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Recent News and Articles on the Keywords: autism + mit + retardation  Related to the article below (Last Update: 8/5/2008)

Repair for Mental Impairment?
RedOrbit, TX - Jul 6, 2008
So striking were the animal results that scientists are beginning drug trials on people with genetic disorders associated with mental retardation and autism ...
Source: Google News

[PDF] … abilities of individuals with autism, individuals with mental retardation, and normally developing … -
N Yirmiya, O Erel, M Shaked, D Solomonica-Levi - Psychological Bulletin, 1998 - psy.miami.edu
... Meta-Analyses Comparing Theory of Mind Abilities of Individuals With Autism,
Individuals With Mental Retardation, and Normally Developing Individuals ...
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Explaining mental retardation and autism to parents
V Shea - The effects of autism on the family, 1984 - books.google.com
16 Explaining Mental Retardation and Autism to Parents VICTORIA SHEA INTRODUCTION
To be told that his or her child has a serious disability is one of the most ...

… of Motion-defined Forms by Individuals with Mental Retardation and Autism: Evidence of Modifiability -
MT Carlin, SA Soraci, KL Hobbs, MJ Bud - Intelligence, 1999 - Elsevier
... All rights reserved. Detection of Motion-defined Forms by Individuals with
Mental Retardation and Autism: Evidence of Modifiability. ...

… Mind Abilities in Individuals with Autism, Down Syndrome, and Mental Retardation of Unknown Etiology -
N Yirmiya, T Pilowsky, D Solomonica-Levi, C … - Journal of Autism and Developmental Disorders, 1999 - Springer
... emerged between individuals with autism and individ- uals with unknownMR, between
individuals with men- tal retardation (unknown MR vs. ...

Differentiating the behavioural profile in autism and mental retardation and testing of a screener -
HC Steinhausen, C Winkler Metzke - European Child & Adolescent Psychiatry, 2004 - Springer
... Z (2002) Behavioural Profiles in Four Mental Retardation Syndromes: Fetal ... Steinhausen
HC (2004) Leben mit Autismus (Living with Autism), Bern, Huber ...

Autism associated with tetrasomy 15: A further report
M Ghaziuddin, S Sheldon, S Venkataraman, L Tsai, N … - European Child & Adolescent Psychiatry, 1993 - Springer
... have de- scribed the presence of mental retardation but au ... of chromosomal de- fects
in autism, this report ... einer Tetrasomie des Chromosoms 15 mit Autismus bei 6 ...

Neurobiology of Autism, Mental Retardation, and Down Syndrome -
CJ Lawrence, I Lott, RJ Haier - Neurobiology of exceptionality. New York: Kluwer/Plenum, 2005 - Springer
... Dendritic and Synaptic pathology in mental retardation.? Pediatric Neu ... Cambridge:
Mit Press ... for susceptibility genes for infantile autism.? American Journal ...

Modularity in developmental cognitive neuropsychology: Evidence from autism and Gilles de la …
S Baron-Cohen - Handbook of mental retardation and development, 1998 - books.google.com
... Abilities and disabilities in autism and mental retardation. ... from an object: Its
implications for theories of autism. ... Cambridge, MA: MIT Press/Brad- ford Books ...

Supporting Providers of In-Home Care: The Needs of Families with Relatives Who Are Disabled.
M Arnold, T Case - The Journal of Rehabilitation, 1993 - questia.com
... by Mit Arnold , Tom Case. ... residential facilities for persons with mental retardation
serving 16 ... impaired; cerebral palsy; spina bifida; autism; epilepsy; mental ...

Autism and Autistic-like Conditions in Mental Retardation. By D. Kraijer. Swets & Zeitlinger, Lisse, …
R Jordan - The Journal of Child Psychology and Psychiatry and Allied …, 1999 - Cambridge Univ Press
... of these children across the degrees of mental retardation, contrasts the ... experienced
in making accurate diagnoses and detecting autism in those ... MIT Press, 1997 ...
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Source: Google Scholar

MIT corrects inherited retardation, autism in mice

Research points to potential drug treatment

CAMBRIDGE, Mass.- Researchers at MIT's Picower Institute for Learning and Memory have corrected key symptoms of mental retardation and autism in mice.

The work, which will be reported in the Dec. 20 issue of Neuron, also indicates that a certain class of drugs could have the same effect. These drugs are not yet approved by the FDA, but will soon be entering into human clinical trials.

Fragile X syndrome (FXS), affecting 100,000 Americans, is the most common inherited cause of mental retardation and autism. The MIT researchers corrected FXS in mice modeling the disease. “These findings have major therapeutic implications for fragile X syndrome and autism,” said study lead author Mark F. Bear, director of the Picower Institute and Picower Professor of Neuroscience at MIT.

The findings support the theory that many of FXS's psychiatric and neurological symptoms-learning disabilities, autistic behavior, childhood epilepsy- stem from too much activation of one of the brain's chief network managers-the metabotropic glutamate receptor mGluR5.

“Fragile X is a disorder of excess-excess synaptic connectivity, protein synthesis, memory extinction, body growth, excitability-and remarkably, all these excesses can be reduced by reducing mGluR5,” said Bear, a Howard Hughes Medical Institute investigator.

Individuals with FXS have mutations in the X chromosome's FMR1 gene, which encodes the fragile X mental retardation protein, FMRP. The MIT study found that FMRP and mGluR5 are at opposite ends of a kind of molecular seesaw. They keep each other in check, and without FMRP, mGluR5 signals run rampant.

Bear and colleagues study how genes and environment interact to refine connections in the brain. Synapses are the brain's connectors and their modifications are the basis for all learning and memory. There's a growing consensus among researchers that developmental brain disorders such as FXS, autism and schizophrenia should be considered “synapsopathies”- diseases of synaptic development and plasticity (the ability to change in response to experience).

Dendritic spines--little nubs on neurons' branchlike projections-receive many of the synaptic inputs from other neurons. Abnormal spines have long been associated with various forms of human mental retardation. In FXS, spines are more numerous, longer and more spindly than they should be. Thin spines tend to form weak connections.

The research team found that a 50 percent reduction in mGluR5 fixed multiple defects in the fragile X mice. In addition to correcting dendritic spines, reduced mGluR5 improved altered brain development and memory, restored normal body growth, and reduced seizures-many of the symptoms experienced by humans with FXS.

The researchers used genetic engineering to reduce mGluR5, but the same thing could be accomplished by a drug. Although not yet approved by the FDA, mGluR5 blockers are entering into human clinical trials. “Insights gained by this study suggest novel therapeutic approaches, not only for fragile X but also for autism and mental retardation of unknown origin,” Bear said.

Earlier this year, MIT Picower Institute researcher Susumu Tonegawa and colleagues reported positive results using a different approach to reversing FXS symptoms. Tonegawa and colleagues identified a key enzyme called p21-activated kinase, or PAK, that affects the number, size and shape of connections between neurons.

###

In addition to Bear, authors include Brown University graduate student Gul Dolen; Picower Institute postdoctoral fellow Emily Osterweil, B.S. Shankaranarayana Rao of the National Institute of Mental Health and Neuroscience in India; MIT graduate students Gordon B. Smith and Benjamin D. Auerbach; and Sumantra Chattarji of the National Center for Biological Sciences and Tata Institute of Fundamental Research in India.

This work is supported by the National Institute of Mental Health; the National Institute of Child Health and Human Development; the National Fragile X Foundation; FRAXA, a Fragile X research foundation; and the Simons Foundation.

 
 
 
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