| nEUROn | |
|---|---|
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| Role | Experimental Unmanned Combat Air Vehicle |
| Manufacturer | Dassault Aviation |
| Unit cost | €25 million |
| Developed from | AVE-C Moyen Duc |
The Dassault nEUROn is an experimental Unmanned Combat Air Vehicle (UCAV) being developed by the French company Dassault Aviation. This delta wing stealth UCAV project is the final phase of the Dassault LOGIDUC 3-step stealth "combat drone" programme. Until June 2005, the UCAV nEUROn design was a full scale evolution of the twin-engine AVE-C Moyen Duc (2001) tactical UAV whose appearance was inspired by the stealth bomber Northrop Grumman B-2 Spirit. The full scale replica unveiled at the Paris Air Show 2005 revealed the original design was revised to a "less ambitious" single-engine delta. The nEUROn development, originally planned by Dassault as "AVE Grand Duc", evolved to a European cooperation including Swedish Saab, Greek EAB, Swiss RUAG Aerospace, Spanish EADS CASA and Italian Alenia. As a "technology demonstrator", a reduced number of units will be produced to explore new operational concepts for a future generation of autonomous stealth fighter aircraft that will be produced in 2020 or 2025. However Dassault plan to primarily use the data collected by the demonstrator to produce derived UCAVs. The French maker states the nEUROn's Adour engine (tuned from the SEPECAT Jaguar) will be replaced in the production version by a more powerful, specific, engine based on Snecma's M88 from the Dassault Rafale.[1]. According to the DGA, nEUROn test flights will be proceeded in France, Sweden and Italy in early 2010.[2]
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The program has three stated goals:
As a UCAV, nEUROn will be significantly larger and more advanced than other well-known UAV systems like the MQ-1 Predator, with ranges, payloads and capabilities that approach those of manned fighter aircraft. Although the project is not yet closely defined, illustrations and statements by the consortium partners indicate that the nEUROn is envisioned as a competitive system with the American J-UCAS program's Boeing X-45C or Northrop-Grumman X-47B.
Indeed, Saab's February 9, 2006 release notes that nEUROn will be a demonstrator measuring 10 m long by 12 m wide and weighing in at 5 tons. This is roughly the size of a Mirage 2000 fighter. The aircraft will have unmanned autonomous air-to-ground attack capabilities with precision guided munitions, relying on an advanced stealth airframe design to penetrate undetected. Another feature being contemplated is the ability to control squad flight in automatic mode from an advanced fighter like the Rafale or JAS 39 Gripen platform, grouping the nEUROns and controlling the group in a manner similar to many combat real-time strategy computer games.
In 1999, Dassault Aviation launched its LOGIDUC stealth UCAV program, which gave birth to the Dassault AVE-D Petit Duc that flew in July 2000 as the first stealth UAV in Europe, and to the Dassault AVE-C Moyen Duc (2001). Dassault changed the third phase name "Grand Duc" - a full scale advanced version of the Moyen Duc - to the more European sounding nEUROn, as the French project was joined by European partners to reduce its development cost. Great Britain didn't join because it was already involved with an American similar program, neither Germany who desisted officially because the country was unable to afford the financial participation.[1]
During the 2003 Paris Air Show, French Minister of Defence Mme Michèle Alliot-Marie announced a major agreement signed between the French groups EADS France, Dassault Aviation and Thales. The agreement covered a joint-venture to "realise a new unmanned military technology that covers all future activity in combat and strategic reconnaissance aeronautics" i.e. LOGIDUC's phase three, "Grand Duc".
EADS leads a HALE (High Altitude, Long Endurance) UAV project.
Meanwhile, the French defence procurement agency, DGA, acting as the program executive on behalf of the participating countries, has entrusted development of the first nEUROn UCAV demonstrator to Dassault Aviation and its European partners. Sub-contracts have been made with the French industrial firms Thales and EADS France and also with five European firms, Saab (Sweden), EAB (Greece), Alenia (Italy), RUAG Aerospace (Switzerland) and EADS CASA (Spain).
Chief project manager Thierry Prunier comes from Dassault Aviation, and the deputy project managers are Mats Ohlson of Saab and Ermanno Bertolina of Alenia. There is a single link between the executive agency (DGA) and the prime contractor (Dassault), and it will be up to the executive agency to coordinate with the government agencies of the participating countries. It will be up to the prime contractor, meanwhile, to coordinate the work with the other industries.
After Spain joined the programme in early February 2006 (Belgium could join later), work breakdown among the European industrial partners was planned as follows:[3]:
Dassault Aviation: (launched
European project in June 2003)Dassault claims 50% of development and is responsible for the standalone LOGIDUC programme. The nEUROn (2010) will be the third Dassault stealth UAV prototype following the AVE-D Petit Duc (2000) & AVE-C Moyen Duc (2004). The nEUROn project replaces the LOGIDUC final phase AVE Grand Duc.[4][5]
Saab: (joined in
December 22, 2005)Saab claims 25% of development and is also the coordinator for the other Swedish corporations involved.[6]
Alenia Aeronautica: (joined
in mid-2005)Thanks to the technologies developed for the UAV prototype Sky-x (2003) Alenia Aeronautica claims to is the first industrial partner with 22% share of the entire programme. [7]
EADS CASA:
(joined in February 7, 2006)
EAB: (joined in
January 11, 2006)
RUAG: (joined in
mid-2005)
Thales: (joined in June 14,
2005)
EADS France:
(joined in June 2003)The contract is valued at €405 million, and allows industry to begin a three-year system definition and design phase with related low-observability studies. This phase will be followed by the development and assembly phase, and by a first flight in 2011. It is planned that the 2-year flight-test program (2010-2012) will entail about 100 sorties, including the launch of a laser-guided bomb tentatively scheduled for 2012. The initial €400 million budget was increased by €5 million in 2006 due to the addition of a modular bomb bay including a designator and a laser-guided bomb.
On February 2006, DGA had announced that France will provide €202.5 million, half of the program's €405 million ($480 million) budget, while the remaining funds will be supplied by the other participating member nations. In December 2005, the Swedish defence ministry reported the national share would be €75 million, of which €66 million would be financed by Saab AB. The cost of Spain's participation to the program is estimated at €35.5 million, spread over the 2007-2012 period.
Derived production UCAV unit cost is estimated by Dassault to €25 million.
Data from [8]
General characteristics
Performance
Armament
Related development
Comparable aircraft
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| Neuron: neuron (Nerve Cell) | ||
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| NeuroLex ID | sao1417703748 | |
A neuron (pronounced /ˈnjʊərɒn/ N(Y)OOR-on, also known as a neurone or nerve cell) is an excitable cell in the nervous system that processes and transmits information by electrochemical signalling. Neurons are the core components of the brain, the vertebrate spinal cord, the invertebrate ventral nerve cord, and the peripheral nerves. A number of specialized types of neurons exist: sensory neurons respond to touch, sound, light and numerous other stimuli affecting cells of the sensory organs that then send signals to the spinal cord and brain. Motor neurons receive signals from the brain and spinal cord and cause muscle contractions and affect glands. Interneurons connect neurons to other neurons within the same region of the brain or spinal cord. Neurons respond to stimuli, and communicate the presence of stimuli to the central nervous system, which processes that information and sends responses to other parts of the body for action. Neurons do not go through mitosis, and usually cannot be replaced after being destroyed, although astrocytes have been observed to turn into neurons as they are sometimes pluripotent.
| Neuron |
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The complexity and diversity in nervous systems is dependent on the interconnections between neurons, which rely on a limited number of different signals transmitted within the neurons to other neurons or to muscles and glands. The signals are produced and propagated by chemical ions that produce an electrical charge that moves along the neuron.
Neurons exist in a number of different shapes and sizes and can be classified by their morphology and function. The anatomist Camillo Golgi grouped neurons into two types; type I with long axons used to move signals over long distances and type II without axons. Type I cells can be further divided by where the cell body or soma is located. The basic morphology of type I neurons, represented by spinal motor neurons, consists of a cell body called the soma and a long thin axon which is covered by the myelin sheath. Around the cell body is a branching dendritic tree that receives signals from other neurons. The end of the axon has branching terminals (axon terminal) that release neurotransmitters into a gap called the synaptic cleft between the terminals and the dendrites of the next neuron. The anatomy and the properties of the surface membrane determine the behavior of a neuron. The surface membrane is not uniform over the entire length of a neuron, but is modified in specific areas: some regions secrete transmitter substances while other areas respond to the transmitter. Other areas of the neuron membrane have passive electrical properties that affect capacitance and resistance. Within the neuron membrane there are gated ion channels that vary in type, including fast response sodium channels that are voltage-gated and are used to send rapid signals.
Neurons communicate by chemical and electrical synapses in a process known as synaptic transmission. The fundamental process that triggers synaptic transmission is the action potential, a propagating electrical signal that is generated by exploiting the electrically excitable membrane of the neuron. This is also known as a wave of depolarization.
Fully differentiated neurons are permanently amitotic;[1] however, recent research shows that additional neurons throughout the brain can originate from neural stem cells found throughout the brain but in particularly high concentrations in the subventricular zone and subgranular zone through the process of neurogenesis.[2][3][4][5]
The neuron's place as the primary functional unit of the nervous system was first recognized in the early 20th century through the work of the Spanish anatomist Santiago Ramón y Cajal.[6] Cajal proposed that neurons were discrete cells that communicated with each other via specialized junctions, or spaces, between cells.[6] This became known as the neuron doctrine, one of the central tenets of modern neuroscience.[6] To observe the structure of individual neurons, Cajal used a silver staining method developed by his rival, Camillo Golgi.[6] The Golgi stain is an extremely useful method for neuroanatomical investigations because, for reasons unknown, it stains a very small percentage of cells in a tissue, so one is able to see the complete micro structure of individual neurons without much overlap from other cells in the densely packed brain.[7]
ated vertebrate motoneuron.]]
Neurons are highly specialized for the processing and transmission of cellular signals. Given the diversity of functions performed by neurons in different parts of the nervous system, there is, as expected, a wide variety in the shape, size, and electrochemical properties of neurons. For instance, the soma of a neuron can vary from 4 to 100 micrometers in diameter.[8]
Although the canonical view of the neuron attributes dedicated functions to its various anatomical components, dendrites and axons often act in ways contrary to their so-called main function.
Axons and dendrites in the central nervous system are typically only about one micrometer thick, while some in the peripheral nervous system are much thicker. The soma is usually about 10–25 micrometers in diameter and often is not much larger than the cell nucleus it contains. The longest axon of a human motoneuron can be over a meter long, reaching from the base of the spine to the toes. Sensory neurons have axons that run from the toes to the dorsal columns, over 1.5 meters in adults. Giraffes have single axons several meters in length running along the entire length of their necks. Much of what is known about axonal function comes from studying the squid giant axon, an ideal experimental preparation because of its relatively immense size (0.5–1 millimeters thick, several centimeters long).
expressing green fluorescent protein. The red staining indicates GABAergic interneurons. Source PLoS Biology [1] ]]
.]]
Most neurons can be anatomically characterized as:
Furthermore, some unique neuronal types can be identified according to their location in the nervous system and distinct shape. Some examples are:
Afferent and efferent can also refer generally to neurons which, respectively, bring information to or send information from the brain region.
A neuron affects other neurons by releasing a neurotransmitter that binds to chemical receptors. The effect upon the target neuron is determined not by the source neuron or by the neurotransmitter, but by the type of receptor that is activated. A neurotransmitter can be thought of as a key, and a receptor as a lock: the same type of key can here be used to open many different types of locks. Receptors can be classified broadly as excitatory (causing an increase in firing rate), inhibitory (causing a decrease in firing rate), or modulatory (causing long-lasting effects not directly related to firing rate).
In fact, however, the two most common neurotransmitters in the brain, glutamate and GABA, have actions that are largely consistent. Glutamate acts on several different types of receptors, but most of them have effects that are excitatory. Similarly GABA acts on several different types of receptors, but all of them have effects (in adult animals, at least) that are inhibitory. Because of this consistency, it is common for neuroscientists to simplify the terminology by referring to cells that release glutamate as "excitatory neurons," and cells that release GABA as "inhibitory neurons." Since well over 90% of the neurons in the brain release either glutamate or GABA, these labels encompass the great majority of neurons. There are also other types of neurons that have consistent effects on their targets, for example "excitatory" motor neurons in the spinal cord that release acetylcholine, and "inhibitory" spinal neurons that release glycine.
The distinction between excitatory and inhibitory neurotransmitters is not absolute, however. Rather, it depends on the class of chemical receptors present on the target neuron. In principle, a single neuron, releasing a single neurotransmitter, can have excitatory effects on some targets, inhibitory effects on others, and modulatory effects on other still. For example, photoreceptors in the retina constantly release the neurotransmitter glutamate in the absence of light. So-called OFF bipolar cells are, like most neurons, excited by the released glutamate. However, neighboring target neurons called ON bipolar cells are instead inhibited by glutamate, because they lack the typical ionotropic glutamate receptors and instead express a class of inhibitory metabotropic glutamate receptors.[10] When light is present, the photoreceptors cease releasing glutamate, which relieves the ON bipolar cells from inhibition, activating them; this simultaneously removes the excitation from the OFF bipolar cells, silencing them.
Neurons can be classified according to their electrophysiological characteristics:
Neurons differ in the type of neurotransmitter they manufacture. Some examples are
Neurons communicate with one another via synapses, where the axon terminal or en passant boutons (terminals located along the length of the axon) of one cell impinges upon another neuron's dendrite, soma or, less commonly, axon. Neurons such as Purkinje cells in the cerebellum can have over 1000 dendritic branches, making connections with tens of thousands of other cells; other neurons, such as the magnocellular neurons of the supraoptic nucleus, have only one or two dendrites, each of which receives thousands of synapses. Synapses can be excitatory or inhibitory and will either increase or decrease activity in the target neuron. Some neurons also communicate via electrical synapses, which are direct, electrically-conductive junctions between cells.
In a chemical synapse, the process of synaptic transmission is as follows: when an action potential reaches the axon terminal, it opens voltage-gated calcium channels, allowing calcium ions to enter the terminal. Calcium causes synaptic vesicles filled with neurotransmitter molecules to fuse with the membrane, releasing their contents into the synaptic cleft. The neurotransmitters diffuse across the synaptic cleft and activate receptors on the postsynaptic neuron.
The human brain has a huge number of synapses. Each of the 1011 (one hundred billion) neurons has on average 7,000 synaptic connections to other neurons. It has been estimated that the brain of a three-year-old child has about 1015 synapses (1 quadrillion). This number declines with age, stabilizing by adulthood. Estimates vary for an adult, ranging from 1014 to 5 x 1014 synapses (100 to 500 trillion).[13]
In 1937, John Zachary Young suggested that the squid giant axon could be used to study neuronal electrical properties.[14] Being larger than but similar in nature to human neurons, squid cells were easier to study. By inserting electrodes into the giant squid axons, accurate measurements were made of the membrane potential.
The cell membrane of the axon and soma contain voltage-gated ion channels which allow the neuron to generate and propagate an electrical signal (an action potential). These signals are generated and propagated by charge-carrying ions including sodium (Na+), potassium (K+), chloride (Cl-), and calcium (Ca2+).
There are several stimuli that can activate a neuron leading to electrical activity, including pressure, stretch, chemical transmitters, and changes of the electric potential across the cell membrane.[15] Stimuli cause specific ion-channels within the cell membrane to open, leading to a flow of ions through the cell membrane, changing the membrane potential.
Thin neurons and axons require less metabolic expense to produce and carry action potentials, but thicker axons convey impulses more rapidly. To minimize metabolic expense while maintaining rapid conduction, many neurons have insulating sheaths of myelin around their axons. The sheaths are formed by glial cells: oligodendrocytes in the central nervous system and Schwann cells in the peripheral nervous system. The sheath enables action potentials to travel faster than in unmyelinated axons of the same diameter, whilst using less energy. The myelin sheath in peripheral nerves normally runs along the axon in sections about 1 mm long, punctuated by unsheathed nodes of Ranvier which contain a high density of voltage-gated ion channels. Multiple sclerosis is a neurological disorder that results from demyelination of axons in the central nervous system.
Some neurons do not generate action potentials, but instead generate a graded electrical signal, which in turn causes graded neurotransmitter release. Such nonspiking neurons tend to be sensory neurons or interneurons, because they cannot carry signals long distances.
The conduction of nerve impulses is an example of an all-or-none response. In other words, if a neuron responds at all, then it must respond completely. The greater the intensity of stimulation does not produce a stronger signal but can produce more impulses per second. There are different types of receptor response to stimulus, slowly adapting or tonic receptors respond to steady stimulus and produce a steady rate of firing. These tonic receptors most often respond to increased intensity of stimulus by increasing their firing frequency, usually as a power function of stimulus plotted against impulses per second. This can be likened to an intrinsic property of light where to get greater intensity of a specific frequency (color) there has to be more photons, as the photons can't become "stronger" for a specific frequency.
There are a number of other receptor types that are called quickly adapting or phasic receptors, where firing decreases or stops with steady stimulus, examples include; skin when touched by an object causes the neurons to fire, but if the object maintains even pressure against the skin the neurons stop firing. The neurons of the skin and muscles that are responsive to pressure and vibration have filtering accessory structures that aid their function. The pacinian corpuscle is one such structure, it has concentric layers like an onion which form around the axon terminal. When pressure is applied and the corpuscle is deformed, mechanical stimulus is transferred to the axon, which fires. If the pressure is steady there is no more stimulus, thus typically these neurons respond with a transient depolarization during the initial deformation and again when the pressure is removed which cause the corpuscle to change shape again. Other types of adaptation are important in extending the function of a number of other neurons.[16]
tissue.]]
Nerve cell bodies stained with basophilic dyes show numerous microscopic clumps of Nissl substance (named after German psychiatrist and neuropathologist Franz Nissl, 1860–1919), which consists of rough endoplasmic reticulum and associated ribosomal RNA. The prominence of the Nissl substance can be explained by the fact that nerve cells are metabolically very active, and hence are involved in large amounts of protein synthesis.
The cell body of a neuron is supported by a complex meshwork of structural proteins called neurofilaments, which are assembled into larger neurofibrils. Some neurons also contain pigment granules, such as neuromelanin (a brownish-black pigment, byproduct of synthesis of catecholamines) and lipofuscin (yellowish-brown pigment that accumulates with age).
There are different internal structural characteristics between axons and dendrites. Axons typically almost never contain ribosomes, except some in the initial segment. Dendrites contain granular endoplasmic reticulum or ribosomes, with diminishing amounts with distance from the cell body.
The neuron doctrine is the now fundamental idea that neurons are the basic structural and functional units of the nervous system. The theory was put forward by Santiago Ramón y Cajal in the late 19th century. It held that neurons are discrete cells (not connected in a meshwork), acting as metabolically distinct units.
As with all doctrines, there are some exceptions. For example glial cells may also play a role in information processing.[17] Also, electrical synapses are more common than previously thought,[18] meaning that there are direct, cytoplasmic connections between neurons. In fact, there are examples of neurons forming even tighter coupling; the squid giant axon arises from the fusion of multiple neurons that retain individual cell bodies and the crayfish giant axon consists of a series of neurons with high conductance septate junctions[citation needed].
Cajal also postulated the Law of Dynamic Polarization, which states that a neuron receives signals at its dendrites and cell body and transmits them, as action potentials, along the axon in one direction: away from the cell body.[19] The Law of Dynamic Polarization has important exceptions; dendrites can serve as synaptic output sites of neurons[20] and axons can receive synaptic inputs[citation needed].
The number of neurons in the brain varies dramatically from species to species.[21] One estimate puts the human brain at about 100 billion () neurons and 100 trillion () synapses.[21] Another estimate is 86 billion neurons of which 16.3 are in the cerebral cortex and 69 in the cerebellum.[22] By contrast, the nematode worm Caenorhabditis elegans has just 302 neurons making it an ideal experimental subject as scientists have been able to map all of the organism's neurons. By contrast, the fruit fly Drosophila melanogaster has around 100,000 neurons and exhibits many complex behaviors. Many properties of neurons, from the type of neurotransmitters used to ion channel composition, are maintained across species, allowing scientists to study processes occurring in more complex organisms in much simpler experimental systems.
Alzheimer's disease (AD), also known simply as Alzheimer's, is a neurodegenerative disease characterized by progressive cognitive deterioration together with declining activities of daily living and neuropsychiatric symptoms or behavioral changes. The most striking early symptom is loss of short-term memory (amnesia), which usually manifests as minor forgetfulness that becomes steadily more pronounced with illness progression, with relative preservation of older memories. As the disorder progresses, cognitive (intellectual) impairment extends to the domains of language (aphasia), skilled movements (apraxia), recognition (agnosia), and functions such as decision-making and planning get impaired.
Parkinson's disease (also known as Parkinson disease or PD) is a degenerative disorder of the central nervous system that often impairs the sufferer's motor skills and speech. Parkinson's disease belongs to a group of conditions called movement disorders. It is characterized by muscle rigidity, tremor, a slowing of physical movement (bradykinesia), and in extreme cases, a loss of physical movement (akinesia). The primary symptoms are the results of decreased stimulation of the motor cortex by the basal ganglia, normally caused by the insufficient formation and action of dopamine, which is produced in the dopaminergic neurons of the brain. Secondary symptoms may include high level cognitive dysfunction and subtle language problems. PD is both chronic and progressive.
Myasthenia Gravis is a neuromuscular disease leading to fluctuating muscle weakness and fatigability. Weakness is typically caused by circulating antibodies that block acetylcholine receptors at the post-synaptic neuromuscular junction, inhibiting the stimulative effect of the neurotransmitter acetylcholine. Myasthenia is treated with immunosuppressants, cholinesterase inhibitors and, in selected cases, thymectomy.
Demyelination is the act of demyelinating, or the loss of the myelin sheath insulating the nerves. When myelin degrades, conduction of signals along the nerve can be impaired or lost, and the nerve eventually withers. This leads to certain neurodegenerative disorders like multiple sclerosis, chronic inflammatory demyelinating polyneuropathy.
Although most injury responses include a calcium influx signaling to promote resealing of severed parts, axonal injuries initially lead to acute axonal degeneration (AAD), which is rapid separation of the proximal and distal ends within 30 minutes of injury. Degeneration follows with swelling of the axolemma, and eventually leads to bead like formation. Granular disintegration of the axonal cytoskeleton and inner organelles occurs after axolemma degradation. Early changes include accumulation of mitochondria in the paranodal regions at the site of injury. Endoplasmic reticulum degrades and mitochondria swell up and eventually disintegrate. The disintegration is dependent on Ubiquitin and Calpain proteases (caused by influx of calcium ion), suggesting that axonal degeneration is an active process. Thus the axon undergoes complete fragmentation. The process takes about roughly 24 hrs in the PNS, and longer in the CNS. The signaling pathways leading to axolemma degeneration are currently unknown.
Although neurons do not divide or replicate in most parts of the adult vertebrate brain, it is often possible for axons to regrow if they are severed. This can take a long time: after a nerve injury to the human arm, for example, it may take months for feeling to return to the hands and fingers.[citation needed]
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Wikimedia Commons has media related to: Neuron |
[[File:|thumb|right|230px|diagram of neuron]] [[File:|thumb|right|230px|diagram of neuron]] Neurons are also called nerve cells. Neurons are the basic units of the nervous system and its most important part, the brain.
Every neuron has a cell body (sometimes called a soma) and nerve fibres (called axons and dendrites). There are about 100 billion neurons in the human brain.
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There are three classes of neurons: afferent neurons, efferent neurons, and interneurons.
Sensory neurons carry signals from sense organs to the spinal cord and brain.
Relay neurons carry messages from one part of the CNS.
Motor neurons carry signals from the CNS to muscles, motor neurons are connected to the relay neurons. The signal passes between the neurons via synapses. Synapses are microscopic voids between cells where chemicals are released from the axon terminal of one cell to specialized chemical receptors on the dendrite of the receiving cell.
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