The MyMOMA domain of MYO19 encodes for distinct Miro-dependent and Miro-independent mechanisms of interaction with mitochondrial membranes

Bocanegra, Jennifer L.; Fujita, Barbara M.; Melton, Natalie R.; Cowan, James M.; Schinski, Elizabeth L.; Tamir, Tigist Y.; Major, Michael B.; Quintero, Omar A.

doi:10.1101/602938

Cited by 5 publications

(23 citation statements)

References 112 publications

(152 reference statements)

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“…While stable subplasmalemmal actin rings form periodic structures that wrap around axons to support the axonal membrane, dynamic intra‐axonal filaments help to enrich actin at presynaptic terminals (Ganguly et al., 2015; Xu, Zhong, & Zhuang, 2013). It has been reported that mitochondrial receptors Miro1/2 regulate recruitment and stability of myosin‐19, thus likely coordinating MT‐ and actin‐based mitochondrial trafficking in mouse embryonic fibroblasts (MEFs) (Bocanegra et al., 2020; López‐Doménech et al., 2018; Oeding et al., 2018; Quintero et al., 2009). However, the role of myosin‐19 in axonal mitochondrial trafficking is not clear.…”

Section: Developmental Regulation Of Axonal Mitochondrial Motilitymentioning

confidence: 99%

Developmental regulation of microtubule‐based trafficking and anchoring of axonal mitochondria in health and diseases

Cheng

Sheng

2020

Developmental Neurobiology

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Mitochondria are cellular power plants that supply most of the ATP required in the brain to power neuronal growth, function, and regeneration. Given their extremely polarized structures and extended long axons, neurons face an exceptional challenge to maintain energy homeostasis in distal axons, synapses, and growth cones.Anchored mitochondria serve as local energy sources; therefore, the regulation of mitochondrial trafficking and anchoring ensures that these metabolically active areas are adequately supplied with ATP. Chronic mitochondrial dysfunction is a hallmark feature of major aging-related neurodegenerative diseases, and thus, anchored mitochondria in aging neurons need to be removed when they become dysfunctional.Investigations into the regulation of microtubule (MT)-based trafficking and anchoring of axonal mitochondria under physiological and pathological circumstances represent an important emerging area. In this short review article, we provide an updated overview of recent in vitro and in vivo studies showing (1) how mitochondria are transported and positioned in axons and synapses during neuronal developmental and maturation stages, and (2) how altered mitochondrial motility and axonal energy deficits in aging nervous systems link to neurodegeneration and regeneration in a disease or injury setting. We also highlight a major role of syntaphilin as a key MTbased regulator of axonal mitochondrial trafficking and anchoring in mature neurons.

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Section: Developmental Regulation Of Axonal Mitochondrial Motilitymentioning

confidence: 99%

Developmental regulation of microtubule‐based trafficking and anchoring of axonal mitochondria in health and diseases

Cheng

Sheng

2020

Developmental Neurobiology

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“…Differential binding localization studies suggest that Miro1 and Miro2 interact differently with the motor adapters TRAK1 and TRAK2 (van Spronsen et al, 2013). The nGTPase domains of HsMiro1 and HsMiro2, which are believed to play the key role in the interactions with TRAK1/2 (Bocanegra et al, 2019;Oeding et al, 2018), are structurally quite similar, as they exhibit 73% sequence identity and 88% sequence similarity. Consequently, the set of 21 nonhomologous amino acid substitutions between them presumably differentiate the functions of the two proteins.…”

Section: Discussionmentioning

confidence: 99%

Structural assembly of the human Miro1/2 GTPases based on the crystal structure of the N-terminal GTPase domain

Smith

Focia

Chakravarthy

et al. 2019

Preprint

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PDB reference: Crystal structure of the human Miro1 N-terminal GTPase bound to GTP, 6D71 Abstract Dysfunction in mitochondrial dynamics is believed to contribute to a host of neurological disorders and has recently been implicated in cancer metastasis. The outer mitochondrial membrane adapter protein Miro functions in the regulation of mitochondrial mobility and degradation, however, the structural basis for its roles in mitochondrial regulation remain unknown. Here, we report a 1.7Å crystal structure of Nterminal GTPase domain (nGTPase) of human Miro1 bound unexpectedly to GTP, thereby revealing a non-catalytic configuration of the putative GTPase active site. We identify two conserved surfaces of the nGTPase, the "SELFYY" and "ITIP" motifs, that are potentially positioned to mediate dimerization or interaction with binding partners. Additionally, we report small angle X-ray scattering (SAXS) data obtained from the intact soluble HsMiro1 and its paralog HsMiro2. Taken together, the data allow modeling of a crescent-shaped assembly of the full-length soluble domain of HsMiro1/2.

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“…Human mchr-MIRO2 was previously reported (Bocanegra et al 2019). Mouse GFP-TRAK constructs used in these studies were generated using previously reported GFP-TRAK plasmids (Lopez-Domenech et al 2018) as a template.…”

Section: Construct Generationmentioning

confidence: 99%

Characterization of the MIRO-independent mitochondrial association activity of TRAK proteins

Mitchell

Fatima

et al. 2021

Preprint

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Mitochondria are essential to proper cell function, mislocalization of mitochondria leads to disease. Previous research has indicated that MYO19, an unconventional myosin, localizes to the mitochondria outer membrane (MOM) and enables actin-based mitochondrial movement along the cytoskeleton. MOM insertion of MYO19 is assisted by the small GTPase MIRO, a "molecular switch" that facilitates MYO19/mitochondria interactions. MIRO serves as a recruiter of MYO19 to the MOM, rather than the tether/receptor that mediates attachment, as MYO19 contains a second, MIRO-independent mitochondrial association domain. MIRO proteins have previously been reported to serve as attachment points for the microtubule-based motors through interactions with the adaptor protein, TRAK. Past research has identified a MIRO-binding domain of TRAK that directly participates in the interaction with MIRO. We chose to investigate whether the interactions between TRAK and MOM paralleled our hypothesized mechanism for MYO19/MOM interactions by examining the MIRO-mediated enhancement of TRAK protein localization to mitochondria, by identifying the location of a MIRO-independent mitochondrial association domain in the c-terminus of TRAK proteins, and by examining the steady-state binding kinetics of various TRAK constructs to mitochondria. We interpret these data to indicate that MIRO proteins serve in the initial recruitment of TRAK proteins to mitochondria, but that the MIRO-independent domain plays a significant role in long-term association between TRAK and MOM.

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The MyMOMA domain of MYO19 encodes for distinct Miro-dependent and Miro-independent mechanisms of interaction with mitochondrial membranes

Cited by 5 publications

References 112 publications

Developmental regulation of microtubule‐based trafficking and anchoring of axonal mitochondria in health and diseases

Developmental regulation of microtubule‐based trafficking and anchoring of axonal mitochondria in health and diseases

Structural assembly of the human Miro1/2 GTPases based on the crystal structure of the N-terminal GTPase domain

Characterization of the MIRO-independent mitochondrial association activity of TRAK proteins

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