Filaments, fibres and muscles in transparent embryos

Gene inactivation in zebrafish defines new role for troponin T in muscle integrity

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Analysis in the sloth mutant: a 48 hpf wild-type sibling displays normally striated fast fibres (E). In a wildtype sibling injected with the tnnt3a MO (F), myofibrils undergo degradation and actin becomes diffuse. In a sloth mutant embryo (G), actin is distributed in thick filament-free sarcomere-like blocks along myofibrils. In a sloth mutant injected with tnnt3a MO (H), actin remains in blocks rather than dispersed in the cytoplasm.

A new study shows clearly that a muscle protein called troponin T has a role in the formation of muscle fibres and the maintenance of muscle integrity. In a study of gene inactivation in zebrafish, the researchers have shown that defective troponin T can lead to disintegration of muscle fibres.

Using a combination of mutation and gene-knockdown in the zebrafish, the team studied the effect of the loss of several genes at a time. The new observations mirror those seen in some human patients who lack functional troponin T.

Muscle cells are built with an elaborate architecture that enables them to coordinate contraction and to generate force. The basic unit is called a sarcomere: within this, myosin proteins ‘ratchet’ over actin to draw the muscle shorter. Other proteins and molecules, including troponins, modulate contraction and rest cycles. Troponin’s main role in mature muscle is to allow contraction to occur when Ca++ ions are released into the sarcomere as a result of nerve stimulation.

“Zebrafish have great genetics, rapid development and transparent embryos. all of which give us a great way to tease apart the workings of complicated structures such as the sarcomere.

“By adjusting the activity of genes in zebrafish, we have defined a new role for troponin T in maintaining the integrity of the muscle unit, the sarcomere. In the absence of this protein, the sarcomere self-destructs.”

Derek Stemple Senior Group Leader, from the Sanger Institute

There are three types of troponin T, which are expressed in different types of muscle. People who lack working ‘slow-twitch troponin T’ suffer muscle weakness; those who lack working ‘fast-twitch troponin T’ suffer from a disorder where fingers, hands and toes are clenched and contracted. Mutations in the third type of troponin T are associated with heart disease.

When troponin activity is lost, the normal control of actin-myosin activity goes away leading to continuous contraction, which in turn destroys the muscle fibre. The team showed that sarcomeres do not assemble properly when troponin T activity is completely removed. Paradoxically, when the researchers blocked myosin as well as troponin T activity the sarcomere structure was less disrupted and appeared more normal.

This double disruption, however, revealed a second role for troponin T, as the sarcomere structure appeared recovered but one of its components, the thin filament, was still not normal.

“We found a novel role for troponin T in assembly of a component of sarcomeres called thin filaments. Troponin T is required for the proper assembly of thin filaments and thus the production of functioning sarcomeres and hence development of effective muscle.

“The mutational tools and experimental observation from transparent embryos enabled us to detect this subtle but important role for troponin T.”

Mariella Ferrante First author on the study, former researcher at the Sanger Institute and now at the Stazione Zoologica Anton Dohrn in Naples, Italy

The tools available to zebrafish researchers allow a comprehensive and insightful study. Using gene knock-down technologies, the team also explored how disrupting the activity of a single troponin T gene in the zebrafish affects muscle development. Early development appeared normal and sarcomeres appeared largely unaffected, as zebrafish protect by having more than one troponin T gene and protein: if one is lost, another might compensate. However ultimately sarcomere organisation was impaired, causing a loss of muscle function.Mutations in troponin T in the skeletal muscle are linked to at least two human diseases: the consequences of one, Nemaline myopathy, a disease of slow-twitch muscle, resemble the effects of removing functional troponin T in zebrafish.

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Funding

This work was supported by the Wellcome Trust.

Participating Centres

  • Wellcome Trust Sanger Institute, Hinxton, Cambridge, UK

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  • The Wellcome Trust Sanger Institute

    The Wellcome Trust Sanger Institute, which receives the majority of its funding from the Wellcome Trust, was founded in 1992. The Institute is responsible for the completion of the sequence of approximately one-third of the human genome as well as genomes of model organisms and more than 90 pathogen genomes. In October 2006, new funding was awarded by the Wellcome Trust to exploit the wealth of genome data now available to answer important questions about health and disease.

  • The Wellcome Trust

    The Wellcome Trust is a global charitable foundation dedicated to achieving extraordinary improvements in human and animal health. We support the brightest minds in biomedical research and the medical humanities. Our breadth of support includes public engagement, education and the application of research to improve health. We are independent of both political and commercial interests.