Troponin C type 1 explained

Troponin C, also known as TN-C or TnC, is a protein that resides in the troponin complex on actin thin filaments of striated muscle (cardiac, fast-twitch skeletal, or slow-twitch skeletal) and is responsible for binding calcium to activate muscle contraction.[1] [2] Troponin C is encoded by the TNNC1 gene in humans[3] for both cardiac and slow skeletal muscle.

Structure

Cardiac troponin C (cTnC) is a 161-amino acid protein[4] organized into two domains: the regulatory N-terminal domain (cNTnC, residues 1-86), the structural C-terminal domain (cCTnC, residues 93-161), and a flexible linker connecting the two domains (residues 87-92).[5] Each domain contains two EF-hands, Ca2+-binding helix-loop-helix motifs exemplified by proteins like parvalbumin[6] and calmodulin.[7] In cCTnC the two EF-hand motifs constitute two high affinity Ca2+-binding sites.[8] that are occupied at all physiologically relevant calcium concentrations. In contrast, only the second EF-hand in cNTnC binds Ca2+ with low affinity, while the first EF-hand Ca2+-binding site is defunct.[9]

In a typical EF-hand protein like calmodulin, Ca2+ binding induces a closed-to-open conformational transition, exposing a large hydrophobic patch in the open state.[10] Likewise, the cardiac troponin regulatory domain, cNTnC, is in a closed conformation in the apo state (no calcium bound).[11] Upon Ca2+ binding, cNTnC enters into a rapid equilibrium between closed and open forms, however, the closed form still predominates.[5] [12] [13] The structural domain, cCTnC, exists as a "molten globule" in the apo state,[14] but forms a well structured open conformation in the Ca2+-bound state. These structural differences change the relative stabilities of the apo- and Ca2+-bound states, accounting for the divergent Ca2+-binding affinities between the two domains.

Function

In cardiac muscle, cTnC binds to cardiac troponin I (cTnI) and cardiac troponin T (cTnT), whereas cTnC binds to slow skeletal troponin I (ssTnI) and troponin T (ssTnT) in slow-twitch skeletal muscle.

The structural domain of cTnC (cCTnC) is anchored to troponin I and T, forming the so-called IT arm, made up of cTnC93-161, cTnI41-135 and cTnT235-286 (in the cardiac complex).[15] cCTnC binds to helical cTnI41-60 via its large hydrophobic patch, stabilizing the Ca2+-bound open conformation of cCTnC and enhancing its affinity for Ca2+ (from Kd = 40 nM to Kd = 3 nM).[16] [17] cTnT235-286 forms a helical coiled coil with cTnI88-135 that binds to the opposite face of cCTnC.[15] The IT arm is anchored to tropomyosin via adjacent segments of cTnT,[18] [19] [20] so it is believed to move as a unit along with tropomyosin throughout the cardiac cycle.[21] In the low calcium environment present during diastole (~100 nM),[22] tropomyosin is anchored into the "blocked" position along the actin thin filament through the binding of the troponin I inhibitory (cTnI128-147) and C-terminal (cTnI160-209) regions.[23] [24] This prevents actin-myosin cross-bridging and effectively shuts off muscle contraction.

As the cytoplasmic Ca2+ concentration rises to ~1 μM during systole,[22] Ca2+ binding to the regulatory domain of cardiac troponin C (cNTnC) is the key event that leads to muscle contraction. Hydrophobic binding of cNTnC to the "switch" region of troponin I, cTnI148-159, stabilizes the Ca2+-bound open conformation of cNTnC[25] (increasing the Ca2+ binding affinity of cNTnC from about Kd = 5 μM to Kd = 0.8 μM).[26] This binding event removes the adjacent cTnI inhibitory regions from actin and stabilizes tropomyosin in its default "closed" position on the thin filament,[27] allowing actin-myosin cross-bridging and muscle contraction to proceed. Strong actin-myosin interaction can further shift the thin filament into the "open" position.[28] [29]

Physiologic regulation of calcium sensitivity

The calcium sensitivity of the sarcomere, that is, the calcium concentration at which muscle contraction occurs, is directly determined by the calcium binding affinity of cNTnC. To date, there are no known post-translational modifications of cTnC that impact its calcium binding affinity. However, calcium binding by cNTnC is a dynamic process that can be impacted by the closed-to-open conformational equilibrium of cNTnC, the domain positioning of cNTnC, or the relative availability of cTnI148-159, the physiologic binding partner of cNTnC. The closed-to-open equilibrium of cNTnC can be shifted towards the open state by small compounds [30] (see section below on troponin-binding drugs). Domain positioning of cNTnC can be impacted by phosphorylation of cTnI,[31] of which the most important site in humans is Ser22/Ser23.[32] [33] The availability of cTnI148-159 depends on the blocked-closed-open equilibrium of tropomyosin on actin, which can be impacted by any interactions involving the thin filament, including actin-myosin cross-bridging[34] and length dependent activation [35] [36] (also known as stretch activation or the Frank Starling law of the heart). All of these processes can be impacted by mutations (see section below on disease-causing mutations).

Disease-causing mutations

Hypertrophic cardiomyopathy (HCM) is a common condition (prevalence >1:500)[37] characterized by abnormal thickening of the ventricular muscle, classically in the intraventricular septal wall. HCM is described as a disease of the sarcomere, because mutations in the contractile proteins of the sarcomere have been identified in about half of patients with HCM. The cTnC mutations that have been associated with HCM are A8V, L29Q, A31S, C84Y, D145E.[38] [39] [40] In all cases, the mutation was identified in a single patient, so additional genetic testing is needed to confirm or refute the clinical significance of these mutations. With most of these mutations (and with HCM-associated thin filament mutations in general), an increase in cardiac calcium sensitivity has been observed.[41] [42]

Familial dilated cardiomyopathy (DCM) is a rare cause of systolic heart failure (prevalence 1:5000). A wider range of mutations (including some non-sarcomeric proteins as well) is associated with DCM. The cTnC mutations associated with DCM thus far are Y5H, Q50R, D75Y, M103I, D145E (also associated with HCM), I148V, and G159D.[43] [44] Of these, Q50R[45] and G159D[46] co-segregated with disease in affected family members, increasing confidence that they are clinically significant mutations. The biochemical consequences of thin filament DCM-associated mutations are less well established than for HCM, although there has been some suggestion that some of the mutations abolish the calcium desensitizing effect of cTnI phosphorylation at Ser22/23.[47] This may be because some mutations disrupt the precise positioning of cNTnC for triggering muscle contraction when cTnI is unphosphorylated.[48]

Troponin-binding drugs

Chemical compounds can bind to troponin C to act as troponin activators (calcium sensitizers) or troponin inhibitors (calcium desensitizers). There are already multiple troponin activators that bind to fast skeletal troponin C, of which tirasemtiv[49] has been tested in multiple clinical trials.[50] [51] [52] In contrast, there are no known compounds that bind with high affinity to cardiac troponin C. The calcium sensitizer, levosimendan, is purported to bind to troponin C, but only weak or inconsistent binding has been detected,[53] [54] [55] precluding any structure determination. In contrast, levosimendan inhibits type 3 phosphodiesterase with nanomolar affinity,[56] so its biological target is controversial.[57]

Some compounds have been identified to bind cNTnC with low affinity and act as troponin activators: DFBP-O[58] (a structural analog of levosimendan), 4-(4-(2,5-dimethylphenyl)-1-piperazinyl)-3-pyridinamine (NCI147866),[59] and bepridil.[60] The calmodulin antagonist, W7, has also been found to bind to cNTnC to act as a troponin inhibitor.[61] All of these compounds bind to the hydrophobic patch in the open conformation of cNTnC, with troponin activators promoting interaction with the cTnI switch peptide and troponin inhibitors destabilizing the interaction.

A number of compounds can also bind to cCTnC with low affinity: EMD 57033,[62] resveratrol,[63] bepridil,[64] and EGCG.[65] All of these compounds are renowned for their promiscuity, and the biological significance of these interactions is unknown. In particular, it is unknown how interaction with cCTnC influences the calcium affinity of cNTnC.

Theoretically, a cardiac troponin activator could be useful for increasing cardiac contractility in the treatment of systolic heart failure, whereas a troponin inhibitor could be used to favor relaxation in the treatment of diastolic heart failure. Troponin modulators could also be used to reverse the impact of cardiomyopathy-causing mutations in the thin filament.

External links

Notes and References

  1. Schreier T, Kedes L, Gahlmann R . Cloning, structural analysis, and expression of the human slow twitch skeletal muscle/cardiac troponin C gene . The Journal of Biological Chemistry . 265 . 34 . 21247–53 . Dec 1990 . 10.1016/S0021-9258(17)45353-1 . 2250022 . free .
  2. Townsend PJ, Yacoub MH, Barton PJ . Assignment of the human cardiac/slow skeletal muscle troponin C gene (TNNC1) between D3S3118 and GCT4B10 on the short arm of chromosome 3 by somatic cell hybrid analysis . Annals of Human Genetics . 61 . Pt 4 . 375–7 . Jul 1997 . 9365790 . 10.1046/j.1469-1809.1997.6140375.x . 2997137 .
  3. Web site: Entrez Gene: TNNC1 troponin C type 1 (slow).
  4. Web site: Troponin C, slow skeletal and cardiac muscles . Cardiac Organellar Protein Atlas Knowledgebase (COPaKB) — Protein Information . 2015-03-15 . 2015-09-24 . https://web.archive.org/web/20150924025540/http://www.heartproteome.org/copa/ProteinInfo.aspx?QType=Protein%20ID&QValue=P63316 . dead .
  5. Sia SK, Li MX, Spyracopoulos L, Gagné SM, Liu W, Putkey JA, Sykes BD . Structure of cardiac muscle troponin C unexpectedly reveals a closed regulatory domain . The Journal of Biological Chemistry . 272 . 29 . 18216–21 . Jul 1997 . 9218458 . 10.1074/jbc.272.29.18216. free .
  6. Kretsinger RH, Nockolds CE . Carp muscle calcium-binding protein. II. Structure determination and general description . The Journal of Biological Chemistry . 248 . 9 . 3313–26 . May 1973 . 10.1016/S0021-9258(19)44043-X . 4700463 . free .
  7. Strynadka NC, James MN . Crystal structures of the helix-loop-helix calcium-binding proteins . Annual Review of Biochemistry . 58 . 1 . 951–999 . June 1989 . 2673026 . 10.1146/annurev.bi.58.070189.004511 .
  8. Li MX, Saude EJ, Wang X, Pearlstone JR, Smillie LB, Sykes BD . Kinetic studies of calcium and cardiac troponin I peptide binding to human cardiac troponin C using NMR spectroscopy . European Biophysics Journal . 31 . 4 . 245–256 . Jul 2002 . 12122471 . 10.1007/s00249-002-0227-1 . 23676865 .
  9. van Eerd JP, Takahashi K . The amino acid sequence of bovine cardiac tamponin-C. Comparison with rabbit skeletal troponin-C . Biochemical and Biophysical Research Communications . 64 . 1 . 122–7 . May 1975 . 1170846 . 10.1016/0006-291x(75)90227-2.
  10. Gifford JL, Walsh MP, Vogel HJ . Structures and metal-ion-binding properties of the Ca2+-binding helix-loop-helix EF-hand motifs . The Biochemical Journal . 405 . 2 . 199–221 . Jul 2007 . 17590154 . 10.1042/BJ20070255 . 11770498 .
  11. Spyracopoulos L, Li MX, Sia SK, Gagné SM, Chandra M, Solaro RJ, Sykes BD . Calcium-induced structural transition in the regulatory domain of human cardiac troponin C . Biochemistry . 36 . 40 . 12138–46 . Oct 1997 . 9315850 . 10.1021/bi971223d . 6509305 .
  12. Eichmüller C, Skrynnikov NR . A new amide proton R1rho experiment permits accurate characterization of microsecond time-scale conformational exchange . Journal of Biomolecular NMR . 32 . 4 . 281–293 . Aug 2005 . 16211482 . 10.1007/s10858-005-0658-y . 44304061 .
  13. Cordina NM, Liew CK, Gell DA, Fajer PG, Mackay JP, Brown LJ . Effects of calcium binding and the hypertrophic cardiomyopathy A8V mutation on the dynamic equilibrium between closed and open conformations of the regulatory N-domain of isolated cardiac troponin C . Biochemistry . 52 . 11 . 1950–1962 . Mar 2013 . 23425245 . 10.1021/bi4000172 .
  14. Brito RM, Krudy GA, Negele JC, Putkey JA, Rosevear PR . Calcium plays distinctive structural roles in the N- and C-terminal domains of cardiac troponin C . The Journal of Biological Chemistry . 268 . 28 . 20966–73 . Oct 1993 . 10.1016/S0021-9258(19)36880-2 . 8407932 . free .
  15. Takeda S, Yamashita A, Maeda K, Maéda Y . Structure of the core domain of human cardiac troponin in the Ca(2+)-saturated form . Nature . 424 . 6944 . 35–41 . Jul 2003 . 12840750 . 10.1038/nature01780 . 2003Natur.424...35T . 2174019 .
  16. Johnson JD, Potter JD . Detection of two classes of Ca2+ binding sites in troponin C with circular dichroism and tyrosine fluorescence . The Journal of Biological Chemistry . 253 . 11 . 3775–7 . Jun 1978 . 10.1016/S0021-9258(17)34754-3 . 649605 . free .
  17. Johnson JD, Collins JH, Robertson SP, Potter JD . A fluorescent probe study of Ca2+ binding to the Ca2+-specific sites of cardiac troponin and troponin C . The Journal of Biological Chemistry . 255 . 20 . 9635–40 . Oct 1980 . 10.1016/S0021-9258(18)43439-4 . 7430090 . free .
  18. Pearlstone JR, Smillie LB . Identification of a second binding region on rabbit skeletal troponin-T for alpha-tropomyosin . FEBS Letters . 128 . 1 . 119–22 . Jun 1981 . 7274451 . 10.1016/0014-5793(81)81095-2. 85355424 .
  19. Jin JP, Chong SM . Localization of the two tropomyosin-binding sites of troponin T . Archives of Biochemistry and Biophysics . 500 . 2 . 144–150 . Aug 2010 . 20529660 . 10.1016/j.abb.2010.06.001 . 2904419.
  20. Tanokura M, Ohtsuki I . Interactions among chymotryptic troponin T subfragments, tropomyosin, troponin I and troponin C . Journal of Biochemistry . 95 . 5 . 1417–21 . May 1984 . 6746613 . 10.1093/oxfordjournals.jbchem.a134749 .
  21. Sevrieva I, Knowles AC, Kampourakis T, Sun YB . Regulatory domain of troponin moves dynamically during activation of cardiac muscle . Journal of Molecular and Cellular Cardiology . 75 . 181–7 . Oct 2014 . 25101951 . 10.1016/j.yjmcc.2014.07.015 . 4169182.
  22. Bers DM . Calcium fluxes involved in control of cardiac myocyte contraction . Circulation Research . 87 . 4 . 275–81 . Aug 2000 . 10948060 . 10.1161/01.res.87.4.275. free .
  23. Tripet B, Van Eyk JE, Hodges RS . Mapping of a second actin-tropomyosin and a second troponin C binding site within the C terminus of troponin I, and their importance in the Ca2+-dependent regulation of muscle contraction . Journal of Molecular Biology . 271 . 5 . 728–50 . Sep 1997 . 9299323 . 10.1006/jmbi.1997.1200 .
  24. Ramos CH . Mapping subdomains in the C-terminal region of troponin I involved in its binding to troponin C and to thin filament . The Journal of Biological Chemistry . 274 . 26 . 18189–95 . Jun 1999 . 10373418 . 10.1074/jbc.274.26.18189. free .
  25. Li MX, Spyracopoulos L, Sykes BD . Binding of cardiac troponin-I147-163 induces a structural opening in human cardiac troponin-C . Biochemistry . 38 . 26 . 8289–98 . Jun 1999 . 10387074 . 10.1021/bi9901679 .
  26. Davis JP, Norman C, Kobayashi T, Solaro RJ, Swartz DR, Tikunova SB . Effects of thin and thick filament proteins on calcium binding and exchange with cardiac troponin C . Biophysical Journal . 92 . 9 . 3195–3206 . May 2007 . 17293397 . 10.1529/biophysj.106.095406 . 1852344. 2007BpJ....92.3195D .
  27. von der Ecken J, Müller M, Lehman W, Manstein DJ, Penczek PA, Raunser S . Structure of the F-actin-tropomyosin complex . Nature . 519 . 7541 . 114–117 . Mar 2015 . 25470062 . 10.1038/nature14033 . 4477711. 2015Natur.519..114V .
  28. Behrmann E, Müller M, Penczek PA, Mannherz HG, Manstein DJ, Raunser S . Structure of the rigor actin-tropomyosin-myosin complex . Cell . 150 . 2 . 327–38 . Jul 2012 . 22817895 . 10.1016/j.cell.2012.05.037 . 4163373.
  29. von der Ecken J, Heissler SM, Pathan-Chhatbar S, Manstein DJ, Raunser S . Cryo-EM structure of a human cytoplasmic actomyosin complex at near-atomic resolution . Nature . 534 . 7609 . 724–28 . Jun 2016 . 27324845 . 10.1038/nature18295 . 2016Natur.534..724E . 4472407 .
  30. Hwang PM, Sykes BD . Targeting the sarcomere to correct muscle function . Nature Reviews. Drug Discovery . Apr 2015 . 25881969 . 10.1038/nrd4554 . 14 . 5 . 313–28. 21888079 .
  31. Hwang PM, Cai F, Pineda-Sanabria SE, Corson DC, Sykes BD . The cardiac-specific N-terminal region of troponin I positions the regulatory domain of troponin C . Proceedings of the National Academy of Sciences of the United States of America . 111 . 40 . 14412–14417 . Oct 2014 . 25246568 . 10.1073/pnas.1410775111 . 4210035. 2014PNAS..11114412H . free .
  32. Zhang J, Guy MJ, Norman HS, Chen YC, Xu Q, Dong X, Guner H, Wang S, Kohmoto T, Young KH, Moss RL, Ge Y . Top-down quantitative proteomics identified phosphorylation of cardiac troponin I as a candidate biomarker for chronic heart failure . Journal of Proteome Research . 10 . 9 . 4054–65 . Sep 2011 . 21751783 . 10.1021/pr200258m . 3170873.
  33. Kobayashi T, Yang X, Walker LA, Van Breemen RB, Solaro RJ . A non-equilibrium isoelectric focusing method to determine states of phosphorylation of cardiac troponin I: identification of Ser-23 and Ser-24 as significant sites of phosphorylation by protein kinase C . Journal of Molecular and Cellular Cardiology . 38 . 1 . 213–8 . Jan 2005 . 15623438 . 10.1016/j.yjmcc.2004.10.014 .
  34. Rieck DC, Li KL, Ouyang Y, Solaro RJ, Dong WJ . Structural basis for the in situ Ca(2+) sensitization of cardiac troponin C by positive feedback from force-generating myosin cross-bridges . Archives of Biochemistry and Biophysics . 537 . 2 . 198–209 . Sep 2013 . 23896515 . 10.1016/j.abb.2013.07.013 . 3836555.
  35. Wijnker PJ, Sequeira V, Foster DB, Li Y, Dos Remedios CG, Murphy AM, Stienen GJ, van der Velden J . Length-dependent activation is modulated by cardiac troponin I bisphosphorylation at Ser23 and Ser24 but not by Thr143 phosphorylation . American Journal of Physiology. Heart and Circulatory Physiology . 306 . 8 . H1171–81 . Apr 2014 . 24585778 . 10.1152/ajpheart.00580.2013 . 3989756.
  36. Wijnker PJ, Sequeira V, Witjas-Paalberends ER, Foster DB, dos Remedios CG, Murphy AM, Stienen GJ, van der Velden J . Phosphorylation of protein kinase C sites Ser42/44 decreases Ca(2+)-sensitivity and blunts enhanced length-dependent activation in response to protein kinase A in human cardiomyocytes . Archives of Biochemistry and Biophysics . 554 . 11–21 . Jul 2014 . 24814372 . 10.1016/j.abb.2014.04.017 . 4121669.
  37. Semsarian C, Ingles J, Maron MS, Maron BJ . New Perspectives on the Prevalence of Hypertrophic Cardiomyopathy . Journal of the American College of Cardiology . 65 . 12 . 1249–1254 . Mar 2015 . 25814232 . 10.1016/j.jacc.2015.01.019 . free .
  38. Parvatiyar MS, Landstrom AP, Figueiredo-Freitas C, Potter JD, Ackerman MJ, Pinto JR . A mutation in TNNC1-encoded cardiac troponin C, TNNC1-A31S, predisposes to hypertrophic cardiomyopathy and ventricular fibrillation . The Journal of Biological Chemistry . 287 . 38 . 31845–55 . Sep 2012 . 22815480 . 10.1074/jbc.M112.377713 . 3442518. free .
  39. Landstrom AP, Parvatiyar MS, Pinto JR, Marquardt ML, Bos JM, Tester DJ, Ommen SR, Potter JD, Ackerman MJ . Molecular and functional characterization of novel hypertrophic cardiomyopathy susceptibility mutations in TNNC1-encoded troponin C . Journal of Molecular and Cellular Cardiology . 45 . 2 . 281–288 . Aug 2008 . 18572189 . 10.1016/j.yjmcc.2008.05.003 . 2627482.
  40. Hoffmann B, Schmidt-Traub H, Perrot A, Osterziel KJ, Gessner R . First mutation in cardiac troponin C, L29Q, in a patient with hypertrophic cardiomyopathy . Human Mutation . 17 . 6 . 524 . Jun 2001 . 11385718 . 10.1002/humu.1143 . 28579333 . free .
  41. Willott RH, Gomes AV, Chang AN, Parvatiyar MS, Pinto JR, Potter JD . Mutations in Troponin that cause HCM, DCM AND RCM: what can we learn about thin filament function? . Journal of Molecular and Cellular Cardiology . 48 . 5 . 882–892 . May 2010 . 19914256 . 10.1016/j.yjmcc.2009.10.031 .
  42. Chang AN, Parvatiyar MS, Potter JD . Troponin and cardiomyopathy . Biochemical and Biophysical Research Communications . 369 . 1 . 74–81 . Apr 2008 . 18157941 . 10.1016/j.bbrc.2007.12.081 .
  43. Lim CC, Yang H, Yang M, Wang CK, Shi J, Berg EA, Pimentel DR, Gwathmey JK, Hajjar RJ, Helmes M, Costello CE, Huo S, Liao R . A novel mutant cardiac troponin C disrupts molecular motions critical for calcium binding affinity and cardiomyocyte contractility . Biophysical Journal . 94 . 9 . 3577–89 . May 2008 . 18212018 . 10.1529/biophysj.107.112896 . 2292379. 2008BpJ....94.3577L .
  44. Hershberger RE, Norton N, Morales A, Li D, Siegfried JD, Gonzalez-Quintana J . Coding sequence rare variants identified in MYBPC3, MYH6, TPM1, TNNC1, and TNNI3 from 312 patients with familial or idiopathic dilated cardiomyopathy . Circulation: Cardiovascular Genetics . 3 . 2 . 155–161 . Apr 2010 . 20215591 . 10.1161/CIRCGENETICS.109.912345 . 2908892.
  45. van Spaendonck-Zwarts KY, van Tintelen JP, van Veldhuisen DJ, van der Werf R, Jongbloed JD, Paulus WJ, Dooijes D, van den Berg MP . Peripartum cardiomyopathy as a part of familial dilated cardiomyopathy . Circulation . 121 . 20 . 2169–2175 . May 2010 . 20458010 . 10.1161/CIRCULATIONAHA.109.929646 . free .
  46. Mogensen J, Murphy RT, Shaw T, Bahl A, Redwood C, Watkins H, Burke M, Elliott PM, McKenna WJ . Severe disease expression of cardiac troponin C and T mutations in patients with idiopathic dilated cardiomyopathy . Journal of the American College of Cardiology . 44 . 10 . 2033–2040 . Nov 2004 . 15542288 . 10.1016/j.jacc.2004.08.027 . free .
  47. Memo M, Leung MC, Ward DG, dos Remedios C, Morimoto S, Zhang L, Ravenscroft G, McNamara E, Nowak KJ, Marston SB, Messer AE . Familial dilated cardiomyopathy mutations uncouple troponin I phosphorylation from changes in myofibrillar Ca²⁺ sensitivity . Cardiovascular Research . 99 . 1 . 65–73 . Jul 2013 . 23539503 . 10.1093/cvr/cvt071 . free .
  48. Hwang PM, Cai F, Pineda-Sanabria SE, Corson DC, Sykes BD . The cardiac-specific N-terminal region of troponin I positions the regulatory domain of troponin C . Proceedings of the National Academy of Sciences of the United States of America . 111 . 40 . 14412–14417 . Oct 2014 . 25246568 . 10.1073/pnas.1410775111 . 4210035. 2014PNAS..11114412H . free .
  49. Russell AJ, Hartman JJ, Hinken AC, Muci AR, Kawas R, Driscoll L, Godinez G, Lee KH, Marquez D, Browne WF, Chen MM, Clarke D, Collibee SE, Garard M, Hansen R, Jia Z, Lu PP, Rodriguez H, Saikali KG, Schaletzky J, Vijayakumar V, Albertus DL, Claflin DR, Morgans DJ, Morgan BP, Malik FI . Activation of fast skeletal muscle troponin as a potential therapeutic approach for treating neuromuscular diseases . Nature Medicine . 18 . 3 . 452–455 . Mar 2012 . 22344294 . 10.1038/nm.2618 . 3296825.
  50. Shefner JM, Wolff AA, Meng L . The relationship between tirasemtiv serum concentration and functional outcomes in patients with ALS . Amyotrophic Lateral Sclerosis & Frontotemporal Degeneration . 14 . 7–8 . 582–5 . Dec 2013 . 23952600 . 10.3109/21678421.2013.817587 . 25563161 .
  51. Bauer TA, Wolff AA, Hirsch AT, Meng LL, Rogers K, Malik FI, Hiatt WR. William R. Hiatt . Effect of tirasemtiv, a selective activator of the fast skeletal muscle troponin complex, in patients with peripheral artery disease . Vascular Medicine . 19 . 4 . 297–306 . May 2014 . 24872402 . 10.1177/1358863X14534516 . 25185883 . free .
  52. Sanders DB, Rosenfeld J, Dimachkie MM, Meng L, Malik FI, Andrews J, Barohn R, Corse A, Deboo A, Felice K, Harati Y, Heiman-Patterson T, Howard JF, Jackson C, Juel V, Katz J, Lee J, Massey J, McVey A, Mozaffar T, Pasnoor M, Small G, So Y, Wang AK, Weinberg D, Wolff AA . A double-blinded, randomized, placebo-controlled trial to evaluate efficacy, safety, and tolerability of single doses of tirasemtiv in patients with acetylcholine receptor-binding antibody-positive myasthenia gravis . Neurotherapeutics . 12 . 2 . 455–60 . Apr 2015 . 25742919 . 10.1007/s13311-015-0345-y . 4404445.
  53. Sorsa T, Pollesello P, Permi P, Drakenberg T, Kilpeläinen I . Interaction of levosimendan with cardiac troponin C in the presence of cardiac troponin I peptides . Journal of Molecular and Cellular Cardiology . 35 . 9 . 1055–61 . Sep 2003 . 12967628 . 10.1016/s0022-2828(03)00178-0.
  54. Robertson IM, Baryshnikova OK, Li MX, Sykes BD . Defining the binding site of levosimendan and its analogues in a regulatory cardiac troponin C-troponin I complex . Biochemistry . 47 . 28 . 7485–95 . Jul 2008 . 18570382 . 10.1021/bi800438k . 2652250.
  55. Kleerekoper Q, Putkey JA . Drug binding to cardiac troponin C . The Journal of Biological Chemistry . 274 . 34 . 23932–9 . Aug 1999 . 10446160 . 10.1074/jbc.274.34.23932. free .
  56. Szilágyi S, Pollesello P, Levijoki J, Kaheinen P, Haikala H, Edes I, Papp Z . The effects of levosimendan and OR-1896 on isolated hearts, myocyte-sized preparations and phosphodiesterase enzymes of the guinea pig . European Journal of Pharmacology . 486 . 1 . 67–74 . Feb 2004 . 14751410 . 10.1016/j.ejphar.2003.12.005.
  57. Ørstavik Ø, Manfra O, Andressen KW, Andersen GØ, Skomedal T, Osnes JB, Levy FO, Krobert KA . The inotropic effect of the active metabolite of levosimendan, OR-1896, is mediated through inhibition of PDE3 in rat ventricular myocardium . PLOS ONE . 10 . 3 . e0115547 . 2015 . 25738589 . 10.1371/journal.pone.0115547 . 4349697. 2015PLoSO..1015547O . free .
  58. Robertson IM, Sun YB, Li MX, Sykes BD . A structural and functional perspective into the mechanism of Ca2+-sensitizers that target the cardiac troponin complex . Journal of Molecular and Cellular Cardiology . 49 . 6 . 1031–41 . Dec 2010 . 20801130 . 10.1016/j.yjmcc.2010.08.019 . 2975748.
  59. Lindert S, Li MX, Sykes BD, McCammon JA . Computer-aided drug discovery approach finds calcium sensitizer of cardiac troponin . Chemical Biology & Drug Design . 85 . 2 . 99–106 . Feb 2015 . 24954187 . 10.1111/cbdd.12381 . 4456024.
  60. Wang X, Li MX, Sykes BD . Structure of the regulatory N-domain of human cardiac troponin C in complex with human cardiac troponin I147-163 and bepridil . The Journal of Biological Chemistry . 277 . 34 . 31124–33 . Aug 2002 . 12060657 . 10.1074/jbc.M203896200 . free.
  61. Oleszczuk M, Robertson IM, Li MX, Sykes BD . Solution structure of the regulatory domain of human cardiac troponin C in complex with the switch region of cardiac troponin I and W7: the basis of W7 as an inhibitor of cardiac muscle contraction . Journal of Molecular and Cellular Cardiology . 48 . 5 . 925–33 . May 2010 . 20116385 . 10.1016/j.yjmcc.2010.01.016 . 2854253.
  62. Wang X, Li MX, Spyracopoulos L, Beier N, Chandra M, Solaro RJ, Sykes BD . Structure of the C-domain of human cardiac troponin C in complex with the Ca2+ sensitizing drug EMD 57033 . The Journal of Biological Chemistry . 276 . 27 . 25456–66 . Jul 2001 . 11320096 . 10.1074/jbc.M102418200 . free .
  63. Pineda-Sanabria SE, Robertson IM, Sykes BD . Structure of trans-resveratrol in complex with the cardiac regulatory protein troponin C . Biochemistry . 50 . 8 . 1309–20 . Mar 2011 . 21226534 . 10.1021/bi101985j . 3043152.
  64. Li Y, Love ML, Putkey JA, Cohen C . Bepridil opens the regulatory N-terminal lobe of cardiac troponin C . Proceedings of the National Academy of Sciences of the United States of America . 97 . 10 . 5140–5 . May 2000 . 10792039 . 10.1073/pnas.090098997 . 25795. 2000PNAS...97.5140L . free .
  65. Robertson IM, Li MX, Sykes BD . Solution structure of human cardiac troponin C in complex with the green tea polyphenol, (-)-epigallocatechin 3-gallate . The Journal of Biological Chemistry . 284 . 34 . 23012–23 . Aug 2009 . 19542563 . 10.1074/jbc.M109.021352 . 2755708. free .
  66. Zong NC, Li H, Li H, Lam MP, Jimenez RC, Kim CS, Deng N, Kim AK, Choi JH, Zelaya I, Liem D, Meyer D, Odeberg J, Fang C, Lu HJ, Xu T, Weiss J, Duan H, Uhlen M, Yates JR, Apweiler R, Ge J, Hermjakob H, Ping P . Integration of cardiac proteome biology and medicine by a specialized knowledgebase . Circulation Research . 113 . 9 . 1043–53 . Oct 2013 . 23965338 . 4076475 . 10.1161/CIRCRESAHA.113.301151 .