Mechanisms of Drp1 Recruitment to Mitochondria

Mechanisms of Drp1 Recruitment to Mitochondria

<p>Dynamin-related protein 1 (Drp1) is a GTPase of the dynamin superfamily that catalyzes mitochondrial fission in the cell. Cytosolic Drp1 is recruited to mitochondria by receptors anchored to the outer mitochondrial membrane. Once there, Drp1 assembles into a complex around the mitochondrial...

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Main Author: Liu, Raymond
Format: Others
Published: 2017
Online Access:https://thesis.library.caltech.edu/10239/1/RL%20Thesis%2020170602.pdf
Liu, Raymond (2017) Mechanisms of Drp1 Recruitment to Mitochondria. Dissertation (Ph.D.), California Institute of Technology. doi:10.7907/Z99Z92ZF. https://resolver.caltech.edu/CaltechTHESIS:05312017-190514797 <https://resolver.caltech.edu/CaltechTHESIS:05312017-190514797>
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spelling ndltd-CALTECH-oai-thesis.library.caltech.edu-102392019-10-05T03:04:37Z Mechanisms of Drp1 Recruitment to Mitochondria Liu, Raymond <p>Dynamin-related protein 1 (Drp1) is a GTPase of the dynamin superfamily that catalyzes mitochondrial fission in the cell. Cytosolic Drp1 is recruited to mitochondria by receptors anchored to the outer mitochondrial membrane. Once there, Drp1 assembles into a complex around the mitochondrial circumference to drive division via a GTP-dependent constriction process. The four known receptors of Drp1 are Fis1, Mff, MiD51, and MiD49, but stable interactions between Drp1 and these proteins have not been established. In addition, though mounting evidence suggests these receptors have non-redundant roles in their interaction with Drp1, mechanistic details explaining these distinctions are lacking. Here we address these questions, and show that the Insert B domain of Drp1 inhibits its interaction with Mff. Removal of this domain stabilizes a complex of Drp1 and Mff in vitro. In addition, we show that Drp1 oligomerization is a requirement for Mff recruitment, but not for MiD51 or MiD49-mediated recruitment. Together the results suggest a model in which Drp1 recruitment to mitochondria is regulated by the oligomeric state of Drp1, such that Mff, MiD51, and MiD49 recruit different subpopulations of Drp1 from the cytosol.</p> <p>With this model as a framework, we analyze the effect that a Drp1 R403C mutant, identified in several human patients presenting with encephalopathy and refractory epilepsy, has on mitochondrial morphology in cultured cells. We find that the loss of Drp1 oligomerization in these mutants impedes its ability to be recruited by Mff, leading to abnormal elongation of the mitochondrial population.</p> 2017 Thesis NonPeerReviewed application/pdf https://thesis.library.caltech.edu/10239/1/RL%20Thesis%2020170602.pdf https://resolver.caltech.edu/CaltechTHESIS:05312017-190514797 Liu, Raymond (2017) Mechanisms of Drp1 Recruitment to Mitochondria. Dissertation (Ph.D.), California Institute of Technology. doi:10.7907/Z99Z92ZF. https://resolver.caltech.edu/CaltechTHESIS:05312017-190514797 <https://resolver.caltech.edu/CaltechTHESIS:05312017-190514797> https://thesis.library.caltech.edu/10239/
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format Others
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description <p>Dynamin-related protein 1 (Drp1) is a GTPase of the dynamin superfamily that catalyzes mitochondrial fission in the cell. Cytosolic Drp1 is recruited to mitochondria by receptors anchored to the outer mitochondrial membrane. Once there, Drp1 assembles into a complex around the mitochondrial circumference to drive division via a GTP-dependent constriction process. The four known receptors of Drp1 are Fis1, Mff, MiD51, and MiD49, but stable interactions between Drp1 and these proteins have not been established. In addition, though mounting evidence suggests these receptors have non-redundant roles in their interaction with Drp1, mechanistic details explaining these distinctions are lacking. Here we address these questions, and show that the Insert B domain of Drp1 inhibits its interaction with Mff. Removal of this domain stabilizes a complex of Drp1 and Mff in vitro. In addition, we show that Drp1 oligomerization is a requirement for Mff recruitment, but not for MiD51 or MiD49-mediated recruitment. Together the results suggest a model in which Drp1 recruitment to mitochondria is regulated by the oligomeric state of Drp1, such that Mff, MiD51, and MiD49 recruit different subpopulations of Drp1 from the cytosol.</p> <p>With this model as a framework, we analyze the effect that a Drp1 R403C mutant, identified in several human patients presenting with encephalopathy and refractory epilepsy, has on mitochondrial morphology in cultured cells. We find that the loss of Drp1 oligomerization in these mutants impedes its ability to be recruited by Mff, leading to abnormal elongation of the mitochondrial population.</p>
author Liu, Raymond
spellingShingle Liu, Raymond
Mechanisms of Drp1 Recruitment to Mitochondria
author_facet Liu, Raymond
author_sort Liu, Raymond
title Mechanisms of Drp1 Recruitment to Mitochondria
title_short Mechanisms of Drp1 Recruitment to Mitochondria
title_full Mechanisms of Drp1 Recruitment to Mitochondria
title_fullStr Mechanisms of Drp1 Recruitment to Mitochondria
title_full_unstemmed Mechanisms of Drp1 Recruitment to Mitochondria
title_sort mechanisms of drp1 recruitment to mitochondria
publishDate 2017
url https://thesis.library.caltech.edu/10239/1/RL%20Thesis%2020170602.pdf
Liu, Raymond (2017) Mechanisms of Drp1 Recruitment to Mitochondria. Dissertation (Ph.D.), California Institute of Technology. doi:10.7907/Z99Z92ZF. https://resolver.caltech.edu/CaltechTHESIS:05312017-190514797 <https://resolver.caltech.edu/CaltechTHESIS:05312017-190514797>
work_keys_str_mv AT liuraymond mechanismsofdrp1recruitmenttomitochondria
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