The<scp>MYO</scp>6 interactome: selective motor‐cargo complexes for diverse cellular processes

Jonge, Janeska J. de; Batters, Christopher; O’Loughlin, Thomas; Arden, Susan D.; Buß, Folma

doi:10.1002/1873-3468.13486

Cited by 38 publications

(28 citation statements)

References 100 publications

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“…This confirms our previous results (using immunogold technique) showing that MYO6 localized to both Golgi sub-domains in wild-type mice males [ 12 ]. Targeting of MYO6 to different cellular compartments in mammalian cells involves a range of binding partners [ 15 ] and so we next analyzed which adaptor protein may function with MYO6 during acrosome biogenesis. We tested several MYO6 interacting proteins including TOM1/L2, GIPC1, optineurin, DOCK7, LRCH3, and LARG for their localization, and only observed the presence of TOM1/L2 in close vicinity to the Golgi complex.…”

Section: Resultsmentioning

confidence: 99%

Loss of myosin VI expression affects acrosome/acroplaxome complex morphology during mouse spermiogenesis†

Zakrzewski

Rędowicz

Buß

et al. 2020

Biology of Reproduction

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During spermiogenesis in mammals, actin filaments and a variety of actin-binding proteins are involved in the formation and function of highly specialized testis-specific structures. Actin-based motor proteins, such as myosin Va and VIIa, play a key role in this complex process of spermatid transformation into mature sperm. We have previously demonstrated that myosin VI (MYO6) is also expressed in mouse testes. It is present in actin-rich structures important for spermatid development, including one of the earliest events in spermiogenesis—acrosome formation. Here, we demonstrate using immunofluorescence, cytochemical, and ultrastructural approaches that MYO6 is involved in maintaining the structural integrity of these specialized actin-rich structures during acrosome biogenesis in mouse. We show that MYO6 together with its binding partner TOM1/L2 is present at/around the spermatid Golgi complex and the nascent acrosome. Depletion of MYO6 in Snell’s waltzer mice causes structural disruptions of the Golgi complex and affects the acrosomal granule positioning within the developing acrosome. In summary, our results suggest that MYO6 plays an anchoring role during the acrosome biogenesis mainly by tethering of different cargo/membranes to highly specialized actin-related structures.

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Section: Resultsmentioning

confidence: 99%

Loss of myosin VI expression affects acrosome/acroplaxome complex morphology during mouse spermiogenesis†

Zakrzewski

Rędowicz

Buß

et al. 2020

Biology of Reproduction

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“…This feature allows MYO6 to move molecules or vesicles from the plasma membrane toward the cell interior, thereby playing essential roles in regulating endocytosis [23,26,29]. This cytoskeletal motor also controls additional intracellular trafficking events, such as exocytosis and autophagy [26,29,133]. The complexity of MYO6 functions is further illustrated by its localization in the nucleus, where it participates in the regulation of gene expression [134,135].…”

Section: Class VI Myosinsmentioning

confidence: 99%

Myosin Motors: Novel Regulators and Therapeutic Targets in Colorectal Cancer

Naydenov

Lechuga

Huang

et al. 2021

Cancers

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Colorectal cancer (CRC) remains the third most common cause of cancer and the second most common cause of cancer deaths worldwide. Clinicians are largely faced with advanced and metastatic disease for which few interventions are available. One poorly understood aspect of CRC involves altered organization of the actin cytoskeleton, especially at the metastatic stage of the disease. Myosin motors are crucial regulators of actin cytoskeletal architecture and remodeling. They act as mechanosensors of the tumor environments and control key cellular processes linked to oncogenesis, including cell division, extracellular matrix adhesion and tissue invasion. Different myosins play either oncogenic or tumor suppressor roles in breast, lung and prostate cancer; however, little is known about their functions in CRC. This review focuses on the functional roles of myosins in colon cancer development. We discuss the most studied class of myosins, class II (conventional) myosins, as well as several classes (I, V, VI, X and XVIII) of unconventional myosins that have been linked to CRC development. Altered expression and mutations of these motors in clinical tumor samples and their roles in CRC growth and metastasis are described. We also evaluate the potential of using small molecular modulators of myosin activity to develop novel anticancer therapies.

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“…Recently, septins have been screened as binding partners of the complex LRCH3/ DOCK7/DOCK8/MYO6 on actin filaments [172][173][174]. DOCKs, corresponding to the Dedicator of CytoKinesis family, are GEF proteins of RhoA/Rac/Cdc42 that regulate F-actin organization (for review [175]) and MT dynamics [176].…”

Section: Jnk and Septinsmentioning

confidence: 99%

Cytoskeleton and Associated Proteins: Pleiotropic JNK Substrates and Regulators

Benoit

Baillet

Poüs

2021

IJMS

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This review extensively reports data from the literature concerning the complex relationships between the stress-induced c-Jun N-terminal kinases (JNKs) and the four main cytoskeleton elements, which are actin filaments, microtubules, intermediate filaments, and septins. To a lesser extent, we also focused on the two membrane-associated cytoskeletons spectrin and ESCRT-III. We gather the mechanisms controlling cytoskeleton-associated JNK activation and the known cytoskeleton-related substrates directly phosphorylated by JNK. We also point out specific locations of the JNK upstream regulators at cytoskeletal components. We finally compile available techniques and tools that could allow a better characterization of the interplay between the different types of cytoskeleton filaments upon JNK-mediated stress and during development. This overview may bring new important information for applied medical research.

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TheMYO6 interactome: selective motor‐cargo complexes for diverse cellular processes

Cited by 38 publications

References 100 publications

Loss of myosin VI expression affects acrosome/acroplaxome complex morphology during mouse spermiogenesis†

Loss of myosin VI expression affects acrosome/acroplaxome complex morphology during mouse spermiogenesis†

Myosin Motors: Novel Regulators and Therapeutic Targets in Colorectal Cancer

Cytoskeleton and Associated Proteins: Pleiotropic JNK Substrates and Regulators

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