Biology:Membrane protein

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Short description: Proteins that are part of, or interact with, biological membranes
Membrane protein complexes of photosynthesis in the thylakoid membrane

Membrane proteins are common proteins that are part of, or interact with, biological membranes. Membrane proteins fall into several broad categories depending on their location. Integral membrane proteins are a permanent part of a cell membrane and can either penetrate the membrane (transmembrane) or associate with one or the other side of a membrane (integral monotopic). Peripheral membrane proteins are transiently associated with the cell membrane.

Membrane proteins are common, and medically important—about a third of all human proteins are membrane proteins, and these are targets for more than half of all drugs.[1] Nonetheless, compared to other classes of proteins, determining membrane protein structures remains a challenge in large part due to the difficulty in establishing experimental conditions that can preserve the correct conformation of the protein in isolation from its native environment.

Function

Membrane proteins perform a variety of functions vital to the survival of organisms:[2]

The localization of proteins in membranes can be predicted reliably using hydrophobicity analyses of protein sequences, i.e. the localization of hydrophobic amino acid sequences.

Integral membrane proteins

Schematic representation of transmembrane proteins: 1. a single transmembrane α-helix (bitopic membrane protein) 2. a polytopic transmembrane α-helical protein 3. a polytopic transmembrane β-sheet protein
The membrane is represented in light-brown.
Main pages: Biology:Integral membrane protein and Biology:Transmembrane protein

Integral membrane proteins are permanently attached to the membrane. Such proteins can be separated from the biological membranes only using detergents, nonpolar solvents, or sometimes denaturing agents.[citation needed] They can be classified according to their relationship with the bilayer:

  • Integral polytopic proteins are transmembrane proteins that span across the membrane more than once. These proteins may have different transmembrane topology.[4][5] These proteins have one of two structural architectures:
  • Bitopic proteins are transmembrane proteins that span across the membrane only once. Transmembrane helices from these proteins have significantly different amino acid distributions to transmembrane helices from polytopic proteins.[7]
  • Integral monotopic proteins are integral membrane proteins that are attached to only one side of the membrane and do not span the whole way across.

Peripheral membrane proteins

Schematic representation of the different types of interaction between monotopic membrane proteins and the cell membrane: 1. interaction by an amphipathic α-helix parallel to the membrane plane (in-plane membrane helix) 2. interaction by a hydrophobic loop 3. interaction by a covalently bound membrane lipid (lipidation) 4. electrostatic or ionic interactions with membrane lipids (e.g. through a calcium ion)
Main page: Biology:Peripheral membrane protein

Peripheral membrane proteins are temporarily attached either to the lipid bilayer or to integral proteins by a combination of hydrophobic, electrostatic, and other non-covalent interactions. Peripheral proteins dissociate following treatment with a polar reagent, such as a solution with an elevated pH or high salt concentrations.[citation needed]

Integral and peripheral proteins may be post-translationally modified, with added fatty acid, diacylglycerol[8] or prenyl chains, or GPI (glycosylphosphatidylinositol), which may be anchored in the lipid bilayer.

Polypeptide toxins

Main page: Biology:Pore-forming toxin

Polypeptide toxins and many antibacterial peptides, such as colicins or hemolysins, and certain proteins involved in apoptosis, are sometimes considered a separate category. These proteins are water-soluble but can aggregate and associate irreversibly with the lipid bilayer and become reversibly or irreversibly membrane-associated.[citation needed]

In genomes

Membrane proteins, like soluble globular proteins, fibrous proteins, and disordered proteins, are common.[9] It is estimated that 20–30% of all genes in most genomes encode for membrane proteins.[10][11] For instance, about 1000 of the ~4200 proteins of E. coli are thought to be membrane proteins, 600 of which have been experimentally verified to be membrane resident.[12] In humans, current thinking suggests that fully 30% of the genome encodes membrane proteins.[13]

In disease

Membrane proteins are the targets of over 50% of all modern medicinal drugs.[1] Among the human diseases in which membrane proteins have been implicated are heart disease, Alzheimer's and cystic fibrosis.[13]

Purification of membrane proteins

Although membrane proteins play an important role in all organisms, their purification has historically, and continues to be, a huge challenge for protein scientists. In 2008, 150 unique structures of membrane proteins were available,[14] and by 2019 only 50 human membrane proteins had had their structures elucidated.[13] In contrast, approximately 25% of all proteins are membrane proteins.[15] Their hydrophobic surfaces make structural and especially functional characterization difficult.[13][16] Detergents can be used to render membrane proteins water-soluble, but these can also alter protein structure and function.[13] Making membrane proteins water-soluble can also be achieved through engineering the protein sequence, replacing selected hydrophobic amino acids with hydrophilic ones, taking great care to maintain secondary structure while revising overall charge.[13]

Affinity chromatography is one of the best solutions for purification of membrane proteins. The activity of membrane proteins decreases very fast in contrast to other proteins.[citation needed] So, affinity chromatography provides a fast and specific purification of membrane proteins. The polyhistidine-tag is a commonly used tag for membrane protein purification,[17] and the alternative rho1D4 tag has also been successfully used.[18][19]

See also

References

  1. 1.0 1.1 "How many drug targets are there?". Nature Reviews. Drug Discovery 5 (12): 993–6. December 2006. doi:10.1038/nrd2199. PMID 17139284. 
  2. "Mapping the human membrane proteome: a majority of the human membrane proteins can be classified according to function and evolutionary origin". BMC Biology 7: 50. August 2009. doi:10.1186/1741-7007-7-50. PMID 19678920. 
  3. "The substitution of Arg149 with Cys fixes the melibiose transporter in an inward-open conformation". Biochimica et Biophysica Acta (BBA) - Biomembranes 1828 (8): 1690–9. August 2013. doi:10.1016/j.bbamem.2013.03.003. PMID 23500619. open access
  4. "Membrane-protein topology". Nature Reviews. Molecular Cell Biology 7 (12): 909–18. December 2006. doi:10.1038/nrm2063. PMID 17139331. 
  5. Gerald Karp (2009). Cell and Molecular Biology: Concepts and Experiments. John Wiley and Sons. pp. 128–. ISBN 978-0-470-48337-4. https://books.google.com/books?id=arRGYE0GxRQC&pg=PA128. Retrieved 13 November 2010. 
  6. "Assembly of β-barrel proteins into bacterial outer membranes". Biochimica et Biophysica Acta (BBA) - Molecular Cell Research 1843 (8): 1542–50. August 2014. doi:10.1016/j.bbamcr.2013.10.009. PMID 24135059. 
  7. "Charged residues next to transmembrane regions revisited: "Positive-inside rule" is complemented by the "negative inside depletion/outside enrichment rule"". BMC Biology 15 (1): 66. July 2017. doi:10.1186/s12915-017-0404-4. PMID 28738801. open access
  8. "Structure of the alternative complex III in a supercomplex with cytochrome oxidase". Nature 557 (7703): 123–126. May 2018. doi:10.1038/s41586-018-0061-y. PMID 29695868. Bibcode2018Natur.557..123S. 
  9. "SCOP2 prototype: a new approach to protein structure mining". Nucleic Acids Research 42 (Database issue): D310-4. January 2014. doi:10.1093/nar/gkt1242. PMID 24293656. 
  10. Liszewski, Kathy (1 October 2015). "Dissecting the Structure of Membrane Proteins". Genetic Engineering & Biotechnology News 35 (17): 1, 14, 16–17. doi:10.1089/gen.35.17.02. http://www.genengnews.com/gen-articles/dissecting-the-structure-of-membrane-proteins/5583/. 
  11. "Predicting transmembrane protein topology with a hidden Markov model: application to complete genomes". Journal of Molecular Biology 305 (3): 567–80. January 2001. doi:10.1006/jmbi.2000.4315. PMID 11152613. https://pdfs.semanticscholar.org/05e7/f7d5d5a08e0bcaca7497951c9560c546353d.pdf. open access
  12. "Global topology analysis of the Escherichia coli inner membrane proteome". Science 308 (5726): 1321–3. May 2005. doi:10.1126/science.1109730. PMID 15919996. Bibcode2005Sci...308.1321D. open access
  13. 13.0 13.1 13.2 13.3 13.4 13.5 Martin, Joseph; Sawyer, Abigail (2019). "Elucidating the Structure of Membrane Proteins". BioTechniques (Future Science) 66 (4): 167–170. doi:10.2144/btn-2019-0030. PMID 30987442. open access
  14. "Overcoming the challenges of membrane protein crystallography". Current Opinion in Structural Biology 18 (5): 581–6. October 2008. doi:10.1016/j.sbi.2008.07.001. PMID 18674618. 
  15. "Predicting transmembrane protein topology with a hidden Markov model: application to complete genomes". Journal of Molecular Biology 305 (3): 567–80. January 2001. doi:10.1006/jmbi.2000.4315. PMID 11152613. https://pdfs.semanticscholar.org/05e7/f7d5d5a08e0bcaca7497951c9560c546353d.pdf. open access
  16. "Membrane proteins: always an insoluble problem?". Biochemical Society Transactions 44 (3): 790–5. June 2016. doi:10.1042/BST20160025. PMID 27284043. 
  17. "Genetic Approach to Facilitate Purification of Recombinant Proteins with a Novel Metal Chelate Adsorbent". Nature Biotechnology 6 (11): 1321–1325. November 1988. doi:10.1038/nbt1188-1321. 
  18. "Expression, surface immobilization, and characterization of functional recombinant cannabinoid receptor CB2". Biochimica et Biophysica Acta (BBA) - Proteins and Proteomics 1834 (10): 2045–56. October 2013. doi:10.1016/j.bbapap.2013.06.003. PMID 23777860. 
  19. "Large-scale production and study of a synthetic G protein-coupled receptor: human olfactory receptor 17-4". Proceedings of the National Academy of Sciences of the United States of America 106 (29): 11925–30. July 2009. doi:10.1073/pnas.0811089106. PMID 19581598. Bibcode2009PNAS..10611925C. 

Further reading

External links

Organizations

Membrane protein databases