''et al.'' |title=A recombinant human 'mini'-hexokinase is catalytically active and regulated by hexose 6-phosphates. |journal=Biochem. J. |volume=285 ( Pt 1) |issue=  |pages= 193–9 |year= 1992 |pmid= 1637300 |doi=  }}
+This gene encodes a 100 kDa [[homodimer]] with a regulatory [[N-terminal]] domain (1-475), [[catalytic]] [[C-terminal]] domain (residues 476-917), and an [[alpha-helix]] connecting its two subunits.<ref name=pmid12432216/><ref name=pmid9493266>{{cite journal | vauthors = Aleshin AE, Zeng C, Bourenkov GP, Bartunik HD, Fromm HJ, Honzatko RB | title = The mechanism of regulation of hexokinase: new insights from the crystal structure of recombinant human brain hexokinase complexed with glucose and glucose-6-phosphate | journal = Structure | volume = 6 | issue = 1 | pages = 39–50 | date = Jan 1998 | pmid = 9493266 | doi=10.1016/s0969-2126(98)00006-9}}</ref><ref name=pmid10686099>{{cite journal | vauthors = Aleshin AE, Kirby C, Liu X, Bourenkov GP, Bartunik HD, Fromm HJ, Honzatko RB | title = Crystal structures of mutant monomeric hexokinase I reveal multiple ADP binding sites and conformational changes relevant to allosteric regulation | journal = Journal of Molecular Biology | volume = 296 | issue = 4 | pages = 1001–15 | date = Mar 2000 | pmid = 10686099 | doi = 10.1006/jmbi.1999.3494 }}</ref><ref name=pmid16892082>{{cite journal | vauthors = Robey RB, Hay N | title = Mitochondrial hexokinases, novel mediators of the antiapoptotic effects of growth factors and Akt | journal = Oncogene | volume = 25 | issue = 34 | pages = 4683–96 | date = Aug 2006 | pmid = 16892082 | doi = 10.1038/sj.onc.1209595 }}</ref> Both terminal domains are composed of a large subdomain and a small subdomain. The flexible region of the C-terminal large subdomain ([[amino acid|residues]] 766–810) can adopt various positions and is proposed to interact with the [[Base (chemistry)|base]] of ATP. Moreover, glucose and G6P bind in close proximity at the N- and C-terminal domains and stabilize a common conformational state of the C-terminal domain.<ref name=pmid9493266/><ref name=pmid10686099/> According to one model, G6P acts as an [[allosteric]] inhibitor which binds the N-terminal domain to stabilize its closed conformation, which then stabilizes a conformation of the C-terminal flexible subdomain that blocks ATP. A second model posits that G6P acts as an active inhibitor that stabilizes the closed conformation and competes with ATP for the C-terminal binding site.<ref name=pmid9493266/> Results from several studies suggest that the C-terminal is capable of both catalytic and regulatory action.<ref name=pmid9540816>{{cite journal|last1=Cárdenas|first1=ML|last2=Cornish-Bowden|first2=A|last3=Ureta|first3=T|title=Evolution and regulatory role of the hexokinases.|journal=Biochimica et Biophysica Acta|date=5 March 1998|volume=1401|issue=3|pages=242–64|pmid=9540816|doi=10.1016/s0167-4889(97)00150-x}}</ref> Meanwhile, the hydrophobic N-terminal lacks enzymatic activity by itself but contains the G6P regulatory site and the PBD, which is responsible for the protein’s stability and binding to the  [[outer mitochondrial membrane]] (OMM).<ref name=pmid12432216/><ref name=pmid9056853>{{cite journal | vauthors = Printz RL, Osawa H, Ardehali H, Koch S, Granner DK | title = Hexokinase II gene: structure, regulation and promoter organization | journal = Biochemical Society Transactions | volume = 25 | issue = 1 | pages = 107–12 | date = Feb 1997 | pmid = 9056853 | doi=10.1042/bst0250107}}</ref><ref name=pmid16892082/><ref name=pmid24018046>{{cite journal | vauthors = Schindler A, Foley E | title = Hexokinase 1 blocks apoptotic signals at the mitochondria | journal = Cellular Signalling | volume = 25 | issue = 12 | pages = 2685–92 | date = Dec 2013 | pmid = 24018046 | doi = 10.1016/j.cellsig.2013.08.035 }}</ref>
-*{{cite journal  | author=Magnani M, Serafini G, Bianchi M, ''et al.'' |title=Human hexokinase type I microheterogeneity is due to different amino-terminal sequences. |journal=J. Biol. Chem. |volume=266 |issue= 1 |pages= 502–5 |year= 1991 |pmid= 1985912 |doi=  }}
-*{{cite journal  | author=Adams V, Griffin LD, Gelb BD, McCabe ER |title=Protein kinase activity of rat brain hexokinase. |journal=Biochem. Biophys. Res. Commun. |volume=177 |issue= 3 |pages= 1101–6 |year= 1991 |pmid= 2059200 |doi=  }}
+== Function ==
-*{{cite journal  | author=Murakami K, Blei F, Tilton W, ''et al.'' |title=An isozyme of hexokinase specific for the human red blood cell (HKR) |journal=Blood |volume=75 |issue= 3 |pages= 770–5 |year= 1990 |pmid= 2297576 |doi=  }}
-*{{cite journal  | author=Nishi S, Seino S, Bell GI |title=Human hexokinase: sequences of amino- and carboxyl-terminal halves are homologous. |journal=Biochem. Biophys. Res. Commun. |volume=157 |issue= 3 |pages= 937–43 |year= 1989 |pmid= 3207429 |doi=  }}
+As one of two mitochondrial isoforms of hexokinase and a member of the sugar kinase family, HK1 [[catalyze]]s the [[rate-limiting]] and first obligatory step of glucose metabolism, which is the ATP-dependent phosphorylation of glucose to G6P.<ref name=pmid9493266/><ref name=pmid23068103/><ref name=pmid16892082/><ref name=pmid22018957>{{cite journal | vauthors = Regenold WT, Pratt M, Nekkalapu S, Shapiro PS, Kristian T, Fiskum G | title = Mitochondrial detachment of hexokinase 1 in mood and psychotic disorders: implications for brain energy metabolism and neurotrophic signaling | journal = Journal of Psychiatric Research | volume = 46 | issue = 1 | pages = 95–104 | date = Jan 2012 | pmid = 22018957 | doi = 10.1016/j.jpsychires.2011.09.018 }}</ref> Physiological levels of G6P can regulate this process by inhibiting HK1 as [[negative feedback]], though [[inorganic phosphate]] (P<sub>i</sub>) can relieve G6P inhibition.<ref name=pmid9493266/><ref name=pmid9056853/><ref name=pmid16892082/> However, unlike [[HK2]] and [[HK3]], HK1 itself is not directly regulated by P<sub>i</sub>, which better suits its ubiquitous [[catabolic]] role.<ref name=pmid23068103/> By phosphorylating glucose, HK1 effectively prevents glucose from leaving the cell and, thus, commits glucose to energy metabolism.<ref name=pmid9493266/><ref name=pmid24018046/><ref name=pmid9056853/><ref name=pmid16892082/> Moreover, its localization and attachment to the OMM promotes the coupling of glycolysis to mitochondrial [[oxidative phosphorylation]], which greatly enhances ATP production by direct recycling of mitochondrial ATP/ADP to meet the cell’s energy demands.<ref name=pmid22018957/><ref name=pmid16892082/><ref name=pmid24560881>{{cite journal | vauthors = Shan D, Mount D, Moore S, Haroutunian V, Meador-Woodruff JH, McCullumsmith RE | title = Abnormal partitioning of hexokinase 1 suggests disruption of a glutamate transport protein complex in schizophrenia | journal = Schizophrenia Research | volume = 154 | issue = 1–3 | pages = 1–13 | date = Apr 2014 | pmid = 24560881 | doi = 10.1016/j.schres.2014.01.028 | pmc=4151500}}</ref> Specifically, OMM-bound HK1 binds [[VDAC1]] to trigger opening of the [[mitochondrial permeability transition pore]] and release mitochondrial ATP to further fuel the glycolytic process.<ref name=pmid16892082/><ref name=pmid23068103/>
-*{{cite journal  | author=Rijksen G, Akkerman JW, van den Wall Bake AW, ''et al.'' |title=Generalized hexokinase deficiency in the blood cells of a patient with nonspherocytic hemolytic anemia. |journal=Blood |volume=61 |issue= 1 |pages= 12–8 |year= 1983 |pmid= 6848140 |doi=  }}
-*{{cite journal  | author=Bianchi M, Magnani M |title=Hexokinase mutations that produce nonspherocytic hemolytic anemia. |journal=Blood Cells Mol. Dis. |volume=21 |issue= 1 |pages= 2–8 |year= 1995 |pmid= 7655856 |doi= 10.1006/bcmd.1995.0002 }}
+Another critical function for OMM-bound HK1 is cell survival and protection against [[oxidative damage]].<ref name=pmid22018957/><ref name=pmid23068103/> Activation of [[Akt]] [[kinase]] is mediated by HK1-VDAC1 coupling as part of the growth factor-mediated phosphatidyl inositol 3-kinase (PI3)/Akt cell survival intracellular signaling pathway, thus preventing [[cytochrome c]] release and subsequent apoptosis.<ref name=pmid22018957/><ref name=pmid12432216/><ref name=pmid16892082/><ref name=pmid23068103/> In fact, there is evidence that VDAC binding by the anti-apoptotic HK1 and by the pro-apoptotic [[creatine kinase]] are mutually exclusive, indicating that the absence of HK1 allows creatine kinase to bind and open VDAC.<ref name=pmid23068103/> Furthermore, HK1 has demonstrated anti-[[apoptotic]] activity by antagonizing [[Bcl-2]] proteins located at the OMM, which then inhibits [[TNF]]-induced apoptosis.<ref name=pmid12432216/><ref name=pmid24018046/>
-*{{cite journal  | author=Blachly-Dyson E, Zambronicz EB, Yu WH, ''et al.'' |title=Cloning and functional expression in yeast of two human isoforms of the outer mitochondrial membrane channel, the voltage-dependent anion channel. |journal=J. Biol. Chem. |volume=268 |issue= 3 |pages= 1835–41 |year= 1993 |pmid= 8420959 |doi=  }}
-*{{cite journal  | author=Aleshin AE, Zeng C, Fromm HJ, Honzatko RB |title=Crystallization and preliminary X-ray analysis of human brain hexokinase. |journal=FEBS Lett. |volume=391 |issue= 1-2 |pages= 9–10 |year= 1996 |pmid= 8706938 |doi=  }}
+In the [[prefrontal cortex]], HK1 putatively forms a protein complex with [[EAAT2]], [[Na+/K+ ATPase]], and [[aconitase]], which functions to remove [[glutamate]] from the perisynaptic space and maintain low basal levels in the [[synaptic cleft]].<ref name=pmid24560881/>
-*{{cite journal  | author=Visconti PE, Olds-Clarke P, Moss SB, ''et al.'' |title=Properties and localization of a tyrosine phosphorylated form of hexokinase in mouse sperm. |journal=Mol. Reprod. Dev. |volume=43 |issue= 1 |pages= 82–93 |year= 1996 |pmid= 8720117 |doi= 10.1002/(SICI)1098-2795(199601)43:1<82::AID-MRD11>3.0.CO;2-6 |doilabel=10.1002/(SICI)1098-2795(199601)43:1&#60;82::AID-MRD11&#62;3.0.CO;2-6 }}
-*{{cite journal  | author=Mori C, Nakamura N, Welch JE, ''et al.'' |title=Testis-specific expression of mRNAs for a unique human type 1 hexokinase lacking the porin-binding domain. |journal=Mol. Reprod. Dev. |volume=44 |issue= 1 |pages= 14–22 |year= 1997 |pmid= 8722688 |doi= 10.1002/(SICI)1098-2795(199605)44:1<14::AID-MRD2>3.0.CO;2-W |doilabel=10.1002/(SICI)1098-2795(199605)44:1&#60;14::AID-MRD2&#62;3.0.CO;2-W }}
+In particular, HK1 is the most ubiquitously expressed isoform out of the four hexokinases, and constitutively expressed in most tissues, though it is majorly found in [[brain]], [[kidney]], and [[red blood cell]]s (RBCs).<ref name=pmid12432216/><ref name=pmid9493266/><ref name=pmid24018046/><ref name=pmid23068103/><ref name=pmid24560881/><ref name=pmid16892082/><ref name=pmid4058069>{{cite journal|last1=Reid|first1=S|last2=Masters|first2=C|title=On the developmental properties and tissue interactions of hexokinase.|journal=Mechanisms of ageing and development|date=1985|volume=31|issue=2|pages=197–212|pmid=4058069|doi=10.1016/s0047-6374(85)80030-0}}</ref> Its high abundance in the [[retina]], specifically the photoreceptor inner segment, outer plexiform layer, inner nuclear layer, inner plexiform layer, and ganglion cell layer, attests to its crucial metabolic purpose.<ref name=pmid25316723>{{cite journal | vauthors = Wang F, Wang Y, Zhang B, Zhao L, Lyubasyuk V, Wang K, Xu M, Li Y, Wu F, Wen C, Bernstein PS, Lin D, Zhu S, Wang H, Zhang K, Chen R | title = A missense mutation in HK1 leads to autosomal dominant retinitis pigmentosa | journal = Investigative Ophthalmology & Visual Science | volume = 55 | issue = 11 | pages = 7159–64 | date = Nov 2014 | pmid = 25316723 | doi = 10.1167/iovs.14-15520 | pmc=4224578}}</ref> It is also expressed in cells derived from [[hematopoietic]] [[stem cell]]s, such as RBCs, [[leukocyte]]s, and [[platelet]]s, as well as from erythroid-progenitor cells.<ref name=pmid12432216/> Of note, HK1 is the sole hexokinase isoform found in the cells and tissues which rely most heavily on glucose metabolism for their function, including brain, erythrocytes, platelets, leukocytes, and [[fibroblast]]s.<ref name=pmid21781351>{{cite journal | vauthors = Gjesing AP, Nielsen AA, Brandslund I, Christensen C, Sandbæk A, Jørgensen T, Witte D, Bonnefond A, Froguel P, Hansen T, Pedersen O | title = Studies of a genetic variant in HK1 in relation to quantitative metabolic traits and to the prevalence of type 2 diabetes | journal = BMC Medical Genetics | volume = 12 | page = 99 | date = 25 July 2011 | pmid = 21781351 | doi = 10.1186/1471-2350-12-99 | pmc=3161933}}</ref> In rats, it is also the predominant hexokinase in fetal tissues, likely due to their constitutive glucose utilization.<ref name=pmid9056853/><ref name=pmid4058069/>
-*{{cite journal  | author=Murakami K, Piomelli S |title=Identification of the cDNA for human red blood cell-specific hexokinase isozyme. |journal=Blood |volume=89 |issue= 3 |pages= 762–6 |year= 1997 |pmid= 9028305 |doi=  }}
-*{{cite journal  | author=Ruzzo A, Andreoni F, Magnani M |title=An erythroid-specific exon is present in the human hexokinase gene. |journal=Blood |volume=91 |issue= 1 |pages= 363–4 |year= 1998 |pmid= 9414310 |doi=  }}
+== Clinical significance ==
-*{{cite journal  | author=Travis AJ, Foster JA, Rosenbaum NA, ''et al.'' |title=Targeting of a germ cell-specific type 1 hexokinase lacking a porin-binding domain to the mitochondria as well as to the head and fibrous sheath of murine spermatozoa. |journal=Mol. Biol. Cell |volume=9 |issue= 2 |pages= 263–76 |year= 1998 |pmid= 9450953 |doi=  }}
-*{{cite journal  | author=Aleshin AE, Zeng C, Bourenkov GP, ''et al.'' |title=The mechanism of regulation of hexokinase: new insights from the crystal structure of recombinant human brain hexokinase complexed with glucose and glucose-6-phosphate. |journal=Structure |volume=6 |issue= 1 |pages= 39–50 |year= 1998 |pmid= 9493266 |doi=  }}
+[[Mutations]] in this gene are associated with type 4H of [[Charcot–Marie–Tooth disease]], also known as Russe-type hereditary motor and sensory neuropathy (HMSNR).<ref>{{OMIM|605285}}</ref> Due to the crucial role of HK1 in glycolysis, hexokinase deficiency has been identified as a cause of erythroenzymopathies associated with [[hereditary non-spherocytic hemolytic anemia]] (HNSHA). Likewise, HK1 deficiency has resulted in [[wikt:cerebral|cerebral]] [[white matter]] injury, malformations, and psychomotor retardation, as well as  latent [[diabetes mellitus]] and pan[[myelopathy]].<ref name=pmid12432216/> Meanwhile, HK1 is highly expressed in [[cancer]]s, and its anti-apoptotic effects have been observed in highly glycolytic [[hepatoma]] cells.<ref name=pmid24018046/><ref name=pmid12432216/>
-*{{cite journal  | author=Ruzzo A, Andreoni F, Magnani M |title=Structure of the human hexokinase type I gene and nucleotide sequence of the 5' flanking region. |journal=Biochem. J. |volume=331 ( Pt 2) |issue=  |pages= 607–13 |year= 1998 |pmid= 9531504 |doi=  }}
-*{{cite journal  | author=Aleshin AE, Zeng C, Bartunik HD, ''et al.'' |title=Regulation of hexokinase I: crystal structure of recombinant human brain hexokinase complexed with glucose and phosphate. |journal=J. Mol. Biol. |volume=282 |issue= 2 |pages= 345–57 |year= 1998 |pmid= 9735292 |doi= 10.1006/jmbi.1998.2017 }}
+=== Neurodegenerative disorders ===
-*{{cite journal  | author=Murakami K, Kanno H, Miwa S, Piomelli S |title=Human HKR isozyme: organization of the hexokinase I gene, the erythroid-specific promoter, and transcription initiation site. |journal=Mol. Genet. Metab. |volume=67 |issue= 2 |pages= 118–30 |year= 1999 |pmid= 10356311 |doi= 10.1006/mgme.1999.2842 }}
-}}
+HK1 may be causally linked to [[mood disorder|mood]] and [[psychotic disorders]], including [[unipolar depression]] (UPD), [[bipolar disorder]] (BPD), and [[schizophrenia]] via both its roles in energy metabolism and cell survival. For instance, the accumulation of lactate in the brains of BPD and SCHZ patients potentially results from the decoupling of HK1 from the OMM, and by extension, glycolysis from mitochondrial oxidative, phosphorylation. In the case of SCHZ, decreasing  HK1 attachment to the OMM in the [[parietal cortex]] resulted in decreased glutamate reuptake capacity and, thus, glutamate spillover from the [[synapse]]s. The released glutamate activates extrasynaptic glutamate receptors, leading to altered structure and function of glutamate circuits, [[synaptic plasticity]], frontal cortical dysfunction, and ultimately, the cognitive deficits characteristic of SCHZ.<ref name=pmid24560881/> Similarly, Hk1 mitochondrial detachment has been associated with [[hypothyroidism]], which involves abnormal brain development and increased risk for [[depression (mood)|depression]], while its attachment leads to [[neural]] growth.<ref name=pmid22018957/> In [[Parkinson’s disease]], HK1 detachment from VDAC via [[Parkin (ligase)|Parkin]]-mediated [[ubiquitylation]] and degradation disrupts the MPTP on [[Depolarization|depolarized]] mitochondria, consequently blocking mitochondrial localization of Parkin and halting glycolysis.<ref name=pmid23068103/> Further research is required to determine the relative HK1 detachment needed in various cell types for different psychiatric disorders. This research can also contribute to developing therapies to target causes of the detachment, from gene mutations to interference by factors such as [[beta-amyloid]] peptide and [[insulin]].<ref name=pmid22018957/>
+=== Retinitis pigmentosa ===
+A [[heterozygous]] [[missense mutation]] in the ''HK1'' gene (a change at position 847 from glutamate to lysine) has been linked to [[retinitis pigmentosa]].<ref name=pmid25190649>{{cite journal | vauthors = Sullivan LS, Koboldt DC, Bowne SJ, Lang S, Blanton SH, Cadena E, Avery CE, Lewis RA, Webb-Jones K, Wheaton DH, Birch DG, Coussa R, Ren H, Lopez I, Chakarova C, Koenekoop RK, Garcia CA, Fulton RS, Wilson RK, Weinstock GM, Daiger SP | title = A dominant mutation in hexokinase 1 (HK1) causes retinitis pigmentosa | journal = Investigative Ophthalmology & Visual Science | volume = 55 | issue = 11 | pages = 7147–58 | date = Nov 2014 | pmid = 25190649 | doi = 10.1167/iovs.14-15419 | pmc=4224580}}</ref><ref name=pmid25316723/> Since this [[substitution mutation]] is located far from known functional sites and does not impair the enzyme’s glycolytic activity, it is likely that the mutation acts through another biological mechanism unique to the retina.<ref name=pmid25190649/> Notably, studies in mouse retina reveal interactions between Hk1, the mitochondrial metallochaperone Cox11, and the chaperone protein Ranbp2, which serve to maintain normal metabolism and function in the retina. Thus, the mutation may disrupt these interactions and lead to retinal degradation.<ref name=pmid25316723/> Alternatively, this mutation may act through the enzyme’s anti-apoptotic function, as disrupting the regulation of the hexokinase-mitochondria association by insulin receptors could trigger photoreceptor apoptosis and retinal degeneration.<ref name=pmid25190649/><ref name=pmid25316723/> In this case, treatments that preserve the hexokinase–mitochondria association may serve as a potential therapeutic approach.<ref name=pmid25316723/>
+== Interactions ==
+HK1 is known to [[protein-protein interaction|interact]] with:
+*[[VDAC]],<ref name=pmid23068103/>
+*[[Parkin (ligase)|Parkin]],<ref name=pmid23068103/>
+*[[EAAT2]],<ref name=pmid24560881/>
+*[[Na+/K+ ATPase]],<ref name=pmid24560881/> and
+*[[Aconitase]].<ref name=pmid24560881/>
+==Interactive pathway map==
+{{GlycolysisGluconeogenesis_WP534|highlight=HK1}}
+==See also==
+{{Portal|Mitochondria}}
+*[[Hexokinase]]
+*[[HK2]]
+*[[HK3]]
+*[[Glucokinase]]
+== References ==
+{{reflist|33em}}
+== Further reading ==
+{{refbegin|33em}}
+* {{cite journal | vauthors = Daniele A, Altruda F, Ferrone M, Silengo L, Romeo G, Archidiacono N, Rocchi M | title = Mapping of human hexokinase 1 gene to 10q11----qter | journal = Human Heredity | volume = 42 | issue = 2 | pages = 107–10 | year = 1992 | pmid = 1572668 | doi = 10.1159/000154049 }}
+* {{cite journal | vauthors = Magnani M, Bianchi M, Casabianca A, Stocchi V, Daniele A, Altruda F, Ferrone M, Silengo L | title = A recombinant human 'mini'-hexokinase is catalytically active and regulated by hexose 6-phosphates | journal = The Biochemical Journal | volume = 285 | issue = 1 | pages = 193–9 | date = Jul 1992 | pmid = 1637300 | pmc = 1132765 | doi =  10.1042/bj2850193}}
+* {{cite journal | vauthors = Magnani M, Serafini G, Bianchi M, Casabianca A, Stocchi V | title = Human hexokinase type I microheterogeneity is due to different amino-terminal sequences | journal = The Journal of Biological Chemistry | volume = 266 | issue = 1 | pages = 502–5 | date = Jan 1991 | pmid = 1985912 | doi =  }}
+* {{cite journal | vauthors = Adams V, Griffin LD, Gelb BD, McCabe ER | title = Protein kinase activity of rat brain hexokinase | journal = Biochemical and Biophysical Research Communications | volume = 177 | issue = 3 | pages = 1101–6 | date = Jun 1991 | pmid = 2059200 | doi = 10.1016/0006-291X(91)90652-N }}
+* {{cite journal | vauthors = Murakami K, Blei F, Tilton W, Seaman C, Piomelli S | title = An isozyme of hexokinase specific for the human red blood cell (HKR) | journal = Blood | volume = 75 | issue = 3 | pages = 770–5 | date = Feb 1990 | pmid = 2297576 | doi =  }}
+* {{cite journal | vauthors = Nishi S, Seino S, Bell GI | title = Human hexokinase: sequences of amino- and carboxyl-terminal halves are homologous | journal = Biochemical and Biophysical Research Communications | volume = 157 | issue = 3 | pages = 937–43 | date = Dec 1988 | pmid = 3207429 | doi = 10.1016/S0006-291X(88)80964-1 }}
+* {{cite journal | vauthors = Rijksen G, Akkerman JW, van den Wall Bake AW, Hofstede DP, Staal GE | title = Generalized hexokinase deficiency in the blood cells of a patient with nonspherocytic hemolytic anemia | journal = Blood | volume = 61 | issue = 1 | pages = 12–8 | date = Jan 1983 | pmid = 6848140 | doi =  }}
+* {{cite journal | vauthors = Bianchi M, Magnani M | title = Hexokinase mutations that produce nonspherocytic hemolytic anemia | journal = Blood Cells, Molecules & Diseases | volume = 21 | issue = 1 | pages = 2–8 | year = 1995 | pmid = 7655856 | doi = 10.1006/bcmd.1995.0002 }}
+* {{cite journal | vauthors = Blachly-Dyson E, Zambronicz EB, Yu WH, Adams V, McCabe ER, Adelman J, Colombini M, Forte M | title = Cloning and functional expression in yeast of two human isoforms of the outer mitochondrial membrane channel, the voltage-dependent anion channel | journal = The Journal of Biological Chemistry | volume = 268 | issue = 3 | pages = 1835–41 | date = Jan 1993 | pmid = 8420959 | doi =  }}
+* {{cite journal | vauthors = Aleshin AE, Zeng C, Fromm HJ, Honzatko RB | title = Crystallization and preliminary X-ray analysis of human brain hexokinase | journal = FEBS Letters | volume = 391 | issue = 1–2 | pages = 9–10 | date = Aug 1996 | pmid = 8706938 | doi = 10.1016/0014-5793(96)00688-6 }}
+* {{cite journal | vauthors = Visconti PE, Olds-Clarke P, Moss SB, Kalab P, Travis AJ, de las Heras M, Kopf GS | title = Properties and localization of a tyrosine phosphorylated form of hexokinase in mouse sperm | journal = Molecular Reproduction and Development | volume = 43 | issue = 1 | pages = 82–93 | date = Jan 1996 | pmid = 8720117 | doi = 10.1002/(SICI)1098-2795(199601)43:1<82::AID-MRD11>3.0.CO;2-6 }}
+* {{cite journal | vauthors = Mori C, Nakamura N, Welch JE, Shiota K, Eddy EM | title = Testis-specific expression of mRNAs for a unique human type 1 hexokinase lacking the porin-binding domain | journal = Molecular Reproduction and Development | volume = 44 | issue = 1 | pages = 14–22 | date = May 1996 | pmid = 8722688 | doi = 10.1002/(SICI)1098-2795(199605)44:1<14::AID-MRD2>3.0.CO;2-W }}
+* {{cite journal | vauthors = Murakami K, Piomelli S | title = Identification of the cDNA for human red blood cell-specific hexokinase isozyme | journal = Blood | volume = 89 | issue = 3 | pages = 762–6 | date = Feb 1997 | pmid = 9028305 | doi =  }}
+* {{cite journal | vauthors = Ruzzo A, Andreoni F, Magnani M | title = An erythroid-specific exon is present in the human hexokinase gene | journal = Blood | volume = 91 | issue = 1 | pages = 363–4 | date = Jan 1998 | pmid = 9414310 | doi =  }}
+* {{cite journal | vauthors = Travis AJ, Foster JA, Rosenbaum NA, Visconti PE, Gerton GL, Kopf GS, Moss SB | title = Targeting of a germ cell-specific type 1 hexokinase lacking a porin-binding domain to the mitochondria as well as to the head and fibrous sheath of murine spermatozoa | journal = Molecular Biology of the Cell | volume = 9 | issue = 2 | pages = 263–76 | date = Feb 1998 | pmid = 9450953 | pmc = 25249 | doi = 10.1091/mbc.9.2.263 }}
+* {{cite journal | vauthors = Aleshin AE, Zeng C, Bourenkov GP, Bartunik HD, Fromm HJ, Honzatko RB | title = The mechanism of regulation of hexokinase: new insights from the crystal structure of recombinant human brain hexokinase complexed with glucose and glucose-6-phosphate | journal = Structure | volume = 6 | issue = 1 | pages = 39–50 | date = Jan 1998 | pmid = 9493266 | doi = 10.1016/S0969-2126(98)00006-9 }}
+* {{cite journal | vauthors = Ruzzo A, Andreoni F, Magnani M | title = Structure of the human hexokinase type I gene and nucleotide sequence of the 5' flanking region | journal = The Biochemical Journal | volume = 331 | issue = 2 | pages = 607–13 | date = Apr 1998 | pmid = 9531504 | pmc = 1219395 | doi =  10.1042/bj3310607}}
+* {{cite journal | vauthors = Aleshin AE, Zeng C, Bartunik HD, Fromm HJ, Honzatko RB | title = Regulation of hexokinase I: crystal structure of recombinant human brain hexokinase complexed with glucose and phosphate | journal = Journal of Molecular Biology | volume = 282 | issue = 2 | pages = 345–57 | date = Sep 1998 | pmid = 9735292 | doi = 10.1006/jmbi.1998.2017 }}
+* {{cite journal | vauthors = Murakami K, Kanno H, Miwa S, Piomelli S | title = Human HKR isozyme: organization of the hexokinase I gene, the erythroid-specific promoter, and transcription initiation site | journal = Molecular Genetics and Metabolism | volume = 67 | issue = 2 | pages = 118–30 | date = Jun 1999 | pmid = 10356311 | doi = 10.1006/mgme.1999.2842 }}
 {{refend}}
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 {{Glycolysis enzymes}}