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08/10/2015 17:00

New details of the transmission of stimuli in living organisms unveiled

Dagmar Baroke Abteilung Kommunikation
Paul Scherrer Institut (PSI)

    Researchers unveil new details of how cells in a living organism process stimuli. So-called G-proteins, which help conduct external stimuli that reach a cell into its interior, play a central role here. For the first time, the study shows which parts of the G-proteins are vital for their function. Researchers from the Paul Scherrer Institute PSI, ETH Zurich, the pharmaceutical company Roche and the British MRC Laboratory of Molecular Biology report their results in the journals Nature and Nature Structural and Molecular Biology.

    When we see an object, the following essentially happens: the light emanating from the object hits our eye, whereupon nerve cells transmit a signal to the brain, which the brain interprets as an image of the object. The signal transmission is triggered by the protein rhodopsin, a so-called G-protein-couple receptor. This protein in the retinal cells is activated as soon as light reaches the eye. Rhodopsin acts as a switch which, once flicked, transmits the signal to G-proteins inside the cell. These amplify the signal and relay it in the cell. Many pairs of G-protein-coupled receptors and G-proteins work in a similar way. The adrenalin receptor in muscle cells, for instance, is activated when the body releases the hormone adrenalin in a stress situation. In this case, the corresponding G-protein relays the signal, which culminates in the tensing of the muscles. A team headed by researchers from the Paul Scherrer Institute (PSI) and ETH Zurich together with the the British MRC Laboratory of Molecular Biology and the pharmaceutical company Roche provide new details of how the activation of these proteins takes place. The findings can be transferred to other processes, such as smell, taste and many more where similar proteins are involved in the signal transmission. Moreover, they could help to develop novel, improved drugs.

    Nobel Prize-winning research

    Thanks to decades of research scientists have learnt a great deal about the interplay between G-proteins and the corresponding receptors (G-protein-coupled receptors or GPCRs for short). In 1994 and 2012, for instance, Nobel Prizes were awarded for the discovery of these receptors and the clarification of their coupling mechanism with the G-proteins. The details of how the G-protein is activated, however, were not clear until now. The new study plugs this gap, revealing how the shape of G-proteins is altered during their activation and which protein components are behind these changes.

    A few components set the tone

    Like all proteins, G-proteins are made up of building blocks which experts refer to as amino acids. In proteins, these amino acids are linked to each other in a particular sequence according to a precise blueprint encoded in our DNA. The G-protein studied here is composed of 354 amino acids. In order to find out how this G-protein is activated, the authors of the study exchanged every single one of these 354 amino acids with another amino acid. They then measured how the exchange affected the degree of activation of the G-protein.

    “The analysis of the measurements reveals that only one small group of around twenty amino acids plays a major role in activating the G-protein,” explains Dawei Sun, who conducted the experiments as part of his PhD dissertation at PSI. Sure enough, only exchanging these particular amino acids had a significant influence on the activation of the G-protein, while swapping the remaining amino acids produced no significant effect. The researchers detected the influence of the essential amino acids in changes in the shape of a section of the G-protein, which resembled a rolled-out streamer (helix structure) in a deactivated state. “When the key amino acids were switched, this structure lacked its usual twists,” explains Dmitry Veprintsev, the leading researcher on the study at PSI’s Laboratory of Biomolecular Research. “This enabled us to demonstrate that the helix structure disappears at least temporarily during the activation of the G-protein,” adds Veprintsev.

    Useful for almost one in three drugs

    The significance of this result is not limited to one single protein: the newly discovered mechanism is universal. In other words, it is not only involved in the particular G-protein examined in this study, but rather in all G-proteins. This conclusion is supported by extensive computer calculations conducted by a team led by Madan Babu from the MRC Laboratory of Molecular Biology and recently published in the journal Nature. Veprintsev stresses that the present study has identified the essential amino acids that play a role in the activation mechanism of a G-protein. Gebhard Schertler, the head of the Biology and Chemistry Research Department at PSI, explains that this knowledge significantly aids the development of drugs that function through the activation of a GPCR receptor and the corresponding G-protein. The potential benefit is not to be underestimated: today, around 30 per cent of all available drugs already unleash their effect in this way. Moreover, the consequences could go beyond the G-proteins. “Our method can be applied in future to other important proteins to understand their activation mechanism,” assures Veprintsev.

    Text: Paul Scherrer Institute/Leonid Leiva

    About PSI

    The Paul Scherrer Institute PSI develops, builds and operates large, complex research facilities and makes them available to the national and international research community. The institute's own key research priorities are in the fields of matter and materials, energy and environment and human health. PSI is committed to the training of future generations. Therefore about one quarter of our staff are post-docs, post-graduates or apprentices. Altogether PSI employs 1900 people, thus being the largest research institute in Switzerland. The annual budget amounts to approximately CHF 350 million.

    Contact:
    Dr Dmitry Veprintsev, Projektleiter, Laboratory of Biomolecular Research
    Paul Scherrer Institute,
    Telephone: +41 (0)56 310 5246
    E-Mail: dmitry.veprintsev@psi.ch

    Dr Gregor Cicchetti
    Scientific Relations Manager
    Biology and Chemistry Research Department
    Telephone: +41 (0)56 310 5382
    E-Mail: gregor.cicchetti@psi.ch

    Original publication

    Probing Gαi1 protein activation at single–amino acid resolution
    Dawei Sun, Tilman Flock, Xavier Deupi, Shoji Maeda, Milos Matkovic, Sandro Mendieta, Daniel Mayer, Roger Dawson, Gebhard F.X. Schertler, M. Madan Babu, Dmitry Veprintsev
    Nature Structural & Molecular Biology, 10 August 2015
    http://nature.com/articles/doi:10.1038/nsmb.3070


    More information:

    http://psi.ch/8ZA5 Text of the press release with pictures
    http://www.psi.ch/lbr Laboratory of Biomolecular Research at PSI


    Images

    The study’s leading researcher Dmitry Veprintsev in one of PSI’s labs, where the G-proteins are prepared for the measurements.
    The study’s leading researcher Dmitry Veprintsev in one of PSI’s labs, where the G-proteins are prep ...
    Paul Scherrer Institute/Mahir Dzambegovic.
    None

    Simplified depiction of the structure of the G-protein studied (in grey) and the receptor coupled to it. The spheres represent the amino acids that are crucial for the activation of the G-protein.
    Simplified depiction of the structure of the G-protein studied (in grey) and the receptor coupled to ...
    Dawei Sun
    None


    Criteria of this press release:
    Journalists
    Biology, Chemistry, Medicine
    transregional, national
    Research results, Scientific Publications
    English


     

    The study’s leading researcher Dmitry Veprintsev in one of PSI’s labs, where the G-proteins are prepared for the measurements.


    For download

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    Simplified depiction of the structure of the G-protein studied (in grey) and the receptor coupled to it. The spheres represent the amino acids that are crucial for the activation of the G-protein.


    For download

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