Microtubule organizing center
The microtubule-organizing center (MTOC) is a
structure found in eukaryotic cells from which microtubules emerge. MTOCs have two main functions: the organization of
eukaryotic flagella and cilia and the organization of the mitotic and meiotic spindle apparatus, which separate the chromosomes during cell division. The MTOC is a major site of microtubule nucleation and can be visualized in cells by immunohistochemical detection
of γ-tubulin. The morphological characteristics of MTOCs vary between
the different phyla and kingdoms.[1] In animals, the two most important types of MTOCs are 1) the basal bodies associated with cilia and flagella and 2) the centrosome associated with spindle formation.
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Organization
Microtubule arrangement in a 9+2 axoneme of bronchiolar cilia
Microtubule-organizing centers function as the site where microtubule
formation begins, as well as a location where free-ends of microtubules attract
to.[2] Within the cells, microtubule-organizing centers can take on many
different forms. An array of microtubules can arrange themselves in a pinwheel
structure to form the basal bodies, which can lead to the formation of
microtubule arrays in the cytoplasm or the 9+2 axoneme. Other arrangements range from fungi
spindle pole bodies to the eukaryotic chromosomal kinetochores (flat, laminated plaques). MTOCs can be freely dispersed throughout
the cytoplasm or centrally localized as foci. The most notable MTOCs are the
centrosome at interphase and the mitotic spindle poles.
Centrioles can act as markers for MTOCs in the cell.[2] If they are freely distributed in the cytoplasm, centrioles can
gather during differentiation to become MTOCs. They can also be focused around
a centrosome as a single MTOC, though centrosomes can work as an MTOC absent of
centrioles.
In interphase ]
Most animal cells have one MTOC during interphase, usually located near the nucleus, and generally associated closely with the Golgi apparatus. The MTOC is made up of a pair of centrioles at its center, and is surrounded by pericentriolar
material (PCM) that is important for microtubule nucleation.
Microtubules are anchored at the MTOC by their minus ends, while their plus
ends continue to grow into the cell periphery. The polarity of the microtubules
is important for cellular transport, as the motor proteins kinesin and dynein typically move preferentially in the "plus" and
"minus" directions respectively, along a microtubule, allowing
vesicles to be directed to or from the endoplasmic
reticulum and Golgi apparatus.
Particularly for the Golgi apparatus, structures associated with the apparatus
travel towards the minus end of a microtubule and aid in the overall structure
and site of the Golgi in the cell.[3]
Centrosomes
Main article: Centrosomes
Movements of the microtubules are based on the actions of the centrosome.[1] Each daughter cell after the cessation of mitosis contains one
primary MTOC.[2] Before cell division begins, the interphase MTOC replicates to form
two distinct MTOCs (now typically referred to as centrosomes). During cell
division, these centrosomes move to opposite ends of the cell and nucleate
microtubules to help form the mitotic/meiotic spindle. If the MTOC does not
replicate, the spindle cannot form, and mitosis ceases prematurely.[1]
γ-tubulin is a protein located at the centrosome that nucleates the
microtubules by interacting with the tubulin monomer subunit in the microtubule
at the minus end.[1] Organization of the microtubules at the MTOC, or centrosome in this
case, is determined by the polarity of the microtubules defined by y-tubulin.[1]
Basal body
Main article: Basal body
In epithelial cells, MTOCs also anchor and organize the microtubules that
make up cilia. As with the centrosome, these MTOCs stabilize and give direction
to the microtubules, in this case to allow unidirectional movement of the
cilium itself, rather than vesicles moving along it.
Spindle pole body ]
Main article: Spindle pole body
In yeasts and some algae, the MTOC is embedded into the nuclear envelope as a spindle pole body. Centrioles do not exist in
the MTOCs of yeast and fungi.[1] In these organisms, the nuclear envelope does not break down during
mitosis and the spindle pole body serves to connect cytoplasmic with nuclear
microtubules. The disc-shaped spindle pole body is organized into three layers:
the central plaque, inner plaque, and outer plaque. The central plaque is
embedded in the membrane, while the inner plaque is an amorphous intranuclear
layer, and the outer plaque is the layer located in the cytoplasm.[1]
In plants
Plant cells lack centrioles or spindle pole bodies except in their
flagellate male gametes, and they are entirely absent in the conifers and flowering plants.[4] Instead, the nuclear envelope itself appears to function as the main
MTOC for microtubule nucleation and spindle organization during plant cell mitosis.
Signal transduction
The MTOC reorients itself during signal transduction, primarily during
wound repair or immune responses.[5] The MTOC is relocalized to a position between the edge of the cell
and the nucleus in cells like macrophages, fibroblasts, and endothelial cells.
Organelles like the Golgi apparatus aid in the reorientation of the MTOC which
can occur rapidly. Transduction signals cause microtubules to grow or contract,
as well as cause the centrosome to become motile. The MTOC is located in a
perinuclear position and contains the negative ends of microtubules while the
positive ends grow rapidly towards the edge of the cell. The Golgi apparatus reorients
along with the MTOC, and together cause the cell to seemingly send a polarized
signal.[5]
In immune responses, upon interaction with a target cell in response to
antigen-specific loaded antigen-presenting cells, immune cells, such as
the T cells, natural
killer cells, and cytotoxic T lymphocytes,
localize their MTOCs near the contact zone between the immune cell and the
target cell. For T cells, the T cell receptor signaling response causes the
reorientation of the MTOC by microtubules shortening to bring the MTOC to the
site of interaction of the T cell receptor.
Referances :
https://en.wikipedia.org/wiki/Microtubule#:~:text=Microtubules%20are%20polymers%20of%20tubulin,between%2011%20and%2015%20nm.
[5]
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