Sodium-coupled monocarboxylate transporter 2

From WikiProjectMed
Jump to navigation Jump to search

Sodium-coupled monocarboxylate transporter 2 (i.e., SMCT2, also termed SLC5A12) is a plasma membrane transport protein in the solute carrier family. It transports sodium cations (i.e., Na+) in association with the anionic forms (see conjugated base) of certain short-chain fatty acids (i.e., SC-FAs) and other agents through the plasma membrane from the outside to the inside of cells.[1] The only other member of the sodium-coupled monocarboxylate transporter group (sometimes referred to as the SLC5A family[2]), SMCT1, similarly co-transports SC-FAs and other agents into cells. Monocarboxylate transporters (MCTs) are also transport proteins in the solute carrier family. They co-transport the anionic forms of various compounds into cells in association with hydrogen cations (i.e. H+).[3] Four of the 14 MCTs, i.e. SLC16A1 (i.e., MCT1), SLC16A7 (i.e., MCT22), SLC16A8 (i.e., MCT3), and SLC16A3 (i.e., MCT4), transport some of the same SC-FAs anions that the two SMCTs transport into cells.[2][4] SC-FAs do diffuse into cells independently of transport proteins but at the levels normally occurring in tissues greater amounts of the SC-FAs are brought into cells that express a SC-FA transporter.[1][3]

The human gene responsible for producing SMCT2 protein, i.e., the SLC5A12 gene, is located at position 14.2 on the "p" (i.e., short) arm of chromosome 11 (position notated as chromosome 11p14.2).[5] The full length SMCT2 protein product of this gene consist of 618 amino acids[6] and has a 57% identity with the SMCT1 protein at the amino acid level.[7] The gene for SMCT2 in mice and rats is termed the Slc5a12 gene.

Studies indicate that the SMCT2 on intestinal epithelial cells promotes their uptake of intra-intestinal SC-FAs and subsequent diffusion of the SC-FAs into the systemic circulation. These SC-FAs serve as energy sources for[8] and activators of diverse responses in[9][10][11] a wide range of cell types in the intestinal wall and throughout the entire body. Studies also suggest that: 1) SMCT2 in the kidney tubule cells contributes to the reabsorption of urinary SC-FAs that would otherwise be wasted in the urine; 2) the SMCT2 on the Müller cells in the eye promotes their uptake SC-FAs which they pass on to retinal neurons that use them as energy sources;[12] and 3) the SCMT2 on skeletal muscle cells may contribute to regulating their lactic acid levels.[13]

Tissues and cells expressing SMCT2

The SMCT2 protein and/or its messenger RNA is expressed by the human and/or murine: epithelial cells in the proximal (i.e., initial and middle portions) of the small intestine; epithelial cells in the renal tubules of the kidney;[7] Müeller cells in the retina,[12] and skeletal muscles throughout the body.[13]

Agents transmitted by or blocking SMCT2

The SC-FAs transported into cells by SMCT2 include butyric, proprionic, pyruvic, lactic, acetic, and β-hydroxybutyric acids. SMCT2 also transports into cells the anionic forms of nicotinic acid[1][7][13] and gamma-hydroxybutyric acid.[2] Nonsteroidal anti-inflammatory drugs such as ibuprofen, ketoprofen, and fenoprofen bind to but are not transported by SMCT2. However, their binding blocks the binding and thereby transportation of the anionic SC-FAs and, presumably, the other anionic compounds that SMTC2 normally transports into cells. SMCT1 likewise transports these SC-FAs and nicotinic acid and is blocked by the cited anti-inflammatory drugs.[8] SMCT2 does have much lower affinities than SMCT1 for binding the SC-FAs and therefore is better suited to transport larger amounts of SC-FAs when their concentrations are high.[1][13]

Functions of SMCT2

Gastrointestinal tract

SC-FAs inside the gastrointestinal tract come from the ingested food or are released by intestinal bacteria as fermentation products of the ingested food. SMCT2-bearing cells are located in the epithelial cells of the proximal portion (primarily the jejunum[14]) of the small intestine but are not in the large intestine or cecum. Cells bearing the SMCT2 transporter, which has relatively low affinity for the SC-FAs, are suited to transport the high levels of dietary SC-FAs that are usually found in the proximal small intestine. Cells bearing the SMCT1 transporter, which has a relatively high affinity for the SC-FAs, are located in the large intestine and cecum. These cells are suited to take up the relatively low concentrations of the SC-FAs that are present in these sites.[1][7][14] The SC-FAs in the gastrointestinal tracts diffuse into the intestinal wall and transported by SMCT2 (and other intestinal SC-FA transporters[15]) serve as energy sources for cells located in the intestinal wall and throughout the body.[8] They also stimulate various functions in cells of the intestine and throughout the body that express one of the SC-FA receptors, i.e., free fatty acid receptor 2, free fatty acid receptor 3, or hydroxycarboxylic acid receptor 2. (For the functions elicited by SC-FA's activation of these receptors see free fatty acid receptor 2 functions, free fatty acid receptor 3 functions, and hydroxycarboxylic acid receptor 2 functions.)[10][11][16] In addition, the SC-FAs that enter cells can directly activate certain signal transduction pathways and thereby elicit cellular responses independently of the three cited SC-FA receptors.[9]

Urinary tract

Studies in mice indicate that SMCT2 is located in the brush borders of the cells lining the kidney's proximal tubules with decreasing numbers of SMTC2-exressing cells in proximal tubule segments S1, S2, and S3.[8] In contrast, SMCT1 is mostly limited to the S3, i.e., most distal, segment of the proximal tubules.[5][13] Thus, the kidney's proximal tubules consist of SMCT1-bearing cells that transfer the higher levels of SC-FAs found in the proximal tubules while the SMCT1-bearing cells are active in transferring the lower levels of SC-FAs in more distal part of the proximal tubules.[5] Other studies have shown that 1) mice lacking SMCT1 due to the knockout of their Slc8a5 gene had massive increases in the levels of lactic acid in their urine[17] and 2) C/ebpδ gene knockout mice (these mice do not express SCMT1 or SCMT2 in their kidney tissues) likewise have a marked increase in urinary excretion of lactic and also show decreases in their lactic acid blood levels.[18] These findings indicate that, in mice, SMCT1 is involved in the reabsorption of urine SC-FAs and that SMCT2 may also do so but studies on SLC5A12 gene knockout mice are needed to prove this.[17]

Eyes

Müller cells (also termed Müller glia) are critical non-neural components of the retina. They form and maintain the retina's structure, control retinal immune responses by, e.g., releasing inflammatory mediators and engulfing dead cell debris, and provide retinal neurons with essential nutrients, particularly the SC-FA, pyruvic acid.[19] SMCT2 has been detected in the Müller cells of mouse retinas and, based on indirect studies, the human rMC-1 Müeller cell line. These studies suggest that the function of SMCT2 in the retinal Müller cells of mice and humans is to take up SC-FAs and transfer of them to retinal neurons for their use as energy sources, particularly at times when other energy sources are less available.[12]

Skeletal muscle

Skeletal muscles accumulate lactic acid during their contractions. This lactic acid, particularly if in excess, moves out of the skeletal muscles and either diffuses into the systemic circulation or is transferred into skeletal muscles that do not have an excessive buildup of lactic acid. The transfer of lactic acid out and into human skeletal muscle has been thought to be mediated by the H+-coupled monocarboxylate transporters, MCT1 and MCT4.[20] However, a more recent study detected SMCT2 and SMCT1 in the skeletal muscles of mice and suggested that they may contribute to the transport of SC-FAs in skeletal muscles in mice.[13] Further studies are needed to determine if SCMT2 and/or SMCT1 are expressed by human skeletal muscle and contribute to the transport of lactic acid in mouse and/or human skeletal muscle.

See also

Sodium-coupled monocarboxylate transporter 1

References

  1. ^ a b c d e Sivaprakasam S, Bhutia YD, Yang S, Ganapathy V (December 2017). "Short-Chain Fatty Acid Transporters: Role in Colonic Homeostasis". Comprehensive Physiology. 8 (1): 299–314. doi:10.1002/cphy.c170014. ISBN 9780470650714. PMC 6019286. PMID 29357130.
  2. ^ a b c Felmlee MA, Morse BL, Morris ME (January 2021). "γ-Hydroxybutyric Acid: Pharmacokinetics, Pharmacodynamics, and Toxicology". The AAPS Journal. 23 (1): 22. doi:10.1208/s12248-020-00543-z. PMC 8098080. PMID 33417072.
  3. ^ a b Felmlee MA, Jones RS, Rodriguez-Cruz V, Follman KE, Morris ME (April 2020). "Monocarboxylate Transporters (SLC16): Function, Regulation, and Role in Health and Disease". Pharmacological Reviews. 72 (2): 466–485. doi:10.1124/pr.119.018762. PMC 7062045. PMID 32144120.
  4. ^ Song W, Li D, Tao L, Luo Q, Chen L (January 2020). "Solute carrier transporters: the metabolic gatekeepers of immune cells". Acta Pharmaceutica Sinica. B. 10 (1): 61–78. doi:10.1016/j.apsb.2019.12.006. PMC 6977534. PMID 31993307.
  5. ^ a b c Gopal E, Umapathy NS, Martin PM, Ananth S, Gnana-Prakasam JP, Becker H, Wagner CA, Ganapathy V, Prasad PD (November 2007). "Cloning and functional characterization of human SMCT2 (SLC5A12) and expression pattern of the transporter in kidney". Biochimica et Biophysica Acta (BBA) - Biomembranes. 1768 (11): 2690–7. doi:10.1016/j.bbamem.2007.06.031. PMC 2703486. PMID 17692818.
  6. ^ "UniProt".
  7. ^ a b c d Iwanaga T, Kishimoto A (2015). "Cellular distributions of monocarboxylate transporters: a review". Biomedical Research (Tokyo, Japan). 36 (5): 279–301. doi:10.2220/biomedres.36.279. PMID 26522146.
  8. ^ a b c d Ganapathy V, Thangaraju M, Gopal E, Martin PM, Itagaki S, Miyauchi S, Prasad PD (2008). "Sodium-coupled monocarboxylate transporters in normal tissues and in cancer". The AAPS Journal. 10 (1): 193–9. doi:10.1208/s12248-008-9022-y. PMC 2751467. PMID 18446519.
  9. ^ a b Elangovan S, Pathania R, Ramachandran S, Ananth S, Padia RN, Srinivas SR, Babu E, Hawthorn L, Schoenlein PV, Boettger T, Smith SB, Prasad PD, Ganapathy V, Thangaraju M (October 2013). "Molecular mechanism of SLC5A8 inactivation in breast cancer". Molecular and Cellular Biology. 33 (19): 3920–35. doi:10.1128/MCB.01702-12. PMC 3811868. PMID 23918800.
  10. ^ a b Kimura I, Ichimura A, Ohue-Kitano R, Igarashi M (January 2020). "Free Fatty Acid Receptors in Health and Disease". Physiological Reviews. 100 (1): 171–210. doi:10.1152/physrev.00041.2018. PMID 31487233. S2CID 201845937.
  11. ^ a b Cosín-Roger J, Ortiz-Masia D, Barrachina MD, Calatayud S (October 2020). "Metabolite Sensing GPCRs: Promising Therapeutic Targets for Cancer Treatment?". Cells. 9 (11): 2345. doi:10.3390/cells9112345. PMC 7690732. PMID 33113952.
  12. ^ a b c Martin PM, Dun Y, Mysona B, Ananth S, Roon P, Smith SB, Ganapathy V (July 2007). "Expression of the sodium-coupled monocarboxylate transporters SMCT1 (SLC5A8) and SMCT2 (SLC5A12) in retina". Investigative Ophthalmology & Visual Science. 48 (7): 3356–63. doi:10.1167/iovs.06-0888. PMID 17591909.
  13. ^ a b c d e f Srinivas SR, Gopal E, Zhuang L, Itagaki S, Martin PM, Fei YJ, Ganapathy V, Prasad PD (December 2005). "Cloning and functional identification of slc5a12 as a sodium-coupled low-affinity transporter for monocarboxylates (SMCT2)". The Biochemical Journal. 392 (Pt 3): 655–64. doi:10.1042/BJ20050927. PMC 1316307. PMID 16104846.
  14. ^ a b Bongarzone S, Barbon E, Ferocino A, Alsulaimani L, Dunn J, Kim J, Sunassee K, Gee A (2020). "Imaging niacin trafficking with positron emission tomography reveals in vivo monocarboxylate transporter distribution". Nuclear Medicine and Biology. 88–89: 24–33. doi:10.1016/j.nucmedbio.2020.07.002. PMC 7599079. PMID 32683248.
  15. ^ Teramae H, Yoshikawa T, Inoue R, Ushida K, Takebe K, Nio-Kobayashi J, Iwanaga T (August 2010). "The cellular expression of SMCT2 and its comparison with other transporters for monocarboxylates in the mouse digestive tract". Biomedical Research (Tokyo, Japan). 31 (4): 239–49. doi:10.2220/biomedres.31.239. PMID 20834181.
  16. ^ Wuerch E, Urgoiti GR, Yong VW (July 2023). "The Promise of Niacin in Neurology". Neurotherapeutics. 20 (4): 1037–1054. doi:10.1007/s13311-023-01376-2. PMC 10457276. PMID 37084148.
  17. ^ a b Frank H, Gröger N, Diener M, Becker C, Braun T, Boettger T (September 2008). "Lactaturia and loss of sodium-dependent lactate uptake in the colon of SLC5A8-deficient mice". The Journal of Biological Chemistry. 283 (36): 24729–37. doi:10.1074/jbc.M802681200. PMC 3259809. PMID 18562324.
  18. ^ Thangaraju M, Ananth S, Martin PM, Roon P, Smith SB, Sterneck E, Prasad PD, Ganapathy V (September 2006). "c/ebpdelta Null mouse as a model for the double knock-out of slc5a8 and slc5a12 in kidney". The Journal of Biological Chemistry. 281 (37): 26769–73. doi:10.1074/jbc.C600189200. PMID 16873376.
  19. ^ Gao H, A L, Huang X, Chen X, Xu H (May 2021). "Müller Glia-Mediated Retinal Regeneration". Molecular Neurobiology. 58 (5): 2342–2361. doi:10.1007/s12035-020-02274-w. PMID 33417229. S2CID 231192160.
  20. ^ Juel C (November 2001). "Current aspects of lactate exchange: lactate/H+ transport in human skeletal muscle". European Journal of Applied Physiology. 86 (1): 12–6. doi:10.1007/s004210100517. PMID 11820315. S2CID 22025637.
Retrieved from "https://mdwiki.org/wiki/Sodium-coupled_monocarboxylate_transporter_2"