CARP interacts with titin at a unique helical N2A sequence and at the domain Ig81 to form a structured complex

Zhou, Tiankun; Fleming, Jennifer R.; Franke, Barbara; Bogomolovas, Julius; Barsukov, Igor; Rigden, Daniel J.; Labeit, Siegfried; Mayans, Olga

doi:10.1002/1873-3468.12362

Cited by 26 publications

(77 citation statements)

References 61 publications

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“…The N2A region of titin plays a role in a number of important binding interactions but little is known about the properties of the individual domains. This is important to understand since different regions in N2A have unique interactions that could be regulated, in part, by domain stability.…”

Section: Resultsmentioning

confidence: 99%

“…The N2A region is believed to play a variety of crucial roles in both cardiac and skeletal muscle and is required for normal muscle function . The signaling and regulatory functions of the N2A region require functional binding sites for both the muscle ankyrin repeat proteins (MARPs) and the p94 protease.…”

Section: Discussionmentioning

confidence: 99%

“…The MARP proteins are transcription factors that regulate stress and damage response in both cardiac and skeletal muscle . CARP, the cardiac muscle member of the family, interacts with titin through a binding site that spans part of the insertion sequence and the I81 domain in response to various types of stress signals . The functional significance of the CARP/titin interaction is still not clear but proposed functions include modulation of titin elasticity, protection from phosphorylation and sequestration of CARP to downregulate its transcriptional activity .…”

Section: Discussionmentioning

confidence: 99%

“…In cardiac muscle, there are two isoforms and the longer of the two titin isoforms (N2BA) includes the N2A region . One important interaction in this region is titin's stretch‐sensing response through binding of CARP (cardiac ankyrin repeat protein) to the insertion sequence and I81 domains in titin's N2A region . CARP binds to the N2A region after being upregulated in response to mechanical and chemical cardiovascular stress …”

Section: Introductionmentioning

confidence: 99%

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Differences in stability and calcium sensitivity of the Ig domains in titin's N2A region

et al. 2020

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Titin is a large filamentous protein that spans half a sarcomere, from Z-disk to M-line. The N2A region within the titin molecule exists between the proximal immunoglobulin (Ig) region and the PEVK region and protein-protein interactions involving this region are required for normal muscle function. The N2A region consists of four Ig domains (I80-I83) with a 105 amino acid linker region between I80 and I81 that has a helical nature. Using chemical stability measurements, we show that predicted differences between the adjacent Ig domains (I81-I83) correlate with experimentally determined differences in chemical stability and refolding kinetics. Our work further shows that I83 has the lowest ΔG unfolding , which is increased in the presence of calcium (pCa 4.3), indicating that Ca 2+ plays a role in stabilizing this immunoglobulin domain. The characteristics of N2A's three Ig domains provide insight into the stability of the binding sites for proteins that interact with the N2A region. This work also provides insights into how Ca 2+ might influence binding events involving N2A. K E Y W O R D Schemical stability, immunoglobulin domain, N2A, titin

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Section: Resultsmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Differences in stability and calcium sensitivity of the Ig domains in titin's N2A region

et al. 2020

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“…As following UDD MARP1 shows no evidence of nuclear localization (Figure 6A–F), therefore interaction with GATA4 is unlikely. However, by binding to titin's N2A region (Figure 6G–P), MARP1 might increase titin‐based stiffness, cross‐link titin filaments12, 49 to sterically hinder signalling, or even form a scaffold for other binding proteins to facilitate N2A‐based hypertrophy signalling. Binding of MARP1 to titin's N2A segment might be facilitated by the differential upregulation of CAPN3, which in its active state (autolytic fragments) is capable of cleaving MARP1, thereby increasing its binding affinity to titin N2A 9.…”

Section: Discussionmentioning

confidence: 99%

Titin‐based mechanosensing modulates muscle hypertrophy

Pijl

Strom

Conijn

et al. 2018

J cachexia sarcopenia muscle

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BackgroundTitin is an elastic sarcomeric filament that has been proposed to play a key role in mechanosensing and trophicity of muscle. However, evidence for this proposal is scarce due to the lack of appropriate experimental models to directly test the role of titin in mechanosensing.MethodsWe used unilateral diaphragm denervation (UDD) in mice, an in vivo model in which the denervated hemidiaphragm is passively stretched by the contralateral, innervated hemidiaphragm and hypertrophy rapidly occurs.ResultsIn wildtype mice, the denervated hemidiaphragm mass increased 48 ± 3% after 6 days of UDD, due to the addition of both sarcomeres in series and in parallel. To test whether titin stiffness modulates the hypertrophy response, RBM20ΔRRM and TtnΔIAjxn mouse models were used, with decreased and increased titin stiffness, respectively. RBM20ΔRRM mice (reduced stiffness) showed a 20 ± 6% attenuated hypertrophy response, whereas the TtnΔIAjxn mice (increased stiffness) showed an 18 ± 8% exaggerated response after UDD. Thus, muscle hypertrophy scales with titin stiffness. Protein expression analysis revealed that titin‐binding proteins implicated previously in muscle trophicity were induced during UDD, MARP1 & 2, FHL1, and MuRF1.ConclusionsTitin functions as a mechanosensor that regulates muscle trophicity.

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Titin UN2A Acts as a Stable, Non‐Polymorphic Scaffold in its Binding to CARP

Stehle,

Fleming,

Bauer

et al. 2023

ChemBioChem

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The N2A segment of titin functions as a pivotal hub for signal transduction and interacts with various proteins involved in structural support, chaperone activities, and transcriptional regulation. Notably, the “unique N2A” (UN2A) subdomain has been shown to interact with the stress‐regulated cardiac ankyrin repeat protein (CARP), which contributes to the regulation of sarcomeric stiffness. Previously, the UN2A domain's three‐dimensional structure was modelled based on its secondary structure content identified by NMR spectroscopy, considering the domain in isolation. In this study, we report experimental long‐range distance distributions by electron paramagnetic resonance (EPR) spectroscopy between the three helixes within the UN2A domain linked to the immunoglobulin domain I81 in the presence and absence of CARP. The data confirm the central three‐helix bundle fold of UN2A and show that this adopts a compact and stable conformation in absence of CARP. After binding to CARP, no significant conformational change was observed, suggesting that the UN2A domain retains its structure upon binding to CARP thereby, mediating the interaction approximately as a rigid‐body.

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CARP interacts with titin at a unique helical N2A sequence and at the domain Ig81 to form a structured complex

Cited by 26 publications

References 61 publications

Differences in stability and calcium sensitivity of the Ig domains in titin's N2A region

Differences in stability and calcium sensitivity of the Ig domains in titin's N2A region

Titin‐based mechanosensing modulates muscle hypertrophy

Titin UN2A Acts as a Stable, Non‐Polymorphic Scaffold in its Binding to CARP

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