scientific commentaries\(\def\hfill{\hskip 5em}\def\hfil{\hskip 3em}\def\eqno#1{\hfil {#1}}\)

IUCrJ
Volume 4| Part 4| July 2017| Pages 306-307
ISSN: 2052-2525

Everyone needs good neighbours – the intricate relationship between the acetylcholine-receptor channel and its membrane environment

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aSchool of Biomedical Sciences, Faculty of Biological Sciences, University of Leeds, Leeds LS2 9JT, UK, and bAstbury Centre for Structural and Molecular Biology, University of Leeds, Leeds, LS2 9JT UK
*Correspondence e-mail: s.p.muench@leeds.ac.uk

Edited by S. S. Hasnain, University of Liverpool, England

The field of electron microscopy (EM) has undergone significant advancement in its capabilities in terms of both the resolution obtainable and the diverse range of systems that can be studied (Subramaniam et al., 2016[Subramaniam, S., Kühlbrandt, W. & Henderson, R. (2016). IUCrJ, 3, 3-7.]). A particular strength of EM has been in determining the structure of membrane proteins, which have proven to be highly challenging owing to the difficulties in overexpressing them and their instability outside of the membrane environment (Rawson et al., 2016[Rawson, S., Davies, S., Lippiat, J. D. & Muench, S. P. (2016). Mol. Membr. Biol. 33, 12-22.]). This is a significant hurdle in structure-based drug design and target validation with ∼60% of drugs targeting membrane proteins, for example G-protein coupled receptors (GPCRs), ion channels and ABC transporters (Overington et al., 2006[Overington, J. P., Al-Lazikani, B. & Hopkins, A. L. (2006). Nat. Rev. Drug Discov. 5, 993-996.]).

One of the best characterized membrane proteins is the acetyl choline (ACh) receptor, a ligand-gated ion channel which consists of a pentamer of protein subunits (β, δ, αδ, γ, αγ) (Fig. 1[link]). Through a series of landmark time-resolved EM experiments the mechanism of traversing the channel has been elucidated, whereby binding of acetyl­choline to αγ causes a displacement of β, which in turn results in an opening of the pore to allow for the passage of Na+ ions (Unwin & Fujiyoshi, 2012[Unwin, N. & Fujiyoshi, Y. (2012). J. Mol. Biol. 422, 617-634.]; Miyazawa et al., 2003[Miyazawa, A., Fujiyoshi, Y. & Unwin, N. (2003). Nature, 423, 949-955.]). This movement of charge is sufficient to initiate an action potential through depolarizing the postsynaptic membrane. However, what is more poorly understood is the role that the surrounding lipidic environment plays in the action of the ACh receptor. This has important implications as the lipid environment has been shown to be involved in catalytic cycling, transport, regulation and/or stability. For example, the β-barrel membrane protein OmpX, has been shown to have pronounced dynamic variability in different lipid environments and detergents (Frey et al., 2017[Frey, L., Lakomek, N., Riek, R. & Bibow, S. (2017). Angew. Chem. Int. Ed. 56, 380-383.]), and cardiolipin can promote dimerization of membrane proteins (Gupta et al., 2017[Gupta, K., Donlan, J. A. C., Hopper, J. T. S., Uzdavinys, P., Landreh, M., Struwe, W. B., Drew, D., Baldwin, A. J., Stansfeld, P. J. & Robinson, C. V. (2017). Nature, 541, 421-424.]). Therefore, it is becoming more important, when studying membrane proteins, that a near-native environment is maintained where possible. This can be partially achieved through approaches such as nanodiscs, which maintain a bilayer environment, or styrene maleic acid copolymers (SMALPs), which extract membrane proteins with their native lipids, but extraction in the native membrane itself is the gold standard (Gao et al., 2016[Gao, Y., Cao, E., Julius, D. & Cheng, Y. (2016). Nature, 534, 347-351.] & Lee et al., 2016[Lee, S. C., Knowles, T. J., Postis, V. L. G., Jamshad, M., Parslow, R. A., Lin, Y., Goldman, A., Sridhar, P., Overduin, M., Muench, S. P. & Dafforn, T. R. (2016). Nat. Protoc. 11, 1149-1162.]).

[Figure 1]
Figure 1
The ACh receptor housed within the membrane environment. The five different subunits are shown with an orange, yellow, green, blue and red surface (note the blue subunit is largely occluded by the other four subunits). The structure was generated from the PDB file (PDB reference: 4aq5) (Unwin & Fujiyoshi, 2012[Unwin, N. & Fujiyoshi, Y. (2012). J. Mol. Biol. 422, 617-634.]).

To this end, the study by Nigel Unwin (Unwin, 2017[Unwin, N. (2017). IUCrJ, 4, 393-399.]) in this issue of IUCrJ has advanced our understanding of the ACh receptor by imaging and reconstructing it in the unperturbed natural membrane. Through advances in the EM field, including more sensitive detectors and stable microscopes, the ACh receptor is examined in a more native environment taking account of the local lipid environment. Two-dimensional classification was used to sort the data, with the best class resulting in a final resolution of 8.4 Å. By using a single-particle helical method as opposed to a Fourier–Bessel helical method, the membrane region is better defined. This shows that in several locations, immediately adjacent to the protein surface, there is a weakening or loss of density. These low-density patches form a microdomain (∼26 Å × 11 Å) enclosed by helices M1 and M4 and polar phospho­lipid headgroups. Smaller patches are also present next to the β, αγ, γ, αδ subunits and the M1 and M4 helices. This loss of density can be attributed to the presence of cholesterol which has a much smaller headgroup than other lipids and is present in larger amounts in the native membrane (∼35 mol%), compared with smaller phospho­lipids such as phosphatidic acid. The presence of cholesterol around the ACh receptor is not a new observation, indeed it had been previously reported (Barrantes, 2010[Barrantes, F. J. (2010). Subcell. Biochem. 51, 467-487.]). However, what sets this study apart is the ability to structurally characterize the location of these rafts around the ACh receptor for the first time. But what role does cholesterol play in ACh-receptor function? It has been suggested within this study that for the β subunit to achieve an outward tilt, opening up the channel, the δ subunit must resist the force. The cholesterol-rich microdomain would reduce the free volume available for molecular motion and thus impose resistance and rigidity next to the δ subunit. This hypothesis is yet to be proven but opens up the next chapter in understanding ACh-receptor structure and function, with improved EM resolution, time-resolved studies, and the use of biochemical and mass spectrometry lipidomic analysis the role of the native lipidic environment will be better understood, providing new insights into this essential membrane protein.

References

First citationBarrantes, F. J. (2010). Subcell. Biochem. 51, 467–487.  CrossRef CAS PubMed Google Scholar
First citationFrey, L., Lakomek, N., Riek, R. & Bibow, S. (2017). Angew. Chem. Int. Ed. 56, 380–383.  CrossRef CAS Google Scholar
First citationGao, Y., Cao, E., Julius, D. & Cheng, Y. (2016). Nature, 534, 347–351.  CrossRef CAS PubMed Google Scholar
First citationGupta, K., Donlan, J. A. C., Hopper, J. T. S., Uzdavinys, P., Landreh, M., Struwe, W. B., Drew, D., Baldwin, A. J., Stansfeld, P. J. & Robinson, C. V. (2017). Nature, 541, 421–424.  CrossRef CAS PubMed Google Scholar
First citationLee, S. C., Knowles, T. J., Postis, V. L. G., Jamshad, M., Parslow, R. A., Lin, Y., Goldman, A., Sridhar, P., Overduin, M., Muench, S. P. & Dafforn, T. R. (2016). Nat. Protoc. 11, 1149–1162.  CrossRef CAS PubMed Google Scholar
First citationMiyazawa, A., Fujiyoshi, Y. & Unwin, N. (2003). Nature, 423, 949–955.  CrossRef PubMed CAS Google Scholar
First citationOverington, J. P., Al-Lazikani, B. & Hopkins, A. L. (2006). Nat. Rev. Drug Discov. 5, 993–996.  CrossRef PubMed CAS Google Scholar
First citationRawson, S., Davies, S., Lippiat, J. D. & Muench, S. P. (2016). Mol. Membr. Biol. 33, 12–22.  CrossRef CAS PubMed Google Scholar
First citationSubramaniam, S., Kühlbrandt, W. & Henderson, R. (2016). IUCrJ, 3, 3–7.  Web of Science CrossRef CAS PubMed IUCr Journals Google Scholar
First citationUnwin, N. (2017). IUCrJ, 4, 393–399.  CrossRef IUCr Journals Google Scholar
First citationUnwin, N. & Fujiyoshi, Y. (2012). J. Mol. Biol. 422, 617–634.  Web of Science CrossRef CAS PubMed Google Scholar

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IUCrJ
Volume 4| Part 4| July 2017| Pages 306-307
ISSN: 2052-2525