johnson and johnson

10 Feb 2013
Sticky Post By Posted in Advocacy, Media, Newspaper Permalink

The Agonizing Fight for Isaac: The Hope and the Hurdles

Sticky Post By On 10 February, 2013

isaac10lf4Andrew McFadyen lives with the agony of knowing that a ground-breaking treatment for his son’s debilitating disease may be just out of reach.

His son Isaac was born with MPS VI, an extremely rare metabolic disorder. At age 2, Isaac was featured in a Globe and Mail series that led to the Ontario government’s decision to fund Naglazyme, the only available treatment for his disease, which costs an annual $300,000 to $1-million a patient.

But despite receiving weekly injections of the drug, Isaac, now 8, is far from leading a normal life. He is more than a head shorter than other boys his age, and has stopped growing. His hands are clawing up and he is losing mobility in his spine, limbs and joints. He will soon be a candidate for corneal transplants and is at high risk for heart disease and a shortened life.

There is hope. Researchers at Mount Sinai Hospital in New York have come up with an experimental treatment for MPS VI. In a study published January in the online journal PLoS One, rats with the disease showed remarkable improvement in mobility and other indicators after taking pentosan polysulfate, an anti-inflammatory drug that costs about $7 a pill.

McFadyen helped fund the study as head of the Isaac Foundation, an organization he runs in addition to his job as a schoolteacher in Kingston, Ont. “We fully believe this treatment will work wonders,” he says.

But in the world of rare diseases, the battles never end.

Experimental treatments that work in rats are often ineffective in humans. Researchers do not know whether the anti-inflammatory drug would interfere with Naglazyme in children who depend on it to stay alive. Testing the drug in children with MPS VI would require an adequate number of patients to convince regulators that the treatment is effective, but only nine children in Canada have Isaac’s disease. To recruit enough patients, a human trial would require international co-operation and approval from a variety of health agencies and ethics boards.

The biggest hurdle, however, would be to convince a pharmaceutical company to make a multimillion-dollar investment in research that may have meagre financial return.

Nevertheless, McFadyen is convinced the drug-approval process can be streamlined if he can just get the pharmaceutical industry on board. He notes that pentosan polysulfate has already been proven safe in humans. Johnson & Johnson holds the patent for the drug under the brand name Elmiron, which was approved decades ago as a treatment for interstitial cystitis (an inflammation of the bladder).

McFadyen has spent the past six months lobbying Johnson & Johnson to fund clinical trials in patients with MPS VI. So far, the company has made no commitments. “They promote themselves as being humanitarian driven,” McFadyen says, “and here they are, sitting on a product that is having dramatic, earth-shattering results in the lab.”

Julian Raiman, a specialist in MPS diseases at the Hospital for Sick Children in Toronto, confirms the findings from the rat studies are promising.

He says the current treatment, Naglazyme (and other forms of enzyme replacement therapy), may decrease the rate of decline in many MPS patients but does not treat the inflammation of the musculoskeletal system associated with MPS disorders. The rat study suggests the anti-inflammatory drug may prove effective for various forms of MPS and other lysosomal storage diseases. The question, Raiman points out, is “can that be mirrored in humans?”

Only clinical trials can tell.

But Durhane Wong-Rieger, president of the Canadian Organization for Rare Disorders, says she doubts Johnson & Johnson “will ever put up money for this trial.”

Later this year, Canada will adopt a regulatory framework to spur new treatments for orphan diseases, she notes. But even so, it would take a multimillion-dollar investment and at least six years to have Elmiron approved for a new indication, she says. Meanwhile, the company’s patent on the drug is running out.

Johnson & Johnson declined an interview request but provided a statement: “A senior staff member in our research-and-development organization has assembled a team to fully evaluate this situation and determine if and how we can be helpful,” it says in part. The statement adds, “Unfortunately, we are not able to help in every situation.”

The company’s annual earnings dropped 27 per cent in 2011 to $9.7-billion, but 2012 saw that number climb to $10.9-billion.

Deb Purcell, whose eight-year-old son Trey has MPS II, says it would “unethical” for Johnson & Johnson not to fund a clinical trial. Purcell, who lives in Vancouver, says she has heard parents in the MPS community considering giving their children Elmiron despite the unknown risks. “There are a lot of desperate families out there.”

McFadyen says he fears that if Johnson & Johnson does not test Elmiron as a potential treatment for MPS, competing drug companies will reformulate the inexpensive oral medication as an injection drug that will hit the market many years from now, at an exorbitant price. It wouldn’t be the first time the pharmaceutical industry has profited from rare diseases, he adds.

“Everyone seems to forget that the lives of kids are hanging in the balance,” he says, “and no dollars can ever bring them back.”

A primer on MPS disorders

MPS VI is an extremely rare genetic disorder that affects an estimated 1,100 people in developed countries worldwide. People born with MPS VI (which stands for mucopolysaccharidosis VI) tend to have stunted growth, irregular facial features, restricted movement and breathing problems. Many require heart-valve surgery.

MPS VI shares similarities with other MPS disorders. MPS patients lack a specific enzyme needed to break down long chains of sugar carbohydrates, which build up in the body’s cells and damage multiple organs. One in 25,000 babies is born with an MPS disease.

The MPS disorders, in turn, are part of a larger group of nearly 50 lysosomal storage disorders. Together, LSDs are estimated to affect about 1 in 7,700 births.

 

ADRIANA BARTON

The Globe and Mail

19 Nov 2012
Sticky Post By Posted in Blog Postings Permalink

War of My Life – A Long Awaited Update

Sticky Post By On 19 November, 2012

Hi Everyone,

Thanks for the patience.  I know there have been many of you wondering what’s been going on with our latest project, #ProjectOneMillion, and if things are progressing.

Since we launched our project, a lot of developments have happened, and things are moving forward (although not at the pace with which we want or expect).  So…I’ve decided to take a minute to give you a rundown about where we’ve been, where we are, and where we’re going!

Initial respose to our #ProjectOneMillion video (http://www.youtube.com/watch?v=iPhisB8_-wM) was incredible.  We quickly raced up the charts on YouTube and had 5000 views.  This was before the push actually began for us to get it trending!  As you know, the drug company that we need to sign on board with us, Johnson and Johnson, the maker of the drug that or children desperately need, was initially hesitant to help us complete the clinical trial for our kids.  After the video launched, I reached out to J and J and began discussions to see how we could obtain their support moving forward.

Well, as things tend to do in the pharmaceutical world, things progressed – but progressed slowly.  J and J agreed to have a teleconference with our Researcher and their medical advisory team.  Our lead physician was also scheduled to be on board.  However, due to numerous scheduling conflicts (and other unmentionable delays!), the teleconference got bumped from September, to early October, to late October, to today.

In the meantime, two other major pharmaceutical companies began a push to develop their own version of the drug that our kids need.  On the surface, this seems like cause for excitement.  However, it’s the farthest thing from exciting.  These companies want to take the current form of the drug and make it into a different form, something that is not in the best interest of our kids.  In addition, because they are creating a “new” treatment, it would have to be approved by the FDA (the drug from J and J is already approved).  As well, this “new” drug would have to go through the development stage, the early clinical trial stage, the late clinical trial stages, etc.  This is a very long process, and it’s time that our kids don’t have.  Finally, because this “new” drug would be considered a treatment for a rare disease, the drug company would gain market exclusivity on the drug for 7-10 years.  This means they can also set whatever price point they want – and this price point would be sure to be ridiculously high (current prices for rare disease treatments rank as some of the most expensive drugs in the world).  Again, this is not in the best interest of our children and will be a barrier to a great many being able to even attain it.  In the end, if one of these two drug companies are successful in creating their own drug, it could be upwards of 6 years before we see it in our children, and it will be incredibly expensive (I gauge these companies could end up making a billion dollars on the backs of our very ill children).

This leads us to today and our teleconference with J and J.  While I cannot share any details, I do want to impress on all of you that are interested, our very real determination to ensure that the drug currently being made and marketed by J and J ends up in our children in very short order, and our very real battle to prevent these other two companies from marketing their own drug.

Why is J and J the best option?  First, it’s already available and already FDA approved for use (and approved for use here in Canada as well).  This availability is paramount to ensure our kids can start their treatment early.  Second – it’s in a form that will allow our children to easly access it’s benefits (i.e – not a needle each and every day).  Third, it’s affordable.  So affordable that drug plans will not even question the cost to them on a yearly basis.

To be clear, we have the team in place to begin a trial immediately.  We have the data (which is incredible), we have the lead physician to run the trial, we have the location and are working on the parameters.  All we need is the ability to cover the cost – 1 million dollars.  My hope is that J and J can come through with help, and you’ve all done so very well in helping us so far.  But we have to get going soon, or one of those 2 drug companies will get their own form of the drug production under way, and our kids will continue to suffer needlessly as they wait for another million dollar treatment to become available to them.

So…there you have it.  I promise, I haven’t been sitting idle since the launch of our Project.  I’ve put off media interviews and my media release, but they are hounding me to chat with them because this is such a big story.  We won’t put them off much longer.  And when I chat with them, I hope I have good news to pass along to them 😉

My hope is that J and J will understand what incredibly good things they can be doing for our childern suffering from rare diseases throughout the world.  My hope is that they will understand the need for their product to go into immediate trial in our kids, and that they will work to block the other two companies trying to make hundreds of millions of dollars off of our kids.

And my hope is that you’ll continue to help us along the way.  There’s work yet to be done, and our kids will need you.

Till I can update again, thanks for your continued support.

With Love,

The Isaac Foundation

03 Oct 2012
Sticky Post By Posted in Advocacy, Media, Newspaper Permalink

Trent Hills Couple Set $1 Million Goal To Find Cure For Disease

Sticky Post By On 3 October, 2012

Son Isaac has extremely rare disease

Northumberland News

TRENT HILLS — Andrew and Ellen McFadyen are prepared to take on big pharma to raise $1 million for a clinical trial of a drug that could prove life-changing for their oldest son.

Isaac, eight, has an extremely rare disease, MPS VI, which requires that he receive treatment for an enzyme deficiency one day a week at Toronto’s SickKids hospital.

The enzyme replacement therapy he began five years ago has slowed down the progress of the disease, which stunts growth, stiffens joints, affects the heart and airways, and shortens lifespan.

There is no cure, but the McFadyens believe one is close at hand. Proving it, however, will take $1 million. Their faith is based on “positive results” from ground-breaking research done in the U.S. that was funded by The Isaac Foundation.

The Meyersburg couple established the foundation in 2005 to raise money for research into innovative treatments and potential cures for MPS VI and other MPS diseases, and to increase public awareness about the disorders.

“One of the projects we’ve been funding for the last three years out of New York City is reversing all of the symptoms of this disease in lab animals; it’s as close to a cure as we’ve ever been,” Mr. McFadyen said. “Now we just need to get it into human clinical trial and ensure the safety is there for our children, which we’re very, very confident it is.”

The drug under study is an oral anti-inflammatory that is already used to treat bladder inflammation and has been approved by Health Canada and the Food and Drug Administration in the U.S.

“We’re incredibly hopeful that this is a turning point in the lives of all kids suffering from MPS,” Mr. McFadyen said. “It’s not a huge trial that needs to be done; probably it would take nine months to have good data.”

To raise the capital required, he conceived Project One Million, which is “very ambitious” but it’s a goal he’s confident can be achieved.

“We’ve set our sights high and we’re going to get it,” he said.

He’s pinning his hopes on getting the American pharmaceutical company that manufactures the anti-inflammatory medication to underwrite the cost of the clinical trial. So far it has refused, but that’s not stopping Mr. McFadyen, whose extensive lobbying persuaded the provincial government several years ago to agree to pay for Isaac’s enzyme replacement therapy, which costs about $400,000 annually for the medication.

In the last two years he was also successful in helping to persuade the Ontario and Saskatchewan governments to extend the same benefit to two other children with MPS VI.

“This product has potential to save thousands and thousands of children’s lives (around the world) and I’m not going to rest until they ensure that product gets effectively used for those kids,” Mr. McFadyen said.

“They know we’re fighting against time,” he said. “I will not sit idly by.”

A teleconference involving researchers at the pharmaceutical company and those Mr. McFadyen has been working with is scheduled for Oct. 11.

“They’ve made no promises, but it’s a start,” he said.

 

SIDEBAR

Cobourg gala to raise money to find a cure

TRENT HILLS – Project One Million is more than about raising a huge amount of capital, “it’s a million conversations, it’s a million people talking about rare diseases,” and making them aware “they can make a difference,” Andrew McFadyen said.One way they can show their support is to attend the third annual Gala for a Cure, which includes dinner, wine tasting, a silent auction, and entertainment by Juno Award-winning musician Ron Sexsmith. The fundraiser will take place Oct. 13 at the Best Western Convention Centre in Cobourg.

Eight-year-old Isaac McFadyen, who has been taking piano lessons for a year, will play a number and present a Lifetime Impact Achievement award to Dr. Lilla Simonaro, whose research has fuelled optimism a cure has been found.

Tickets are $100 per person (a charitable tax receipt will be written for $60). They can be purchased online atwww.theisaacfoundation.com or by phoning 613-328-9136.