Dendrite
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Dendrite | |
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A human neocortical pyramidal neuron stained via Golgi technique. Notice the apical dendrite extending vertically above the soma and the numerous basal dendrites radiating laterally from the base of the cell body. |
- For other uses, see Dendrite (disambiguation).
Dendrites (from Greek dendron, “tree”) are the branched projections of a neuron that act to conduct the electrical stimulation received from other neural cells to the cell body, or soma, of the neuron from which the dendrites project. Electrical stimulation is transmitted onto dendrites by upstream neurons via synapses which are located at various points throughout the dendritic arbor. Dendrites play a critical role in integrating these synaptic inputs and in determining the extent to which action potentials are produced by the neuron.
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[edit] Morphology
Dendrites are made up of dendritic segments which are named according to their relative position to the soma. For example, the initial segment of a dendrite that projects directly from a neuron cell body is called a “first order” segment. When a first order segment branches, its daughter segments are considered “second order” segments. Likewise, daughter segments of second order segments are called “third order” segments. This naming process continues until a dendrite segment ceases to branch. Non-branching dendrites are termed “terminal segments”. In addition, many dendrites contain dendritic spines, small mushroom like protrusions that offer isolated computational compartments on which axon terminals can create synapses.
In general, whereas axons may span the length of nearly a meter, dendrites are more localised around the cell body. Two examples are spinal motor neurons with dendritic arbors of a few millimetres in diameter, and retinal amacrine cells, with arbors of only few hundred micrometers in diameter. Dendrites account for the bulk of the surface area of neurons, with as much as 98% of the neuronal phospholipid bilayer membrane devoted to the dendritic arbor. Additionally, excitatory and inhibitory synapses distribute themselves on the dendritic arbor such that excitatory synapses usually occupy more distal locations while inhibitory synapses are typically located more proximally.
Dendritic morphology, the structural and physical architecture of the dendritic arbor, varies greatly across neuronal type. Dendrites of Purkinje cells, a dominant cell type in the cerebellum, extend from the soma to form a nearly two dimensional arborization. Purkinje cells are stacked in the cerebellum much like dominoes (i.e., with their dendritic arbors parallel to each other) allowing the afferent connections of parallel fibers to run orthogonally through the Purkinje cell dendrites. Pyramidal neurons, the most prevalent excitatory neuron in the cerebral cortex harbour two different classes of dendrites. The apical dendrites extend vertically from the apex of the pyramidally shaped soma and project toward the pial surface of the cerebral hemispheres. The basal dendrites of pyramidal neurons project laterally from the base of the soma. The distinction between different dendrite classes is particularly important for pyramidal neurons as apical dendrites typically receive afferent input from distant sources such as the thalamus while the basal dendrites receive inputs from nearby cortical areas.
[edit] Electrical properties of dendrites
The structure and branching of a neuron's dendrites, as well as the availability and variation in voltage-gated ion conductances, strongly influences how it integrates the input from other neurons, particularly those that input only weakly. This integration is both "temporal" -- involving the summation of stimuli that arrive in rapid succession -- as well as "spatial" -- entailing the aggregation of excitatory and inhibitory inputs from separate branches.
Dendrites were once believed to merely convey stimulation passively. In this example voltage changes measured at the cell body result from activations of distal synapses propagating to the soma without the aid of voltage-gated ion channels. Passive cable theory describes how voltage changes at a particular location on a dendrite transmit this electrical signal through a system of converging dendrite segments of different diameters, lengths, and electrical properties. Based on passive cable theory one can track how changes in a neuron’s dendritic morphology changes the membrane voltage at the soma, and thus how variation in dendrite architectures affects the overall output characteristics of the neuron.
Although passive cable theory offers insights regarding input propagation along dendrite segments, it is important to remember that dendrite membranes are host to a cornucopia of proteins some of which may help amplify or attenuate synaptic input. Sodium, calcium, and potassium channels are all implicated in contributing to input modulation. It is possible that each of these ion species has a family of channel types each with its own biophysical characteristics relevant to synaptic input modulation. Such characteristics include the latency of channel opening, the electrical conductance of the ion pore, the activation voltage, and the activation duration. In this way, a weak input from a distal synapse can be amplified by sodium and calcium currents inroute to the soma so that the effects of distal synapse are no less robust than those of a proximal synapse.
One important feature of dendrites, endowed by their active voltage gated conductances, is their ability to send action potentials back into the dendritic arbor. Known as backpropagating action potentials, these signals depolarize the dendritic arbor and provide a crucial component toward synapse modulation and long-term potentiation.
[edit] Dendrite development
Despite the critical role that dendrites play in the computational tendencies of neurons, very little is known about the process by which dendrites orient themselves in vivo and are compelled to create the intricate branching pattern unique to each specific neuronal class. It is likely that a complex array of extracellular and intracellular cues modulate dendrite development. Early candidates include: Sema3A, Notch, CREST, and Dasm1. Sema3A may act as a dendritic chemoattractant that aids cortical pyramidal neurons in orienting their apical dendrites to the pial surface. Notch acts as a neurotrophic factor in aiding dendrite growth and branching, while CREST may play an important role in regulating calcium dependent growth signals. Dasm1 (Dendrite arborization and synapse maturation 1) expression appears to be highly localized to dendrites and may have substantial influence on dendrite (but not axon) development.
[edit] See also
[edit] References
- Kandel ER, Schwartz JH, Jessell TM. Principles of Neural Science, 4th ed. McGraw-Hill, New York (2000). ISBN 0-8385-7701-6
- Koch C. Biophysics of Computation, Oxford University Press, Oxford (1999). ISBN 0-19-510491-9
- Stuart G, Spruston N, Hausser M. Dendrites, Oxford University Press, USA (2000). ISBN 0-19-850488-8
[edit] External links
- Histology at OU 3_09 - "Slide 3 Spinal cord"