Nanosurfer assay dissects β-cardiac myosin and cardiac myosin-binding protein C interactions

Cardiac myosin-binding protein C (cMyBP-C) modulates cardiac contractility through putative interactions with the myosin S2 tail and/or the thin filament. The relative contribution of these binding-partner interactions to cMyBP-C modulatory function remains unclear. Hence, we developed a “nanosurfer...

Descripción completa

Detalles Bibliográficos
Autores principales: Touma, Anja M., Tang, Wanjian, Rasicci, David V., Vang, Duha, Rai, Ashim, Previs, Samantha B., Warshaw, David M., Yengo, Christopher M., Sivaramakrishnan, Sivaraj
Formato: Online Artículo Texto
Lenguaje:English
Publicado: The Biophysical Society 2022
Materias:
Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9279167/
https://www.ncbi.nlm.nih.gov/pubmed/35591788
http://dx.doi.org/10.1016/j.bpj.2022.05.013
_version_ 1784746336669663232
author Touma, Anja M.
Tang, Wanjian
Rasicci, David V.
Vang, Duha
Rai, Ashim
Previs, Samantha B.
Warshaw, David M.
Yengo, Christopher M.
Sivaramakrishnan, Sivaraj
author_facet Touma, Anja M.
Tang, Wanjian
Rasicci, David V.
Vang, Duha
Rai, Ashim
Previs, Samantha B.
Warshaw, David M.
Yengo, Christopher M.
Sivaramakrishnan, Sivaraj
author_sort Touma, Anja M.
collection PubMed
description Cardiac myosin-binding protein C (cMyBP-C) modulates cardiac contractility through putative interactions with the myosin S2 tail and/or the thin filament. The relative contribution of these binding-partner interactions to cMyBP-C modulatory function remains unclear. Hence, we developed a “nanosurfer” assay as a model system to interrogate these cMyBP-C binding-partner interactions. Synthetic thick filaments were generated using recombinant human β-cardiac myosin subfragments (HMM or S1) attached to DNA nanotubes, with 14- or 28-nm spacing, corresponding to the 14.3-nm myosin spacing in native thick filaments. The nanosurfer assay consists of DNA nanotubes added to the in vitro motility assay so that myosins on the motility surface effectively deliver thin filaments to the DNA nanotubes, enhancing thin filament gliding probability on the DNA nanotubes. Thin filament velocities on nanotubes with either 14- or 28-nm myosin spacing were no different. We then characterized the effects of cMyBP-C on thin filament motility by alternating HMM and cMyBP-C N-terminal fragments (C0–C2 or C1–C2) on nanotubes every 14 nm. Both C0–C2 and C1–C2 reduced thin filament velocity four- to sixfold relative to HMM alone. Similar inhibition occurred using the myosin S1 construct, which lacks the myosin S2 region proposed to interact with cMyBP-C, suggesting that the cMyBP-C N terminus must interact with other myosin head domains and/or actin to slow thin filament velocity. Thin filament velocity was unaffected by the C0–C1f fragment, which lacks the majority of the M-domain, supporting the importance of this domain for inhibitory interaction(s). A C0–C2 fragment with phospho-mimetic replacement in the M-domain showed markedly less inhibition of thin filament velocity compared with its phospho-null counterpart, highlighting the modulatory role of M-domain phosphorylation on cMyBP-C function. Therefore, the nanosurfer assay provides a platform to precisely manipulate spatially dependent cMyBP-C binding-partner interactions, shedding light on the molecular regulation of β-cardiac myosin contractility.
format Online
Article
Text
id pubmed-9279167
institution National Center for Biotechnology Information
language English
publishDate 2022
publisher The Biophysical Society
record_format MEDLINE/PubMed
spelling pubmed-92791672023-06-21 Nanosurfer assay dissects β-cardiac myosin and cardiac myosin-binding protein C interactions Touma, Anja M. Tang, Wanjian Rasicci, David V. Vang, Duha Rai, Ashim Previs, Samantha B. Warshaw, David M. Yengo, Christopher M. Sivaramakrishnan, Sivaraj Biophys J Articles Cardiac myosin-binding protein C (cMyBP-C) modulates cardiac contractility through putative interactions with the myosin S2 tail and/or the thin filament. The relative contribution of these binding-partner interactions to cMyBP-C modulatory function remains unclear. Hence, we developed a “nanosurfer” assay as a model system to interrogate these cMyBP-C binding-partner interactions. Synthetic thick filaments were generated using recombinant human β-cardiac myosin subfragments (HMM or S1) attached to DNA nanotubes, with 14- or 28-nm spacing, corresponding to the 14.3-nm myosin spacing in native thick filaments. The nanosurfer assay consists of DNA nanotubes added to the in vitro motility assay so that myosins on the motility surface effectively deliver thin filaments to the DNA nanotubes, enhancing thin filament gliding probability on the DNA nanotubes. Thin filament velocities on nanotubes with either 14- or 28-nm myosin spacing were no different. We then characterized the effects of cMyBP-C on thin filament motility by alternating HMM and cMyBP-C N-terminal fragments (C0–C2 or C1–C2) on nanotubes every 14 nm. Both C0–C2 and C1–C2 reduced thin filament velocity four- to sixfold relative to HMM alone. Similar inhibition occurred using the myosin S1 construct, which lacks the myosin S2 region proposed to interact with cMyBP-C, suggesting that the cMyBP-C N terminus must interact with other myosin head domains and/or actin to slow thin filament velocity. Thin filament velocity was unaffected by the C0–C1f fragment, which lacks the majority of the M-domain, supporting the importance of this domain for inhibitory interaction(s). A C0–C2 fragment with phospho-mimetic replacement in the M-domain showed markedly less inhibition of thin filament velocity compared with its phospho-null counterpart, highlighting the modulatory role of M-domain phosphorylation on cMyBP-C function. Therefore, the nanosurfer assay provides a platform to precisely manipulate spatially dependent cMyBP-C binding-partner interactions, shedding light on the molecular regulation of β-cardiac myosin contractility. The Biophysical Society 2022-06-21 2022-05-18 /pmc/articles/PMC9279167/ /pubmed/35591788 http://dx.doi.org/10.1016/j.bpj.2022.05.013 Text en © 2022 Biophysical Society. https://creativecommons.org/licenses/by-nc-nd/4.0/This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Articles
Touma, Anja M.
Tang, Wanjian
Rasicci, David V.
Vang, Duha
Rai, Ashim
Previs, Samantha B.
Warshaw, David M.
Yengo, Christopher M.
Sivaramakrishnan, Sivaraj
Nanosurfer assay dissects β-cardiac myosin and cardiac myosin-binding protein C interactions
title Nanosurfer assay dissects β-cardiac myosin and cardiac myosin-binding protein C interactions
title_full Nanosurfer assay dissects β-cardiac myosin and cardiac myosin-binding protein C interactions
title_fullStr Nanosurfer assay dissects β-cardiac myosin and cardiac myosin-binding protein C interactions
title_full_unstemmed Nanosurfer assay dissects β-cardiac myosin and cardiac myosin-binding protein C interactions
title_short Nanosurfer assay dissects β-cardiac myosin and cardiac myosin-binding protein C interactions
title_sort nanosurfer assay dissects β-cardiac myosin and cardiac myosin-binding protein c interactions
topic Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9279167/
https://www.ncbi.nlm.nih.gov/pubmed/35591788
http://dx.doi.org/10.1016/j.bpj.2022.05.013
work_keys_str_mv AT toumaanjam nanosurferassaydissectsbcardiacmyosinandcardiacmyosinbindingproteincinteractions
AT tangwanjian nanosurferassaydissectsbcardiacmyosinandcardiacmyosinbindingproteincinteractions
AT rasiccidavidv nanosurferassaydissectsbcardiacmyosinandcardiacmyosinbindingproteincinteractions
AT vangduha nanosurferassaydissectsbcardiacmyosinandcardiacmyosinbindingproteincinteractions
AT raiashim nanosurferassaydissectsbcardiacmyosinandcardiacmyosinbindingproteincinteractions
AT previssamanthab nanosurferassaydissectsbcardiacmyosinandcardiacmyosinbindingproteincinteractions
AT warshawdavidm nanosurferassaydissectsbcardiacmyosinandcardiacmyosinbindingproteincinteractions
AT yengochristopherm nanosurferassaydissectsbcardiacmyosinandcardiacmyosinbindingproteincinteractions
AT sivaramakrishnansivaraj nanosurferassaydissectsbcardiacmyosinandcardiacmyosinbindingproteincinteractions

Ejemplares similares