Sandbox Reserved 1092
From Proteopedia
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=5JI1 : Myostatin (GDF8)= | =5JI1 : Myostatin (GDF8)= | ||
| - | + | Myostatin was discovered in '''1997''' by geneticists Se-Jin Lee and Alexandra McPherron <ref name="Myostatin">Wikipedia. Myostatin. [https://en.wikipedia.org/wiki/Myostatin]</ref> who demonstrated that a phenotype of exaggerated muscle hypertrophy correlated with mutations in the myostatin gene. It was at first associated with the role it played in the regulation of muscular mass of mice. This new growth factor since then been completely sequenced, and the primary sequences obtained in different animals have been compared. The results showed that there were an '''important correlation''' between the sequences, whatever their origin. <ref name="Structure and synthesis"> Université de Montpellier. Physiologie expérimentale du coeur et des muscles : la myostatine/partenaires de la myostatine. [https://u1046.edu.umontpellier.fr/163-2/abrege-des-proteines-musculaires/myostatine/]</ref> | |
==Classification== | ==Classification== | ||
| - | This protein was firstly named '''Growth/Differentiation Factor 8 (GDF8)''' because it belongs to the group of growth factors. Growth factors constitute a group of proteins that regulate the number of cells, increasing or decreasing their multiplication according to the needs. Then the nomenclature changed and, nowadays, we refer to myostatine as '''MSTN'''. Progressively, the myostatin has been affiliated to the '''TGF-beta family''' (transforming growth factor beta). | + | This protein was firstly named '''Growth/Differentiation Factor 8 (GDF8)''' because it belongs to the group of growth factors. Growth factors constitute a group of proteins that regulate the number of cells, increasing or decreasing their multiplication according to the needs. Then the nomenclature changed and, nowadays, we refer to myostatine as '''MSTN'''. Progressively, the myostatin has been affiliated to the '''TGF-beta family''' (transforming growth factor beta) <ref name="Structure and synthesis"> Université de Montpellier. Physiologie expérimentale du coeur et des muscles : la myostatine/partenaires de la myostatine. [https://u1046.edu.umontpellier.fr/163-2/abrege-des-proteines-musculaires/myostatine/]</ref>. |
= Function <ref name="patho"/>= | = Function <ref name="patho"/>= | ||
| - | Myostatin is a strong '''endogenous, negative regulator of muscle growth''' determining both '''muscle fiber number and size.''' The number of fibers is | + | Myostatin is a strong '''endogenous, negative regulator of muscle growth''' determining both '''muscle fiber number and size.''' The number of fibers is defined during the development of the animal while their size changes while they live, depending on '''activity, nutrition and aging.''' Myostatin acts on this by providing regulation on the growth of muscles. It has been found first in mice which, having their gene encoding for myostatin '''knocked-out''', developed overgrowth of muscles, due to '''hyperplasia and hypertrophy''', which effects are persistent throughout the life of animals. |
Therefore, myostatin appears to act at the level of fiber number during '''embryogenesis''' and its growth in '''adult life.''' | Therefore, myostatin appears to act at the level of fiber number during '''embryogenesis''' and its growth in '''adult life.''' | ||
==Myostatin processing and signal transduction <ref name="patho"/>== | ==Myostatin processing and signal transduction <ref name="patho"/>== | ||
| - | The mechanism of myostatin action is similar to those of the members of '''TGF-beta family.''' The mature peptide binds to one of the two '''activin type II receptors''' which recruits phosphorylates and activates the activin type I receptor, propagating signals along the '''Smad''' pathway. (Smad are receptor-associated proteins) | + | The mechanism of myostatin action is similar to those of the members of '''TGF-beta family.''' The mature peptide binds to one of the two '''activin type II receptors''' which recruits, phosphorylates and activates the activin type I receptor, propagating signals along the '''Smad''' pathway. (Smad are receptor-associated proteins) |
'''Phosphorylated Smad2 and 3''' form heterodimeric complex with '''Smad4'''(common mediator) and they activate the functions of the smad as '''mediators''' of signalling for myostatin : translocating into the '''nucleus''' and activating the transcription of the target genes (through interaction with DNA and other nuclear factors). | '''Phosphorylated Smad2 and 3''' form heterodimeric complex with '''Smad4'''(common mediator) and they activate the functions of the smad as '''mediators''' of signalling for myostatin : translocating into the '''nucleus''' and activating the transcription of the target genes (through interaction with DNA and other nuclear factors). | ||
==Inhibition of myostatin’s function<ref name="patho"/>== | ==Inhibition of myostatin’s function<ref name="patho"/>== | ||
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Some of them (propeptide, follistatin and FLRG) are able to '''increase muscle mass''' when expressed as a transgene in skeletal muscle of wild-type mice. | Some of them (propeptide, follistatin and FLRG) are able to '''increase muscle mass''' when expressed as a transgene in skeletal muscle of wild-type mice. | ||
The increase in muscle mass is greater in follistatin transgenics than in the myostatin null mice and when both are combined, the increase of muscle mass is quadrupled. Therefore, it has been deduced that other ligands cooperate with myostatin to control muscle growth. | The increase in muscle mass is greater in follistatin transgenics than in the myostatin null mice and when both are combined, the increase of muscle mass is quadrupled. Therefore, it has been deduced that other ligands cooperate with myostatin to control muscle growth. | ||
| + | ==Myostatin and satellite cells <ref name="patho"/> == | ||
| + | Satellite cells’ main role concerns the repair of skeletal muscles. | ||
| + | They are activated and proliferate then to respond to tissue damage. | ||
| + | However a small part doesn’t differentiate and return to quiescence to maintain the pool of satellite cells. | ||
| + | This is where myostatin steps in : it represents a key molecule signalling the quiescence of satellite cells. | ||
| + | In myostatin mutant mouse the number of satellite cells increases a lot compared to non mutated mice. | ||
| + | Basically, myostatin maintains satellite cells in a quiescent state during regeneration or muscle growth. | ||
| + | And so, it negatively regulates muscle regeneration after injury. | ||
= Structure and synthesis <ref name="Structure and synthesis"> Université de Montpellier. Physiologie expérimentale du coeur et des muscles : la myostatine/partenaires de la myostatine. [https://u1046.edu.umontpellier.fr/163-2/abrege-des-proteines-musculaires/myostatine/]</ref> = | = Structure and synthesis <ref name="Structure and synthesis"> Université de Montpellier. Physiologie expérimentale du coeur et des muscles : la myostatine/partenaires de la myostatine. [https://u1046.edu.umontpellier.fr/163-2/abrege-des-proteines-musculaires/myostatine/]</ref> = | ||
Current revision
| This Sandbox is Reserved from 25/11/2019, through 30/9/2020 for use in the course "Structural Biology" taught by Bruno Kieffer at the University of Strasbourg, ESBS. This reservation includes Sandbox Reserved 1091 through Sandbox Reserved 1115. |
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