Wednesday, September 10, 2014

New Published Study Verifies Andrew Wakefield’s Research on Autism – Again


Controversial Doctor and Autism Media Channel Director proven right - MMR Vaccine Causes Autism & Inflammatory Bowel Disease

Two landmark events – a government concession in the US Vaccine Court, and a groundbreaking scientific paper – confirm that physician, scientist, and Autism Media Channel [AMC] Director, Dr. Andrew Wakefield, and the parents were right all along.
In a recently published December 13, 2012 vaccine court ruling, hundreds of thousands of dollars were awarded to Ryan Mojabi, [i] whose parents described how “MMR vaccinations,” caused a “severe and debilitating injury to his brain, diagnosed as Autism Spectrum Disorder (‘ASD’).”
Later the same month, the government suffered a second major defeat when young Emily Moller from Houston won compensation following vaccine-related brain injury that, once again, involved MMR and resulted in autism. The cases follow similar successful petitions in the Italian and US courts (including Hannah Poling [ii], Bailey Banks [iii], Misty Hyatt [iv], Kienan Freeman [v], Valentino Bocca [vi], and Julia Grimes [vii]) in which the governments conceded or the court ruled that vaccines had caused brain injury. In turn, this injury led to an ASD diagnosis. MMR vaccine was the common denominator in these cases.
And today, scientists and physicians from Wake Forest University, New York, and Venezuela, reported findings that not only confirm the presence of intestinal disease in children with autism and intestinal symptoms, but also indicate that this disease may be novel. [viii] Using sophisticated laboratory methods Dr. Steve Walker and his colleagues endorsed Wakefield’s original findings by showing molecular changes in the children’s intestinal tissues that were highly distinctive and clearly abnormal.
From 1998 Dr. Wakefield discovered and reported intestinal disease in children with autism. [ix] Based upon the medical histories of the children he linked their disease and their autistic regression to the Measles, Mumps, Rubella (MMR vaccine). He has since been subjected to relentless personal and professional attacks in the media, and from governments, doctors and the pharmaceutical industry. In the wake of demonstrably false and highly damaging allegations of scientific fraud by British journalist Brian Deer and the British Medical Journal, Dr. Wakefield is pursuing defamation proceedings against them in Texas. [x]
While repeated studies from around the world confirmed Wakefield’s bowel disease in autistic children [xi] and his position that safety studies of the MMR are inadequate, [xii] Dr. Wakefield ’s career has been destroyed by false allegations.  Despite this he continues to work tirelessly to help solve the autism catastrophe.
The incidence of autism has rocketed to a risk of around 1 in 25 for children born today. Mean while governments, absent any explanation and fearing loss of public trust, continue to deny the vaccine autism connection despite the concessions in vaccine court.
Speaking from his home in Austin, Texas, Dr. Wakefield said, 
There can be very little doubt that vaccines can and do cause autism. In these children, the evidence for a n adverse reaction involving brain injury following the MMR that progresses to an autism diagnosis is compelling. It’s now a question of the body count. The parents’ story was right all along. Governments must stop playing with words while children continue to be damaged . My hope is that recognition of the intestinal disease in these children will lead to the relief of their suffering. This is long , long overdue .”
Dr. Andrew Wakefield is a best selling author, [xi] founder of the autism research non profit Strategic Autism Initiative (SAI), and Director of the Autism Media Channel.

References

and
[iv] Vaccine Case: An Exception Or A Precedent? February 11, 2009 3:20 PM CBS News By Sharyl Attkisson
[ix] Wakefield AJ. Callous Disregard: Autism and Vaccines – The Truth Behind a Tragedy. 2010. Skyhorse Publishing, NY, NY. Chapter 1, footnotes 1 & 4, p.20
[x] For Affidavits see www.DrWakefieldJusticeFund.org
[xi] Wakefield AJ. Waging War on the Autistic Child. 2012 Skyhorse Publishing NY, NY. Chapter 2, footnotes 2 11, pp. 255 256
[xii] Jefferson T et al, Unintended events following immunization with MMR: a systematic review. Vaccine 21 (2003) 3954–3960
Here is a list of 28 studies from around the world that support Dr. Wakefield’s research:
  1. The Journal of Pediatrics November 1999; 135(5):559-63
  2. The Journal of Pediatrics 2000; 138(3): 366-372
  3. Journal of Clinical Immunology November 2003; 23(6): 504-517
  4. Journal of Neuroimmunology 2005 
  5. Brain, Behavior and Immunity 1993; 7: 97-103
  6. Pediatric Neurology 2003; 28(4): 1-3
  7. Neuropsychobiology 2005; 51:77-85
  8. The Journal of Pediatrics May 2005;146(5):605-10
  9. Autism Insights 2009; 1: 1-11
  10. Canadian Journal of Gastroenterology February 2009; 23(2): 95-98
  11. Annals of Clinical Psychiatry 2009:21(3): 148-161
  12. Journal of Child Neurology June 29, 2009; 000:1-6
  13. Journal of Autism and Developmental Disorders March 2009;39(3):405-13
  14. Medical Hypotheses August 1998;51:133-144.
  15. Journal of Child Neurology July 2000; ;15(7):429-35
  16. Lancet. 1972;2:883–884.
  17. Journal of Autism and Childhood Schizophrenia January-March 1971;1:48-62
  18. Journal of Pediatrics March 2001;138:366-372.
  19. Molecular Psychiatry 2002;7:375-382.
  20. American Journal of Gastroenterolgy April 2004;598-605.
  21. Journal of Clinical Immunology November 2003;23:504-517.
  22. Neuroimmunology April 2006;173(1-2):126-34.
  23. Prog. Neuropsychopharmacol Biol. Psychiatry December 30 2006;30:1472-1477.
  24. Clinical Infectious Diseases September 1 2002;35(Suppl 1):S6-S16
  25. Applied and Environmental Microbiology, 2004;70(11):6459-6465
  26. Journal of Medical Microbiology October 2005;54:987-991
  27. Archivos venezolanos de puericultura y pediatrĂ­a 2006; Vol 69 (1): 19-25.
  28. Gastroenterology. 2005:128 (Suppl 2);Abstract-303

Vaccine Epidemicby Louise Kuo Habakus and Mary Holland J.D.
Vaccine Epidemic bookcover New Published Study Verifies Andrew Wakefields Research on Autism   Again
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Friday, June 20, 2014

Single dose of century-old drug approved for sleeping sickness reverses autism-like symptoms in mice

Date:
June 17, 2014
Source:
University of California, San Diego Health Sciences

Summary:
In a further test of a novel theory that suggests autism is the consequence of abnormal cell communication, researchers report that an almost century-old drug approved for treating sleeping sickness also restores normal cellular signaling in a mouse model of autism, reversing symptoms of the neurological disorder in animals that were the human biological age equivalent of 30 years old.
This image depicts the transmission electron micrograph of a cell mitochondrion.
Credit: Thomas Deerinck, NCMIR, UC San Diego
In a further test of a novel theory that suggests autism is the consequence of abnormal cell communication, researchers at the University of California, San Diego School of Medicine report that an almost century-old drug approved for treating sleeping sickness also restores normal cellular signaling in a mouse model of autism, reversing symptoms of the neurological disorder in animals that were the human biological age equivalent of 30 years old.
The findings, published in the June 17, 2014 online issue of Translational Psychiatry, follow up on similar research published last year by senior author Robert K. Naviaux, MD, PhD, professor of medicine, pediatrics and pathology, and colleagues.
Naviaux said the findings fit neatly with the idea that autism is caused by a multitude of interconnected factors: "Twenty percent of the known factors associated with autism are genetic, but most are not. It's wrong to think of genes and the environment as separate and independent factors. Genes and environmental factors interact. The net result of this interaction is metabolism."
Naviaux, who is co-director of the Mitochondrial and Metabolic Disease Center at UC San Diego, said one of the universal symptoms of autism is metabolic disturbances. "Cells have a halo of metabolites (small molecules involved in metabolism, the set of chemical processes that maintain life) and nucleotides surrounding them. These create a sort of chemical glow that broadcasts the state of health of the cell."
Cells threatened or damaged by microbes, such as viruses or bacteria, or by physical forces or by chemicals, such as pollutants, react defensively, a part of the normal immune response, Naviaux said. Their membranes stiffen. Internal metabolic processes are altered, most notably mitochondria -- the cells' critical "power plants." And communications between cells are dramatically reduced. This is the "cell danger response," said Naviaux, and if it persists, the result can be lasting, diverse impairment. If it occurs during childhood, for example, neurodevelopment is delayed.
"Cells behave like countries at war," said Naviaux. "When a threat begins, they harden their borders. They don't trust their neighbors. But without constant communication with the outside, cells begin to function differently. In the case of neurons, it might be by making fewer or too many connections. One way to look at this related to autism is this: When cells stop talking to each other, children stop talking."
Naviaux and colleagues have focused on a cellular signaling system linked to both mitochondrial function and to the cell's innate immune function. Specifically, they have zeroed in on the role of nucleotides like adenosine triphosphate (ATP) and other signaling mitokines -- molecules generated by distressed mitochondria. These mitokines have separate metabolic functions outside of the cell where they bind to and regulate receptors present on every cell of the body. Nineteen types of so-called purinergic receptors are known to be stimulated by these extracellular nucleotides, and the receptors are known to control a broad range of biological characteristics with relevance to autism, such as impaired language and social skills.
In their latest work, Naviaux again tested the effect of suramin, a well-known inhibitor of purinergic signaling that was first synthesized in 1916 and is used to treat trypanosomiasis or African sleeping sickness, a parasitic disease. They found that suramin blocked the extracellular signaling pathway used by ATP and other mitokines in a mouse model of autism spectrum disorder (ASD), ending the cell danger response and related inflammation. Cells subsequently began behaving normally and autism-like behaviors and metabolism in the mice were corrected.
However, the biological and behavioral benefits of suramin were not permanent, nor preventive. A single dose remained effective in the mice for about five weeks, and then washed out. Moreover, suramin cannot be taken long-term since it can result in anemia and adrenal gland dysfunction.
Still, Naviaux said these and earlier findings are sufficiently encouraging to soon launch a small phase 1 clinical trial with children who have ASD. He expects the trial to begin later this year.
"Obviously correcting abnormalities in a mouse is a long way from a cure in humans, but we think this approach -- antipurinergic therapy -- is a new and fresh way to think about and address the challenge of autism.
"Our work doesn't contradict what others have discovered or done. It's another perspective. Our idea is that this kind of treatment -- eliminating a basic, underlying metabolic dysfunction -- removes a hurdle that might make other non-drug behavioral and developmental therapies of autism more effective. The discovery that a single dose of medicine can fundamentally reset metabolism for weeks means that newer and safer drugs might not need to be given chronically. Members of this new class of medicines might need to be given only intermittently during sensitive developmental windows to unblock metabolism and permit improved development in response to many kinds of behavioral and occupational therapies, and to natural play."
Co-authors are Jane C. Naviaux, Michael A. Schuchbauer and Susan B. Powell of the UCSD Department of Psychiatry; Kefeng Li and Lin Wang, UCSD Mitochondrial and Metabolic Disease Center and UCSD Department of Medicine; and Victoria B. Risbrough, UCSD Department of Psychiatry and San Diego Veterans Affairs Center for Excellence in Stress and Mental Health.
Funding for this research came, in part, from the Jane Botsford Johnson Foundation, the National Institutes of Health (grant MH091407), the UCSD Christini Fund, the Wright Family Foundation and the It Takes Guts Foundation.

Story Source:
The above story is based on materials provided by University of California, San Diego Health SciencesNote: Materials may be edited for content and length.

Journal Reference:
  1. J C Naviaux, M A Schuchbauer, K Li, L Wang, V B Risbrough, S B Powell, R K Naviaux. Reversal of autism-like behaviors and metabolism in adult mice with single-dose antipurinergic therapyTranslational Psychiatry, 2014; 4 (6): e400 DOI: 10.1038/tp.2014.33

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Tuesday, March 11, 2014

Healing Spices for Autism

When I first started putting together some recipe's to make my son's foods that he could actually stomach, I paid very close attention to the spices I was using.  I realized that certain spices like Black Pepper, didn't agree with him and usually caused him discomfort, so I read as much as I could about all the other spices I was finding in the Recipe's I was choosing to for him, and low and behold to my surprise, not only were some of the spices I found better for him in that they calmed his stomach, they actually have healing properties.
Here's a list of some of the spices that I've started using for my son, along with their healthful properties.
Cinnamon
Health Benefits: Balances Blood Sugar and preliminary results from test tube and animal studies suggest that cinnamon oil and cinnamon extract have anti-fungal, anti-bacterial, and anti-parasitic properties.  Candida is a Fungus that normally inhabits all humans, but in kids like ours that rarely have balanced diets, candida can easily flare up out of control, especially those on high sugar diets. Study after study has shown that cinnamon can play a role in the everyday management of blood sugar (glucose) levels and other cardiovascular disease (CVD) risk factors.  
As an example of the effectiveness of Cinnamon, in a recent U.S. study, published in the Journal of the American Board of Family Medicine, 109 people with type 2 diabetes were divided into two groups, with one receiving 1 gram of cinnamon a day and one receiving a placebo. After three months, those taking the cinnamon had a 0.83 percent decrease in their A1C, a measure of blood sugar. (Seven percent or less means the diabetes is controlled, and a decrease between 0.5 and 1.0 percent is considered a significant improvement.) Those taking the placebo had only a 0.37 percent decrease in A1C blood-sugar levels.
Cinnamon May also help prevent and treat:
Cancer, cholesterol problems, food poisoning, heart disease, hypertension, insulin resistance, polycystic ovarian syndrome, stroke, ulcer, vaginal yeast infection, wounds.
How to buy cinnamon:
Ground cinnamon begins to fade in flavor after a few months, so it’s best to buy whole cinnamon quills (or sticks) and grind as needed. The quills are somewhat tough, so you’ll need a sturdy spice grinder or fine grater.

Turmeric and Curcumin 
Health Benefits: Reduces Inflammation!  Inflammation is a huge issue with kids with Autism.  Studies have shown that kids with Autism have larger brains than normal and many physicians believe that this is caused by inflammation, so anything that can help reduce inflammation will help children with Autism.  Curcumin also helps with the cure and prevention of Cancer and reducing Candida outbreaks.
Turmeric is widely used in India, in just about every dish the populace prepares.  Researchers, have observed that the incidence of chronic illnesses among people in India is significantly lower than in most Western countries, especially the United States.  The active ingredient in Turmeric is Curcumin, but they can be bought separately and have different characteristics to bring to the spice table.
The best part about Curcumin is that it's even more powerful than drugs like Advil or even prescription medications in reducing inflammation (thereby reducing pain), without the nasty side effect of killing your liver!
May also help prevent and treat:
Acne, allergies, Alzheimer’s, arthritis, asthma, cancer, cholesterol problems, colitis (inflammatory bowel disease), cystic fibrosis, depression, dermatitis, type 2 diabetes, eczema, eye infection, flatulence, gallbladder disease, gout, gum disease, heart disease, high blood pressure, itching, liver disease, macular degeneration, obesity, pain, Parkinson’s disease, pollution side effects, psoriasis, rash, scleroderma, stroke, wounds.
How to buy turmeric:
If possible, I recommend buying turmeric from Alleppey, since it has nearly twice the curcumin of Turmeric sourced anywhere else.
Coriander
Health Benefits: Eases Digestive Discomfort
People often confuse coriander with cilantro, but while Cilantro comes from the strongly scented leaves of the coriander plant, The spice coriander comes from the seeds of the plan. The seed also contains linalool and geranyl acetate, which are powerful antioxidants. They’re the secret behind many of coriander’s powers, including its ability to soothe digestive ailments.
May also help prevent and treat:
Bloating, cholesterol problems, colic, colon cancer, type 2 diabetes, diarrhea, eczema, flatulence, high blood pressure, IBS, indigestion, insomnia, lead poisoning, liver disease, psoriasis, rosacea, stomachache, ulcer, vaginal yeast infection.
How to buy coriander:
Coriander seeds come in two main varieties: European coriander — which accounts for the majority of the U.S. market — is spherical in shape and more flavorful because of its higher concentration of volatile oils. Indian coriander is more egg-shaped and contains some oils not found in European coriander, resulting in a more lemony scent. Both are pretty interchangeable in cooking. Coriander is also sold powdered, but it’s best to buy whole seeds, as the oils dissipate after a few months once ground.
Fennel Seed
Health Benefits: Calms Colic in Baby's along with Menstrual Cramps
Fennel has also been shown to calm colic in babies. In a study, doctors treated 125 infants with colic, dividing them into one group that received a product containing fennel seed oil and one that received a placebo. The fennel seed product eliminated colic in 65 percent of the babies given it, compared with 24 percent of the placebo group.  We all know that with our kids, they're often suffering from one stomach ailment after another and anything that can help them out, while adding a nice licorice like flavor has to be good!
May also help prevent and treat:
Alzheimer’s, arthritis, cancer, colitis (inflammatory bowel disease), dementia, glaucoma, heart disease, high blood pressure, unwanted hair growth in women and stroke.
How to buy fennel seed:
Fennel seeds are sold whole or ground. Whole fennel seeds are yellow and tinged with green, which indicates top quality. Ground fennel starts to lose its flavor after six months, while whole fennel seeds keep for three years, so it’s best to buy whole and grind as needed.
Ginger
Health Benefits: Quiets Queasiness
For thousands of years, traditional healers worldwide have turned to ginger to help ease nausea of all kinds. For the past few decades, scientists have been proving that ginger works.
A team of gastroenterologists from the University of Michigan and National Yang-Ming University in Taiwan decided to study the effects of using ginger on 13 people with a history of motion sickness. To do so, they asked the people to sit in a spinning chair. They all became nauseated. When the volunteers took 1,000 to 2,000 milligrams of ginger before they sat in the chair, it took them longer to develop nausea, and the nausea was also less intense. (Both doses worked equally well.)
In their study, the researchers also measured blood levels of vasopressin, a key hormone they theorized might play a role in nausea from motion sickness. They found ginger limited the release of vasopressin. The researchers also measured electrical activity in the stomach during the spinning and found that ginger kept the activity “relatively stable” as compared with “chaotic” activity without the spice.
May also help prevent and treat:
Arthritis, asthma, cancer, cholesterol problems, heart attack, heartburn, indigestion, migraine, morning sickness, motion sickness, nausea, stroke, elevated triglycerides.
How to buy ginger:
Opt for fresh gingerroot over the dried, ground stuff, which has a less enticing aroma and far less zip. When buying fresh gingerroot, look for knobs (called “hands”) that are firm with smooth skin. Store fresh, peeled ginger in a paper bag in the refrigerator, where it will keep for two weeks. You can also keep unpeeled ginger indefinitely by freezing it in a freezer bag.
I've just touched the tip of the iceberg here, there are literally dozens of other spices and foods that can help out with ailments, just look around, keep an open mind and enjoy the new flavors in your life!

Wednesday, March 05, 2014

Jump Zone Autism Play Date

Jump Zone Autism Play Date
March 11th 3PM to 7PM
  • Come Join FAN for a fun-filled JUMPING afternoon in a safe, accepting environment!
  • Kids ages 2-12 are welcome to jump!
  • Jump Zone is offering our kids a discounted price of just $5.00 per child for this event.
  • Kids don't forget your socks!
Jump Zone Sunrise
(954) 703-1330
10064 W. Oakland Park Blvd
Sunrise, FL 33351

Please RSVP to cate521105@aol.com, as Jump Zone will add a staff member for every 20 children attending!  Parents must remain onsite to supervise their children.

Friday, February 21, 2014

FREE CARD soccer clinics

CARD, along with Tire Choice and the Ft. Lauderdale Strikers, are sponsoring a second soccer clinic FREE for families registered with CARD. The clinics will take place from 10AM-12PM on March 22 and March 29th, 2014 at Christ Church, 4845 NE 25th Ave. Ft. Lauderdale FL 33308

Thursday, February 20, 2014

Vegan Soy Free Pizza Cakes

Lately my son has been having some issues that were very similar to back when he was diagnosed with Eosinophilic Esophagitis.  In other words, I think he's starting to get ulcers again.  I'm partly to blame I've been adding so many new foods to his diet, and there's a possibility that he's reacting badly to some of those foods, so I decided to try more Vegan Soy free stuff.  (Since in addition to being allergic to Milk & Eggs, he's also Allergic to Soy and has low tolerance for Peanuts.

I was looking around the Internet for some inspiration and came across these Pizza Bites, but after making them they seem more to me like Pizza Cakes, hence the name of the Post.  At any rate, I modified the recipe a bit to fit Jonathan's needs.
  • 2 Cups Grated Cauliflower (washed, dried and grated using a food processor or cheese grater by hand until rice-like or thinner – Note – Approximately one head of cauliflower)
  • 1 Tsp Oregano
  • 2 Tsp Parsley
  • 1/4 Tsp Garlic Powder
  • 2 Tbsp Coconut Oil
  • 1-2 Tbsp Frank’s Hot Sauce
  • 1 Flax Egg (1 Tbsp Flaxseed plus 1 Tsp of Egg Replacer and 3 Tbsp Warm Water)
  • 2 Tbsp of Earths Best Soy Free Margarine
  • 1 Cup Chickpeas (Cooked and Drained)
Your first step in this process is to Grind up the Flaxseed.  (I found it easiest to first mix it with the Egg Replacer and Water, then grind it up (I used my wife's RX mixer).











Your second step is to grate the parsley into something that looks like Rice. (Think I'll make Cauliflower "Fried Rice" for Dinner tonight)







Your  Next Step is to take all the ingredients and mix it all in the Blender.
Here, I mix it in High Speed, then normally you would have to remove the mix and mix thoroughly with the Cauliflower, but in my case, with the Ninja, I simply add the rest and blend at Low Speed.
Your Next Step is to put the mix in a muffin tin, sprayed with a good cooking spray.  Make sure you pack it in.  (I had originally filled in Six, but after packing in and scraping off the top, I filled in another two).



















The Final Result is what you see on the first picture on this page.  Bon Appetite!  And guess, what Even my Pickiest Eater, Jonathan ate them!





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