Motor protein

Last updated April 18, 2024

Motor proteins are a class of molecular motors that can move along the cytoskeleton of cells. They convert chemical energy into mechanical work by the hydrolysis of ATP. Flagellar rotation, however, is powered by a proton pump.^{[ citation needed ]}

Cellular functions

Motor proteins are the driving force behind most active transport of proteins and vesicles in the cytoplasm. Kinesins and cytoplasmic dyneins play essential roles in intracellular transport such as axonal transport and in the formation of the spindle apparatus and the separation of the chromosomes during mitosis and meiosis. Axonemal dynein, found in cilia and flagella, is crucial to cell motility, for example in spermatozoa, and fluid transport, for example in trachea. The muscle protein myosin "motors" the contraction of muscle fibers in animals.

Diseases associated with motor protein defects

The importance of motor proteins in cells becomes evident when they fail to fulfill their function. For example, kinesin deficiencies have been identified as the cause for Charcot-Marie-Tooth disease and some kidney diseases. Dynein deficiencies can lead to chronic infections of the respiratory tract as cilia fail to function without dynein. Numerous myosin deficiencies are related to disease states and genetic syndromes. Because myosin II is essential for muscle contraction, defects in muscular myosin predictably cause myopathies. Myosin is necessary in the process of hearing because of its role in the growth of stereocilia so defects in myosin protein structure can lead to Usher syndrome and non-syndromic deafness.^[1]

Cytoskeletal motor proteins

Motor proteins utilizing the cytoskeleton for movement fall into two categories based on their substrate: microfilaments or microtubules. Actin motors such as myosin move along microfilaments through interaction with actin, and microtubule motors such as dynein and kinesin move along microtubules through interaction with tubulin.

There are two basic types of microtubule motors: plus-end motors and minus-end motors, depending on the direction in which they "walk" along the microtubule cables within the cell.

Actin motors

Myosin

Myosins are a superfamily of actin motor proteins that convert chemical energy in the form of ATP to mechanical energy, thus generating force and movement. The first identified myosin, myosin II, is responsible for generating muscle contraction. Myosin II is an elongated protein that is formed from two heavy chains with motor heads and two light chains. Each myosin head contains actin and ATP binding site. The myosin heads bind and hydrolyze ATP, which provides the energy to walk toward the plus end of an actin filament. Myosin II are also vital in the process of cell division. For example, non-muscle myosin II bipolar thick filaments provide the force of contraction needed to divide the cell into two daughter cells during cytokinesis. In addition to myosin II, many other myosin types are responsible for variety of movement of non-muscle cells. For example, myosin is involved in intracellular organization and the protrusion of actin-rich structures at the cell surface. Myosin V is involved in vesicle and organelle transport.^[2]^[3] Myosin XI is involved in cytoplasmic streaming, wherein movement along microfilament networks in the cell allows organelles and cytoplasm to stream in a particular direction.^[4] Eighteen different classes of myosins are known.^[5]

Genomic representation of myosin motors:^[6]

Microtubule motors

Kinesin

Kinesins are a superfamily of related motor proteins that use a microtubule track in anterograde movement. They are vital to spindle formation in mitotic and meiotic chromosome separation during cell division and are also responsible for shuttling mitochondria, Golgi bodies, and vesicles within eukaryotic cells. Kinesins have two heavy chains and two light chains per active motor. The two globular head motor domains in heavy chains can convert the chemical energy of ATP hydrolysis into mechanical work to move along microtubules.^[7] The direction in which cargo is transported can be towards the plus-end or the minus-end, depending on the type of kinesin. In general, kinesins with N-terminal motor domains move their cargo towards the plus ends of microtubules located at the cell periphery, while kinesins with C-terminal motor domains move cargo towards the minus ends of microtubules located at the nucleus. Fourteen distinct kinesin families are known, with some additional kinesin-like proteins that cannot be classified into these families.^[8]

Genomic representation of kinesin motors:^[6]

Dynein

Dyneins are microtubule motors capable of a retrograde sliding movement. Dynein complexes are much larger and more complex than kinesin and myosin motors. Dyneins are composed of two or three heavy chains and a large and variable number of associated light chains. Dyneins drive intracellular transport toward the minus end of microtubules which lies in the microtubule organizing center near the nucleus.^[9] The dynein family has two major branches. Axonemal dyneins facilitate the beating of cilia and flagella by rapid and efficient sliding movements of microtubules. Another branch is cytoplasmic dyneins which facilitate the transport of intracellular cargos. Compared to 15 types of axonemal dynein, only two cytoplasmic forms are known.^[10]

Genomic representation of dynein motors:^[6]

Plant-specific motors

In contrast to animals, fungi and non-vascular plants, the cells of flowering plants lack dynein motors. However, they contain a larger number of different kinesins. Many of these plant-specific kinesin groups are specialized for functions during plant cell mitosis.^[11] Plant cells differ from animal cells in that they have a cell wall. During mitosis, the new cell wall is built by the formation of a cell plate starting in the center of the cell. This process is facilitated by a phragmoplast, a microtubule array unique to plant cell mitosis. The building of cell plate and ultimately the new cell wall requires kinesin-like motor proteins.^[12]

Another motor protein essential for plant cell division is kinesin-like calmodulin-binding protein (KCBP), which is unique to plants and part kinesin and part myosin.^[13]

Other molecular motors

Besides the motor proteins above, there are many more types of proteins capable of generating forces and torque in the cell. Many of these molecular motors are ubiquitous in both prokaryotic and eukaryotic cells, although some, such as those involved with cytoskeletal elements or chromatin, are unique to eukaryotes. The motor protein prestin,^[14] expressed in mammalian cochlear outer hair cells, produces mechanical amplification in the cochlea. It is a direct voltage-to-force converter, which operates at the microsecond rate and possesses piezoelectric properties.

Related Research Articles

Microtubules are polymers of tubulin that form part of the cytoskeleton and provide structure and shape to eukaryotic cells. Microtubules can be as long as 50 micrometres, as wide as 23 to 27 nm and have an inner diameter between 11 and 15 nm. They are formed by the polymerization of a dimer of two globular proteins, alpha and beta tubulin into protofilaments that can then associate laterally to form a hollow tube, the microtubule. The most common form of a microtubule consists of 13 protofilaments in the tubular arrangement.

The cytoskeleton is a complex, dynamic network of interlinking protein filaments present in the cytoplasm of all cells, including those of bacteria and archaea. In eukaryotes, it extends from the cell nucleus to the cell membrane and is composed of similar proteins in the various organisms. It is composed of three main components: microfilaments, intermediate filaments, and microtubules, and these are all capable of rapid growth or disassembly depending on the cell's requirements.

Cytokinesis is the part of the cell division process and part of mitosis during which the cytoplasm of a single eukaryotic cell divides into two daughter cells. Cytoplasmic division begins during or after the late stages of nuclear division in mitosis and meiosis. During cytokinesis the spindle apparatus partitions and transports duplicated chromatids into the cytoplasm of the separating daughter cells. It thereby ensures that chromosome number and complement are maintained from one generation to the next and that, except in special cases, the daughter cells will be functional copies of the parent cell. After the completion of the telophase and cytokinesis, each daughter cell enters the interphase of the cell cycle.

Microfilaments, also called actin filaments, are protein filaments in the cytoplasm of eukaryotic cells that form part of the cytoskeleton. They are primarily composed of polymers of actin, but are modified by and interact with numerous other proteins in the cell. Microfilaments are usually about 7 nm in diameter and made up of two strands of actin. Microfilament functions include cytokinesis, amoeboid movement, cell motility, changes in cell shape, endocytosis and exocytosis, cell contractility, and mechanical stability. Microfilaments are flexible and relatively strong, resisting buckling by multi-piconewton compressive forces and filament fracture by nanonewton tensile forces. In inducing cell motility, one end of the actin filament elongates while the other end contracts, presumably by myosin II molecular motors. Additionally, they function as part of actomyosin-driven contractile molecular motors, wherein the thin filaments serve as tensile platforms for myosin's ATP-dependent pulling action in muscle contraction and pseudopod advancement. Microfilaments have a tough, flexible framework which helps the cell in movement.

<span class="mw-page-title-main">Cleavage furrow</span> Plasma membrane invagination at the cell division site

In cell biology, the cleavage furrow is the indentation of the cell's surface that begins the progression of cleavage, by which animal and some algal cells undergo cytokinesis, the final splitting of the membrane, in the process of cell division. The same proteins responsible for muscle contraction, actin and myosin, begin the process of forming the cleavage furrow, creating an actomyosin ring. Other cytoskeletal proteins and actin binding proteins are involved in the procedure.

Actin is a family of globular multi-functional proteins that form microfilaments in the cytoskeleton, and the thin filaments in muscle fibrils. It is found in essentially all eukaryotic cells, where it may be present at a concentration of over 100 μM; its mass is roughly 42 kDa, with a diameter of 4 to 7 nm.

<span class="mw-page-title-main">Myosin</span> Superfamily of motor proteins

Myosins are a superfamily of motor proteins best known for their roles in muscle contraction and in a wide range of other motility processes in eukaryotes. They are ATP-dependent and responsible for actin-based motility.

A kinesin is a protein belonging to a class of motor proteins found in eukaryotic cells. Kinesins move along microtubule (MT) filaments and are powered by the hydrolysis of adenosine triphosphate (ATP). The active movement of kinesins supports several cellular functions including mitosis, meiosis and transport of cellular cargo, such as in axonal transport, and intraflagellar transport. Most kinesins walk towards the plus end of a microtubule, which, in most cells, entails transporting cargo such as protein and membrane components from the center of the cell towards the periphery. This form of transport is known as anterograde transport. In contrast, dyneins are motor proteins that move toward the minus end of a microtubule in retrograde transport.

<span class="mw-page-title-main">Dynein</span> Class of enzymes

Dyneins are a family of cytoskeletal motor proteins that move along microtubules in cells. They convert the chemical energy stored in ATP to mechanical work. Dynein transports various cellular cargos, provides forces and displacements important in mitosis, and drives the beat of eukaryotic cilia and flagella. All of these functions rely on dynein's ability to move towards the minus-end of the microtubules, known as retrograde transport; thus, they are called "minus-end directed motors". In contrast, most kinesin motor proteins move toward the microtubules' plus-end, in what is called anterograde transport.

Cytoplasmic streaming, also called protoplasmic streaming and cyclosis, is the flow of the cytoplasm inside the cell, driven by forces from the cytoskeleton. It is likely that its function is, at least in part, to speed up the transport of molecules and organelles around the cell. It is usually observed in large plant and animal cells, greater than approximately 0.1 mm. In smaller cells, the diffusion of molecules is more rapid, but diffusion slows as the size of the cell increases, so larger cells may need cytoplasmic streaming for efficient function.

<span class="mw-page-title-main">Molecular motor</span> Biological molecular machines

Molecular motors are natural (biological) or artificial molecular machines that are the essential agents of movement in living organisms. In general terms, a motor is a device that consumes energy in one form and converts it into motion or mechanical work; for example, many protein-based molecular motors harness the chemical free energy released by the hydrolysis of ATP in order to perform mechanical work. In terms of energetic efficiency, this type of motor can be superior to currently available man-made motors. One important difference between molecular motors and macroscopic motors is that molecular motors operate in the thermal bath, an environment in which the fluctuations due to thermal noise are significant.

<span class="mw-page-title-main">Cell cortex</span> Layer on the inner face of a cell membrane

The cell cortex, also known as the actin cortex, cortical cytoskeleton or actomyosin cortex, is a specialized layer of cytoplasmic proteins on the inner face of the cell membrane. It functions as a modulator of membrane behavior and cell surface properties. In most eukaryotic cells lacking a cell wall, the cortex is an actin-rich network consisting of F-actin filaments, myosin motors, and actin-binding proteins. The actomyosin cortex is attached to the cell membrane via membrane-anchoring proteins called ERM proteins that plays a central role in cell shape control. The protein constituents of the cortex undergo rapid turnover, making the cortex both mechanically rigid and highly plastic, two properties essential to its function. In most cases, the cortex is in the range of 100 to 1000 nanometers thick.

<span class="mw-page-title-main">Protein filament</span> Long chain of protein monomers

In biology, a protein filament is a long chain of protein monomers, such as those found in hair, muscle, or in flagella. Protein filaments form together to make the cytoskeleton of the cell. They are often bundled together to provide support, strength, and rigidity to the cell. When the filaments are packed up together, they are able to form three different cellular parts. The three major classes of protein filaments that make up the cytoskeleton include: actin filaments, microtubules and intermediate filaments.

<span class="mw-page-title-main">Molecular biophysics</span> Interdisciplinary research area

Molecular biophysics is a rapidly evolving interdisciplinary area of research that combines concepts in physics, chemistry, engineering, mathematics and biology. It seeks to understand biomolecular systems and explain biological function in terms of molecular structure, structural organization, and dynamic behaviour at various levels of complexity. This discipline covers topics such as the measurement of molecular forces, molecular associations, allosteric interactions, Brownian motion, and cable theory. Additional areas of study can be found on Outline of Biophysics. The discipline has required development of specialized equipment and procedures capable of imaging and manipulating minute living structures, as well as novel experimental approaches.

Dynactin is a 23 subunit protein complex that acts as a co-factor for the microtubule motor cytoplasmic dynein-1. It is built around a short filament of actin related protein-1 (Arp1).

<span class="mw-page-title-main">KIF15</span> Protein-coding gene in the species Homo sapiens

Kinesin family member 15 is a protein that in humans is encoded by the KIF15 gene.

Intracellular transport is the movement of vesicles and substances within a cell. Intracellular transport is required for maintaining homeostasis within the cell by responding to physiological signals. Proteins synthesized in the cytosol are distributed to their respective organelles, according to their specific amino acid’s sorting sequence. Eukaryotic cells transport packets of components to particular intracellular locations by attaching them to molecular motors that haul them along microtubules and actin filaments. Since intracellular transport heavily relies on microtubules for movement, the components of the cytoskeleton play a vital role in trafficking vesicles between organelles and the plasma membrane by providing mechanical support. Through this pathway, it is possible to facilitate the movement of essential molecules such as membrane‐bounded vesicles and organelles, mRNA, and chromosomes.

Neurotubules are microtubules found in neurons in nervous tissues. Along with neurofilaments and microfilaments, they form the cytoskeleton of neurons. Neurotubules are undivided hollow cylinders that are made up of tubulin protein polymers and arrays parallel to the plasma membrane in neurons. Neurotubules have an outer diameter of about 23 nm and an inner diameter, also known as the central core, of about 12 nm. The wall of the neurotubules is about 5 nm in width. There is a non-opaque clear zone surrounding the neurotubule and it is about 40 nm in diameter. Like microtubules, neurotubules are greatly dynamic and the length of them can be adjusted by polymerization and depolymerization of tubulin.

Edwin W. Taylor is an adjunct professor of cell and developmental biology at Northwestern University. He was elected to the National Academy of Sciences in 2001. Taylor received a BA in physics and chemistry from the University of Toronto in 1952; an MSc in physical chemistry from McMaster University in 1955, and a PhD in biophysics from the University of Chicago in 1957. In 2001 Taylor was elected to the National Academy of Scineces in Cellular and Developmental Biology and Biochemistry.

J. Richard McIntosh is a Distinguished Professor Emeritus in Molecular, Cellular, and Developmental Biology at the University of Colorado Boulder. McIntosh first graduated from Harvard with a BA in Physics in 1961, and again with a Ph.D. in Biophysics in 1968. He began his teaching career at Harvard but has spent most of his career at the University of Colorado Boulder. At the University of Colorado Boulder, McIntosh taught biology courses at both the undergraduate and graduate levels. Additionally, he created an undergraduate course in the biology of cancer towards the last several years of his teaching career. McIntosh's research career looks at a variety of things, including different parts of mitosis, microtubules, and motor proteins.

References

↑ Hirokawa N, Takemura R (October 2003). "Biochemical and molecular characterization of diseases linked to motor proteins". Trends in Biochemical Sciences. 28 (10): 558–65. doi:10.1016/j.tibs.2003.08.006. PMID 14559185.
↑ Alberts B, Johnson A, Lewis J, Raff M, Roberts K, Walter P (2002-01-01). "Molecular Motors". NCBI - National Institutes of Health.
↑ Warshaw, DM (February 2012). "Tilting and twirling as myosin V steps along actin filaments as detected by fluorescence polarization". The Journal of General Physiology. 139 (2): 97–100. doi:10.1085/jgp.201210769. PMC 3269787 . PMID 22291143.
↑ Hartman MA, Spudich JA (April 2012). "The myosin superfamily at a glance". Journal of Cell Science. 125 (Pt 7): 1627–32. doi:10.1242/jcs.094300. PMC 3346823 . PMID 22566666.
↑ Thompson RF, Langford GM (November 2002). "Myosin superfamily evolutionary history". The Anatomical Record. 268 (3): 276–89. doi:10.1002/ar.10160. PMID 12382324. S2CID 635349.
1 2 3 Vale RD (February 2003). "The molecular motor toolbox for intracellular transport". Cell. 112 (4): 467–80. doi: 10.1016/S0092-8674(03)00111-9 . PMID 12600311.
↑ Verhey KJ, Kaul N, Soppina V (2011-01-01). "Kinesin assembly and movement in cells". Annual Review of Biophysics. 40: 267–88. doi:10.1146/annurev-biophys-042910-155310. PMID 21332353.
↑ Miki H, Okada Y, Hirokawa N (September 2005). "Analysis of the kinesin superfamily: insights into structure and function". Trends in Cell Biology. 15 (9): 467–76. doi:10.1016/j.tcb.2005.07.006. PMID 16084724.
↑ Roberts AJ, Kon T, Knight PJ, Sutoh K, Burgess SA (November 2013). "Functions and mechanics of dynein motor proteins". Nature Reviews. Molecular Cell Biology. 14 (11): 713–26. doi:10.1038/nrm3667. PMC 3972880 . PMID 24064538.
↑ Mallik R, Gross SP (November 2004). "Molecular motors: strategies to get along". Current Biology. 14 (22): R971-82. doi: 10.1016/j.cub.2004.10.046 . PMID 15556858. S2CID 14240073.
↑ Vanstraelen M, Inzé D, Geelen D (April 2006). "Mitosis-specific kinesins in Arabidopsis". Trends in Plant Science. 11 (4): 167–75. doi:10.1016/j.tplants.2006.02.004. hdl: 1854/LU-364298 . PMID 16530461.
↑ Smith LG (March 2002). "Plant cytokinesis: motoring to the finish". Current Biology. 12 (6): R206-8. doi: 10.1016/S0960-9822(02)00751-0 . PMID 11909547.
↑ Abdel-Ghany SE, Day IS, Simmons MP, Kugrens P, Reddy AS (July 2005). "Origin and evolution of Kinesin-like calmodulin-binding protein". Plant Physiology. 138 (3): 1711–22. doi:10.1104/pp.105.060913. PMC 1176440 . PMID 15951483.
↑ Dallos P, Fakler B (February 2002). "Prestin, a new type of motor protein". Nature Reviews. Molecular Cell Biology. 3 (2): 104–11. doi:10.1038/nrm730. PMID 11836512. S2CID 7333228.

External links

MBInfo - What are Motor Proteins?
Ron Vale's Seminar: "Molecular Motor Proteins"
Biology of Motor Proteins Institute for Biophysical Chemistry, Göttingen
Jonathan Howard (2001), Mechanics of motor proteins and the cytoskeleton. ISBN 9780878933334

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[Hirokawa-1] Hirokawa N, Takemura R (October 2003). "Biochemical and molecular characterization of diseases linked to motor proteins". Trends in Biochemical Sciences. 28 (10): 558–65. doi:10.1016/j.tibs.2003.08.006. PMID 14559185.

[2] Alberts B, Johnson A, Lewis J, Raff M, Roberts K, Walter P (2002-01-01). "Molecular Motors". NCBI - National Institutes of Health.

[Warshaw-3] Warshaw, DM (February 2012). "Tilting and twirling as myosin V steps along actin filaments as detected by fluorescence polarization". The Journal of General Physiology. 139 (2): 97–100. doi:10.1085/jgp.201210769. PMC 3269787 . PMID 22291143.

[4] Hartman MA, Spudich JA (April 2012). "The myosin superfamily at a glance". Journal of Cell Science. 125 (Pt 7): 1627–32. doi:10.1242/jcs.094300. PMC 3346823 . PMID 22566666.

[Thompson-5] Thompson RF, Langford GM (November 2002). "Myosin superfamily evolutionary history". The Anatomical Record. 268 (3): 276–89. doi:10.1002/ar.10160. PMID 12382324. S2CID 635349.

[Vale-6] 1 2 3 Vale RD (February 2003). "The molecular motor toolbox for intracellular transport". Cell. 112 (4): 467–80. doi: 10.1016/S0092-8674(03)00111-9 . PMID 12600311.

[7] Verhey KJ, Kaul N, Soppina V (2011-01-01). "Kinesin assembly and movement in cells". Annual Review of Biophysics. 40: 267–88. doi:10.1146/annurev-biophys-042910-155310. PMID 21332353.

[Miki-8] Miki H, Okada Y, Hirokawa N (September 2005). "Analysis of the kinesin superfamily: insights into structure and function". Trends in Cell Biology. 15 (9): 467–76. doi:10.1016/j.tcb.2005.07.006. PMID 16084724.

[9] Roberts AJ, Kon T, Knight PJ, Sutoh K, Burgess SA (November 2013). "Functions and mechanics of dynein motor proteins". Nature Reviews. Molecular Cell Biology. 14 (11): 713–26. doi:10.1038/nrm3667. PMC 3972880 . PMID 24064538.

[Mallik-10] Mallik R, Gross SP (November 2004). "Molecular motors: strategies to get along". Current Biology. 14 (22): R971-82. doi: 10.1016/j.cub.2004.10.046 . PMID 15556858. S2CID 14240073.

[Vanstraelen-11] Vanstraelen M, Inzé D, Geelen D (April 2006). "Mitosis-specific kinesins in Arabidopsis". Trends in Plant Science. 11 (4): 167–75. doi:10.1016/j.tplants.2006.02.004. hdl: 1854/LU-364298 . PMID 16530461.

[Smith-12] Smith LG (March 2002). "Plant cytokinesis: motoring to the finish". Current Biology. 12 (6): R206-8. doi: 10.1016/S0960-9822(02)00751-0 . PMID 11909547.

[Abdel-Ghany-13] Abdel-Ghany SE, Day IS, Simmons MP, Kugrens P, Reddy AS (July 2005). "Origin and evolution of Kinesin-like calmodulin-binding protein". Plant Physiology. 138 (3): 1711–22. doi:10.1104/pp.105.060913. PMC 1176440 . PMID 15951483.

[14] Dallos P, Fakler B (February 2002). "Prestin, a new type of motor protein". Nature Reviews. Molecular Cell Biology. 3 (2): 104–11. doi:10.1038/nrm730. PMID 11836512. S2CID 7333228.

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