A role for Mitochondrial Rho GTPase 1 (MIRO1) in motility and membrane dynamics of peroxisomes

Castro, Inês G.; Richards, David P.; Metz, Jeremy; Costello, Joseph L.; Passmore, Josiah B.; Schrader, Tina A.; Gouveia, Ana; Ribeiro, Daniela; Schrader, Michael

doi:10.1111/tra.12549

Cited by 70 publications

(136 citation statements)

References 62 publications

(121 reference statements)

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“…In contrast to these findings, we and Covill-Cooke and colleagues observed the targeting of Miro1 variant 1 to peroxisomes and mitochondria in COS-7 and mouse embryonic fibroblasts (MEFs) [11,14]. This variant, which lacks insert 1, was also shown to interact with Pex19 in a TMD and tail dependent manner.…”

Section: Targeting and Pex19 Bindingcontrasting

confidence: 81%

“…In agreement with this, similar peroxisome accumulations have been previously observed using an inducible cargo assay where kinesin motors are artificially tagged to peroxisomes in a regulated and inducible manner [25]. Furthermore, overexpression of wild type Miro1 or a constitutively active mutant for the 1 st GTPase domain of Miro1, induced a significant increase in peroxisome fast-directed movement [11,13], while silencing of Miro1 significantly decreased peroxisome motility [13]. These results suggest that, analogous to Miro1’s role at mitochondria, peroxisomal Miro1 regulates microtubule-dependent motility of this organelle (Figure 1).…”

Section: Miro1 and Peroxisome Motilitysupporting

confidence: 81%

“…Overexpression of Miro1 (wild-type and constructs mutated in the first GTPase domain) in COS-7 and HeLa cells induced a redistribution of peroxisomes to the cell periphery, an effect that was inhibited by treating the cells with nocodazole, a microtubule depolymerizing drug [11,13]. These results suggest a potential role for Miro1 in peroxisome motility, similar to its role in mitochondrial motility (Figure 1).…”

Section: Miro1 and Peroxisome Motilitymentioning

confidence: 92%

“…As shown in all three studies, Miro1 is no exception to this rule [11,13,14]. However, the conclusions on how this interaction is mediated and which isoforms of Miro1 are targeted to peroxisomes differ between studies.…”

Section: Targeting and Pex19 Bindingmentioning

confidence: 97%

“…Strikingly, little is known about the recruiting factors for these motors and how peroxisome motility is regulated. Recently, we and others have shown that Miro1, an atypical Ras GTPase, is targeted to peroxisomes in mammalian cells, where it regulates peroxisome motility (Figure 1) [11–14]. …”

mentioning

confidence: 99%

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Miro1 – the missing link to peroxisome motility

Castro

Schrader

2018

Communicative & Integrative Biology

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Peroxisomes are ubiquitous, highly dynamic, multifunctional compartments in eukaryotic cells, which perform key roles in cellular lipid metabolism and redox balance. Like other membrane-bound organelles, peroxisomes must move in the cellular landscape to perform localized functions, interact with other organelles and to properly distribute during cell division. However, our current knowledge of peroxisome motility in mammalian cells is still very limited. Recently, three independent studies have identified Miro1 as a regulator of peroxisome motility in mammalian cells. In these studies, the authors show that Miro1 is targeted to peroxisomes in several cell lines, in a process that relies on its interaction with the peroxisomal chaperone Pex19. Interestingly, however, different conclusions are drawn about which Miro1 isoforms are targeted to peroxisomes, how it interacts with Pex19 and most importantly, the type of motility Miro1 is regulating.

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Section: Targeting and Pex19 Bindingcontrasting

confidence: 81%

Section: Miro1 and Peroxisome Motilitysupporting

confidence: 81%

Section: Miro1 and Peroxisome Motilitymentioning

confidence: 92%

Section: Targeting and Pex19 Bindingmentioning

confidence: 97%

mentioning

confidence: 99%

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Miro1 – the missing link to peroxisome motility

Castro

Schrader

2018

Communicative & Integrative Biology

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Controlling contacts—Molecular mechanisms to regulate organelle membrane tethering

et al. 2022

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In recent years, membrane contact sites (MCS), which mediate interactions between virtually all subcellular organelles, have been extensively characterized and shown to be essential for intracellular communication. In this review essay, we focus on an emerging topic: the regulation of MCS. Focusing on the tether proteins themselves, we discuss some of the known mechanisms which can control organelle tethering events and identify apparent common regulatory hubs, such as the VAP interface at the endoplasmic reticulum (ER). We also highlight several currently hypothetical concepts, including the idea of tether oligomerization and redox regulation playing a role in MCS formation. We identify gaps in our current understanding, such as the identity of the majority of kinases/phosphatases involved in tether modification and conclude that a holistic approach-incorporating the formation of multiple MCS, regulated by interconnected regulatory modulators-may be required to fully appreciate the true complexity of these fascinating intracellular communication systems.

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Organelle interplay—peroxisome interactions in health and disease

Schrader

Kamoshita

Islinger

2019

J of Inher Metab Disea

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Peroxisomes are multifunctional, dynamic, membrane‐bound organelles with important functions in cellular lipid metabolism, rendering them essential for human health and development. Important roles for peroxisomes in signaling and the fine‐tuning of cellular processes are emerging, which integrate them in a complex network of interacting cellular compartments. Like many other organelles, peroxisomes communicate through membrane contact sites. For example, peroxisomal growth, positioning, and lipid metabolism involves contacts with the endoplasmic reticulum (ER). Here, we discuss the most recent findings on peroxisome‐organelle interactions including peroxisome‐ER interplay at membrane contacts sites, and functional interplay with mitochondria, lysosomes, and lipid droplets in mammalian cells. We address tether proteins, metabolic cooperation, and the impact of peroxisome interactions on human health and disease.

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A role for Mitochondrial Rho GTPase 1 (MIRO1) in motility and membrane dynamics of peroxisomes

Cited by 70 publications

References 62 publications

Miro1 – the missing link to peroxisome motility

Miro1 – the missing link to peroxisome motility

Controlling contacts—Molecular mechanisms to regulate organelle membrane tethering

Organelle interplay—peroxisome interactions in health and disease

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