Myosin II Tailpiece Determines Its Paracrystal Structure, Filament Assembly Properties, and Cellular Localization

Rönen, Daniel; Ravid, Shoshana

doi:10.1074/jbc.m109.023754

Cited by 49 publications

(78 citation statements)

References 46 publications

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“…7A). Thus in contrast to the complete tailpiece containing both the positively and negatively charged regions, the negatively charged The tailpiece has been shown to be important for determining the isoform specific morphology of NMII paracrystals (28). As the negatively charged region does not promote IICRod 1296 -1854 filament assembly it may be important in determining NMII paracrystal morphology.…”

Section: The Negatively Charged Region Of Nmii-c Tailpiece Regulates mentioning

confidence: 99%

“…NMII isoforms create different paracrystal morphology: NMII-A and NMII-B form large wide filaments (width measuring 1.21 Ϯ 0.4 nm and 1.22 Ϯ 0.38 nm, respectively) while NMII-C forms delicate thin filaments (0.32 Ϯ 0.07 nm) (28). Swapping the negatively charged region of either NMII-A or NMII-B with the negatively charged region of NMII-C resulted in thin filaments similar to NMII-C (0.269 nm Ϯ0.06 and 0.239 nm Ϯ0.04, respectively) ( Fig.…”

Section: The Negatively Charged Region Of Nmii-c Tailpiece Regulates mentioning

confidence: 99%

“…Furthermore, smooth muscle myosin II has a splice variant lacking the tailpiece, which exhibited significantly different properties of filament assembly that were reflected by different molecular packing inside the filament (26). Swapping the tailpieces among the different NMII isoforms showed that the tailpiece affects NMII function in vivo and determines the specific morphology of NMII filaments (28). Additionally, phosphorylating the tailpiece by protein kinase C and casein kinase II resulted in decreased NMII assembly as determined by sedimentation and critical concentration experiments (29 -34).…”

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confidence: 99%

“…This tailpiece has been shown to be an important regulatory domain, affecting NMII filament assembly and cellular functions (24 -28). Removing the tailpiece from chicken smooth muscle myosin II and NMII changed their solubility and impaired the ability of NMII to form large filamentous structures (24,28). Furthermore, smooth muscle myosin II has a splice variant lacking the tailpiece, which exhibited significantly different properties of filament assembly that were reflected by different molecular packing inside the filament (26).…”

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The Positively Charged Region of the Myosin IIC Non-helical Tailpiece Promotes Filament Assembly

Rönen¹,

Rosenberg

Shalev

et al. 2010

Journal of Biological Chemistry

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The motor protein, non-muscle myosin II (NMII), must undergo dynamic oligomerization into filaments to participate in cellular processes such as cell migration and cytokinesis. A small non-helical region at the tail of the long coiled-coil region (tailpiece) is a common feature of all dynamically assembling myosin II proteins. In this study, we investigated the role of the tailpiece in NMII-C self-assembly. We show that the tailpiece is natively unfolded, as seen by circular dichroism and NMR experiments, and is divided into two regions of opposite charge. The positively charged region (Tailpiece 1946(Tailpiece -1967 ) starts at residue 1946 and is extended by seven amino acids at its N terminus from the traditional coiled-coil ending proline (Tailpiece 1953(Tailpiece -1967 ). Pull-down and sedimentation assays showed that the positive Tailpiece 1946 -1967 binds to assembly incompetent NMII-C fragments inducing filament assembly. The negative region, residues 1968 -2000, is responsible for NMII paracrystal morphology as determined by chimeras in which the negative region was swapped between the NMII isoforms. Mixing the positive and negative peptides had no effect on the ability of the positive peptide to bind and induce filament assembly. This study provides molecular insight into the role of the structurally disordered tailpiece of NMII-C in shifting the oligomeric equilibrium of NMII-C toward filament assembly and determining its morphology.Myosin II is a hexameric protein (Fig. 1A) of a family of actinbased molecular motors that are involved in cellular activities such as muscle contraction, cell migration, and cytokinesis (1-4). Each hexamer comprises two identical heavy chains and two sets of light chains. The N-terminal region of myosin II heavy chain is a globular head containing the actin binding and ATPase domains, followed by a large coiled-coil rod, which enables independent myosin II hexamers to assemble into large filaments (1). Non-muscle myosin II (NMII) 4 is a ubiquitous protein expressed by all cell types that mediates cellular processes that require contractility (2-4). In contrast to skeletal myosin II, NMII undergoes dynamic filament assembly-disassembly cycles to facilitate its diverse range of activities (5). NMII can only function when in filament form. Therefore, the process of filament assembly is an important regulatory step controlling NMII action (1). Several crucial factors for NMII filament assembly have been identified, including charge periodicity in the amino acid sequence along the coiled-coil rod and the presence of two small assembly competence domains located at the C terminus of the coiled-coil (6 -11). Additionally myosin II light chain phosphorylation activates the motor domain and promotes filament assembly (12)(13)(14).Three isoforms of NMII (NMII-A, NMII-B, and NMII-C) have been identified in mammals (15-17), each with specific tissue distributions and functions (18 -23). The C terminus of NMII contains a non-helical tailpiece (tailpiece) of 33-47 amino acids depe...

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Section: The Negatively Charged Region Of Nmii-c Tailpiece Regulates mentioning

confidence: 99%

Section: The Negatively Charged Region Of Nmii-c Tailpiece Regulates mentioning

confidence: 99%

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confidence: 99%

mentioning

confidence: 99%

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The Positively Charged Region of the Myosin IIC Non-helical Tailpiece Promotes Filament Assembly

Rönen¹,

Rosenberg

Shalev

et al. 2010

Journal of Biological Chemistry

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“…Most of the reports on the role of the nonhelical tailpieces of vertebrate myosin IIs are based on in vitro studies of tail fragments of the mammalian nonmuscle myosin IIs NMIIA, NMIIB, and, to a lesser extent, NMIIC (22)(23)(24)(25)(26)(27). Phosphorylation by protein kinase C or casein kinase II of one or more serines in the nonhelical tailpieces of NMIIA and NMIIB was reported to inhibit assembly of NMIIB tail fragments but not of NMIIA tail fragments (23,24), as assayed by sedimentation, but in a later study was reported to inhibit the assembly of tail fragments of NMIIA (25).…”

Section: Discussionmentioning

confidence: 99%

Regulation of the filament structure and assembly ofAcanthamoebamyosin II by phosphorylation of serines in the heavy-chain nonhelical tailpiece

Liu

Hong

Shu

et al. 2012

Proc. Natl. Acad. Sci. U.S.A.

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Acanthamoeba myosin II (AMII) has two heavy chains ending in a 27-residue nonhelical tailpiece and two pairs of light chains. In a companion article, we show that five, and only five, serine residues can be phosphorylated both in vitro and in vivo: Ser639 in surface loop 2 of the motor domain and serines 1489, 1494, 1499, and 1504 in the nonhelical tailpiece of the heavy chains. In that paper, we show that phosphorylation of Ser639 down-regulates the actin-activated MgATPase activity of AMII and that phosphorylation of the serines in the nonhelical tailpiece has no effect on enzymatic activity. Here we show that bipolar tetrameric, hexameric, and octameric minifilaments of AMII with the nonhelical tailpiece serines either phosphorylated or mutated to glutamate have longer bare zones and more tightly clustered heads than minifilaments of unphosphorylated AMII, irrespective of the phosphorylation state of Ser639. Although antiparallel dimers of phosphorylated and unphosphorylated myosins are indistinguishable, phosphorylation inhibits dimerization and filament assembly. Therefore, the different structures of tetramers, hexamers, and octamers of phosphorylated and unphosphorylated AMII must be caused by differences in the longitudinal stagger of phosphorylated and unphosphorylated bipolar dimers and tetramers. Thus, although the actin-activated MgATPase activity of AMII is regulated by phosphorylation of Ser639 in loop 2 of the motor domain, the structure of AMII minifilaments is regulated by phosphorylation of one or more of four serines in the nonhelical tailpiece of the heavy chain.A s summarized in the accompanying paper (1), Acanthamoeba myosin II (AMII) is a typical class II myosin with two heavy chains and two pairs of light chains (2, 3). The coiled-coil helical tails of the heavy chains terminate with a 27-residue nonhelical tailpiece, 1483PSSRGGSTRGASARGASVRAGSARAEE1509, which has a pattern of four contiguous repeats of XXSXR (4). Previous work had shown that phosphorylation of two or more of these serines (residues 1489, 1494, 1499, and 1504) correlates with, and was assumed to be responsible for, inactivation of AMII's actin-activated MgATPase activity (5, 6). Also, it had been concluded that only filamentous AMII has actin-activated MgATPase activity (7, 8), and it was inferred that the ATPase activity is regulated by a change in the conformation of the bipolar minifilaments (9-11). However, detailed studies by the Pollard laboratory found no significant differences in either the polymerization properties or electron microscopic images of minifilaments of phosphorylated and dephosphorylated myosins (12-16).The earlier studies were carried out with purified endogenous myosin. To avoid possible complications in enzymatic and structural studies caused by the partial phosphorylation of purified endogenous myosin and incomplete dephosphorylation by phosphatase, we initiated studies on the enzymatic activity and structure of expressed recombinant wild-type, truncated, and mutant myosins before and after phos...

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Non-muscle Myosin II Motor Proteins in Human Health and Diseases

Betapudi

2017

Genome Analysis and Human Health

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Myosin II Tailpiece Determines Its Paracrystal Structure, Filament Assembly Properties, and Cellular Localization

Cited by 49 publications

References 46 publications

The Positively Charged Region of the Myosin IIC Non-helical Tailpiece Promotes Filament Assembly

The Positively Charged Region of the Myosin IIC Non-helical Tailpiece Promotes Filament Assembly

Regulation of the filament structure and assembly ofAcanthamoebamyosin II by phosphorylation of serines in the heavy-chain nonhelical tailpiece

Non-muscle Myosin II Motor Proteins in Human Health and Diseases

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