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From the BBC:

bb Wrote:
Gene therapy 'corrects fragile X'
X chromosome
Fragile X is linked to over-activity in the brain
Gene therapy has been used to alleviate symptoms of a condition which is a leading cause of inherited learning difficulties and autism.

There is currently no treatment for fragile X syndrome, also linked to epilepsy and abnormal body growth, but the new work raises hopes of progress.

A Massachusetts team were able to trigger big improvements in mice by tweaking just one gene.

The results of the study are published in the journal Neuron.


These findings have major therapeutic implications for fragile X syndrome and autism
Dr Mark Bear
Picower Institute for Learning and Memory

Fragile X is caused by the loss of a gene called FMRP which produces a protein which acts as a brake on protein synthesis in specific areas of brain circuitry.

The theory is that this allows another protein - mGluR5 - which stimulates this process to function unchecked, resulting in over-activity in the brain.

The researchers, from the Picower Institute for Learning and Memory at Massachusetts Institute of Technology, examined mice which lack the FMRP gene, and show many of the symptoms associated with fragile X.

They also created mice that not only lacked FMRP, but also had a 50% reduction in mGluR5.

Fewer abnormalities

This second group of mice showed fewer symptoms of fragile X, fewer signs of abnormalities in the brain, and fewer signs of abnormal body growth.


FRAGILE X SYNDROME
Boys usually more severely affected
Main problem is mental impairment
Other symptoms include hyperactivity, attention deficit disorder, emotional and behavioural problems, anxiety and mood swings
There may also be characteristic facial features, such as a long face and large ears
Other physical features include flat feet and hyperextensible joints

For example, loss of the FMRP gene produces overgrowth of connections between nerve cells called dendritic spines.

However, when coupled with a 50% reduction in mGluR5, spine density was completely normal.

The 'double mutant' mice also showed substantial reduction in epileptic seizures.

Lead researcher Dr Mark Bear said: "These findings have major therapeutic implications for fragile X syndrome and autism."

Dr Mark Hirst, scientific adviser to UK Fragile X Society, said: "Whilst we know that many proteins are regulated by the fragile X protein, and are therefore disrupted in fragile X individuals, mGluR5 seems to be one of the most important."

However, he stressed that the mice in the study had benefited from reduced levels of mGluR5 throughout their development - something it would be not be able to replicate in a human drug treatment.

He added: "We must not take our eye off the other proteins that are mis-regulated, as the basis of fragile X syndrome is likely to be more complex and involve other pathways."

Progress marches on, and Science makes another discovery. Very intriguing.

pikajedi4 Wrote:
Cure found for LFA.


Sensationalism much?

Feel I don't know much about this.

Some  people are probably going to grab a such treatment as soon as it gets available. We might wait and see what happens to them or their children.
I think people should be wary of these kinds of treatments.

If the positive anecdotes aren't much different than those of alternative treatments for autism it probably has little or no effect.
What exactly happens to people who get the gene-therapy should be investigated, it might not be that positive even though it might seem that you get rid of the condition.
There is a prenatal genetic test for Fragile X.  So how many pregnancies are terminated (or babies murdered in some people's opinion)?  From a company who makes the test "Fragile X (Fra X) syndrome is the most common inherited type of mental retardation. It occurs in about 1 in 3600 males and 1 in 4000 females."  So it is not even being called autism but mental retardation.  Is anyone going to develop and manufacture gene therapy when there is such a small market for it?

Divide and conquer.  They will eliminate us all.
Gene therapy for Downs...
It is a long leap there- The experiment doesn't actually say what kind of gene therapy, when, or even if it was even used. The quoted experiment used the oldschool technique of mutation and mutation-mutation interaction to test biological interactions. In my opinion, It sounds like they used gene therapy technique to cause a gene knock out event for the second mutation. But well if your grant proposal is on the slate and you need a meal ticket, calling it the former might stir up more interest. In other words- "gene therapy" is more sensational than "gene knock out".

Am I really the only scientist here? Tongue

Gene therapy is more of a curebie threat than you may realize- It is capable of reaching higher efficiency than the current ideal in eugenics, which is to terminate via prenatal. Gene therapy can be used to alter the germ line DNA (gonads) so that only offspring with the ideal DNA are made. It can be made to target exact organs, be permanent or temporary, ect..

On a side note, gene therapy is what created doomsday in the most recent Will Smith movie. The zombie things created by the mutation had poor fashion, bad posture, odd gait, poor voice modulation, poor social skills, and had a "cure" forced upon them. By the end of the movie I felt more sympathetic to the zombie antagonist..

Dun dun dun.
But did they have to kill everyone else? I mean, srsly. Wasn't Will Smith acting the last person alive?

matthe

all this new geneitc science stuff scares the #$%@ out of me.
My friend is a carrier for Fragile X - she had three sons before they realised this - her boys are all severely retarded and will require lifetime care and support in a protected environment.

Joker Wrote:
But did they have to kill everyone else? I mean, srsly. Wasn't Will Smith acting the last person alive?

No.. In fact they aren't actually zombies, although it plays like a zombie movie. They are human, sorta.

At the end of the movie I had trouble discerning the antagonist from the protagonist. (if you see it lets make another thread Tongue )

What is "ideal DNA" in the first place?

Is there such a thing as a "perfectly normal" brain?

Is there a "perfect" brain?

Who is making these distinctions?  It troubles me, that they are being made, in the first place.

Batman55 Wrote:
What is "ideal DNA" in the first place?
---
Who is making these distinctions?  It troubles me, that they are being made, in the first place.


I should add that I can understand "ideals" being set as regards to genetic conditions that threaten a person's physical health/reduce lifespan--conditions that practically no one would oppose a "cure" for.  But I don't quite see how you can set an "ideal" in terms of the established neurotypes--who gets to decide which neurological functioning is superior, and which is inferior?

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