A potent voltage-gated calcium channel inhibitor engineered from a nanobody targeted to auxiliary CaVβ subunits
Inhibiting high-voltage-activated calcium channels (HVACCs; CaV1/CaV2) is therapeutic for myriad cardiovascular and neurological diseases. For particular applications, genetically-encoded HVACC blockers may enable channel inhibition with greater tissue-specificity and versatility than is achievable...
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doaj-e56ce6dd3efa4e69a83ce9aa4dcbc7332021-05-05T17:50:07ZengeLife Sciences Publications LtdeLife2050-084X2019-08-01810.7554/eLife.49253A potent voltage-gated calcium channel inhibitor engineered from a nanobody targeted to auxiliary CaVβ subunitsTravis J Morgenstern0https://orcid.org/0000-0003-2634-8470Jinseo Park1Qing R Fan2https://orcid.org/0000-0002-9330-0963Henry M Colecraft3https://orcid.org/0000-0002-2340-8899Department of Pharmacology, Columbia University, Vagelos College of Physicians and Surgeons, New York, United StatesDepartment of Pharmacology, Columbia University, Vagelos College of Physicians and Surgeons, New York, United StatesDepartment of Pharmacology, Columbia University, Vagelos College of Physicians and Surgeons, New York, United StatesDepartment of Pharmacology, Columbia University, Vagelos College of Physicians and Surgeons, New York, United States; Department of Physiology and Cellular Biophysics, Columbia University, Vagelos College of Physicians and Surgeons, New York, United StatesInhibiting high-voltage-activated calcium channels (HVACCs; CaV1/CaV2) is therapeutic for myriad cardiovascular and neurological diseases. For particular applications, genetically-encoded HVACC blockers may enable channel inhibition with greater tissue-specificity and versatility than is achievable with small molecules. Here, we engineered a genetically-encoded HVACC inhibitor by first isolating an immunized llama nanobody (nb.F3) that binds auxiliary HVACC CaVβ subunits. Nb.F3 by itself is functionally inert, providing a convenient vehicle to target active moieties to CaVβ-associated channels. Nb.F3 fused to the catalytic HECT domain of Nedd4L (CaV-aβlator), an E3 ubiquitin ligase, ablated currents from diverse HVACCs reconstituted in HEK293 cells, and from endogenous CaV1/CaV2 channels in mammalian cardiomyocytes, dorsal root ganglion neurons, and pancreatic β cells. In cardiomyocytes, CaV-aβlator redistributed CaV1.2 channels from dyads to Rab-7-positive late endosomes. This work introduces CaV-aβlator as a potent genetically-encoded HVACC inhibitor, and describes a general approach that can be broadly adapted to generate versatile modulators for macro-molecular membrane protein complexes.https://elifesciences.org/articles/49253calcium channelnanobodyubiquitinNedd4calcium channel betacavia porcellus |
collection |
DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
Travis J Morgenstern Jinseo Park Qing R Fan Henry M Colecraft |
spellingShingle |
Travis J Morgenstern Jinseo Park Qing R Fan Henry M Colecraft A potent voltage-gated calcium channel inhibitor engineered from a nanobody targeted to auxiliary CaVβ subunits eLife calcium channel nanobody ubiquitin Nedd4 calcium channel beta cavia porcellus |
author_facet |
Travis J Morgenstern Jinseo Park Qing R Fan Henry M Colecraft |
author_sort |
Travis J Morgenstern |
title |
A potent voltage-gated calcium channel inhibitor engineered from a nanobody targeted to auxiliary CaVβ subunits |
title_short |
A potent voltage-gated calcium channel inhibitor engineered from a nanobody targeted to auxiliary CaVβ subunits |
title_full |
A potent voltage-gated calcium channel inhibitor engineered from a nanobody targeted to auxiliary CaVβ subunits |
title_fullStr |
A potent voltage-gated calcium channel inhibitor engineered from a nanobody targeted to auxiliary CaVβ subunits |
title_full_unstemmed |
A potent voltage-gated calcium channel inhibitor engineered from a nanobody targeted to auxiliary CaVβ subunits |
title_sort |
potent voltage-gated calcium channel inhibitor engineered from a nanobody targeted to auxiliary cavβ subunits |
publisher |
eLife Sciences Publications Ltd |
series |
eLife |
issn |
2050-084X |
publishDate |
2019-08-01 |
description |
Inhibiting high-voltage-activated calcium channels (HVACCs; CaV1/CaV2) is therapeutic for myriad cardiovascular and neurological diseases. For particular applications, genetically-encoded HVACC blockers may enable channel inhibition with greater tissue-specificity and versatility than is achievable with small molecules. Here, we engineered a genetically-encoded HVACC inhibitor by first isolating an immunized llama nanobody (nb.F3) that binds auxiliary HVACC CaVβ subunits. Nb.F3 by itself is functionally inert, providing a convenient vehicle to target active moieties to CaVβ-associated channels. Nb.F3 fused to the catalytic HECT domain of Nedd4L (CaV-aβlator), an E3 ubiquitin ligase, ablated currents from diverse HVACCs reconstituted in HEK293 cells, and from endogenous CaV1/CaV2 channels in mammalian cardiomyocytes, dorsal root ganglion neurons, and pancreatic β cells. In cardiomyocytes, CaV-aβlator redistributed CaV1.2 channels from dyads to Rab-7-positive late endosomes. This work introduces CaV-aβlator as a potent genetically-encoded HVACC inhibitor, and describes a general approach that can be broadly adapted to generate versatile modulators for macro-molecular membrane protein complexes. |
topic |
calcium channel nanobody ubiquitin Nedd4 calcium channel beta cavia porcellus |
url |
https://elifesciences.org/articles/49253 |
work_keys_str_mv |
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