Two hemophilia drugs being developed could hold blockbuster potential

 

Novo says blood drugs could hold blockbuster potential

COPENHAGEN | Tue May 1, 2012 3:10pm BST

COPENHAGEN (Reuters) – Two hemophilia drugs being developed by Danish drugmaker Novo Nordisk could hold blockbuster potential though sales of its only hemophilia drug on the market will be flat this year, its chief science officer said.

Novo Nordisk aims for a hemophilia drug candidate, Vatreptacog, to replace at least part of the 8.3 billion crowns ($1.48 billion) in annual sales of its only hemophilia drug now in the market, NovoSeven, as sales of that drug decline.

“Vatreptacog can hopefully take over the market which NovoSeven has today,” Mads Krogsgaard Thomsen told Reuters in an interview on Tuesday.

“NovoSeven is a blockbuster today, so you can say that if Vatreptacog takes over after NovoSeven, that drug should hold blockbuster potential,” he said.

Blockbuster is a term used to describe drugs that reach annual sales above $1 billion within five years of launch.

Another of Novo Nordisk’s drug candidates, N8-GP, a long-lasting hemophilia treatment, would compete directly with products from U.S. pharmaceuticals group Baxter International Inc, which today hold blockbuster status.

“If one is lucky enough to make a long-acting N8-GP drug which is a bit better than the competing drugs, then you could be on the way to a blockbuster market, but that is too early to predict,” Thomsen said.

“But the potential is there if the profile turns out right,” he said. ($1 = 5.6205 Danish crowns)

Click here for original Reuters news release

More new drugs are in the pipeline now than in past decades

By Sarah Aldridge | 02.09.2012  by Hemaware

The marketing terms “new and improved” and “longer lasting” are not limited to the latest brand of chewing gum. They also apply to a long list of therapies now in clinical trials for people with bleeding disorders. Some people have waited years for a new recombinant product; others a lifetime for any factor product to treat their rare condition. For many, their patience is about to pay off.

There are more drugs in the pipeline now than in the past few decades. “The companies’ commitment to continue to work on behalf of patients with bleeding disorders is what’s driving it,” says Val D. Bias, CEO of the National Hemophilia Foundation (NHF). The dilemma facing many patients in the future won’t be a lack of medications, but a plethora of products that act in a variety of ways. (See table “Bleeding Disorders Drugs in Human Clinical Trials.”)

For drugs to be approved and licensed by the US Food and Drug Administration (FDA), they have to go through a series of clinical trials. First they are tested on animals, such as mice; then they are tested on humans. Each phase of a clinical trial helps determine the drug’s safety, efficacy, optimal dosage and side effects. (See sidebar, “Clinical Trial Phases.”) The National Institutes of Health clinical trials registry at clinicaltrials.gov lists more than 250 trials on hemophilia and more than 60 on von Willebrand disease (VWD). (See “Clinical Trials 101.”).)

Tried and True vs. Something New

Prophylactic medications to treat hemophilia have given patients a new degree of freedom. They can self-infuse whenever and wherever it’s convenient.

“In terms of hemophilia A and B, I feel that the products we have right now are really good,” says Marion Koerper, MD, NHF medical advisor. She is also director emerita of the hemophilia treatment center at the University of California, San Francisco, where she practices pediatric hematology and oncology. “The factors do work to stop bleeding or, in the case of prophylaxis, prevent bleeding.”

However, prophylaxis is not perfect. “It’s only efficacious if the patient takes it the prescribed way,” Koerper says. The best time to give factor is in the morning before school or work, often the most hectic time of day. For busy families who delay treatment until bedtime, there are consequences. “That is not optimal because the child’s highest levels are while he’s asleep, rather than when he’s running around with his pals on the playground,” says Koerper.

Further, taking a product two or three times a week means that clotting strength can plummet on the off days. “When we give prophylaxis right now for a hemophilia A patient, we’re resolved to the fact that before their next prophy dose, their level in plasma could be as low as about 1% to 2%,” says Steven W. Pipe, MD, medical director, Pediatric Hemophilia and Coagulation Disorders Program, University of Michigan, Ann Arbor. That puts patients at risk for bleeding, especially if there is trauma. “Clearly, that’s not correction of their hemostasis.”

Products With Staying Power

To remedy that risk, pharmaceutical companies are creating new products that last longer in the bloodstream. The amount of factor VIII (FVIII) or factor FIX (FIX) in the blood is measured by its half-life, the time it takes for the amount of factor to be reduced by half. There are many variables involved, including blood type, but FVIII’s half-life is about 8–12 hours; FIX’s is about 18–24 hours. One option is to increase the interval between prophylactic doses, ideally to once a week for FIX products and twice a week for FVIII products. 

Another option is to retain the current prophylactic regimen, but avoid the precipitous drop in clotting factor as the next dosing time approaches. “We may be able to maintain much higher plasma levels than we’ve been able to previously with the same intervals that we’re currently using,” says Pipe.

One way to prevent factor products from degrading too quickly is to attach them to the chemical compound polyethylene glycol (PEG). This process, called PEGylation, increases the size of the factor protein molecule so that it circulates in the blood longer and is not cleared by the kidneys prematurely.

“Another strategy is to fuse the recombinant factor protein molecule to a partner protein that already has a long half-life,” says Pipe. Two naturally occurring partner proteins being fused to the FVIII or FIX molecule are albumin, which moves small molecules through the bloodstream, and Fc, a protein fragment that facilitates binding and recycling of immunoglobulin G (IgG).

Data from early clinical trials on Biogen Idec’s recombinant FVIII and FIX Fc fusion products, rFVIIIFc and rFIXFc, look promising. The A-LONG study on patients with severe hemophilia A showed a 1.7-fold increase in half-life during phase 1/2a clinical trials. B-LONG studies on patients with severe hemophilia B showed a nearly threefold increase in half-life during phase 1/2 trials. (See “Long Strides,” HemAware Summer 2011, p. 14.)

Adjunctive therapies, or drugs that are added to the primary factor product, are also being tested in clinical trials. Some use molecules that bind to tissue factor pathway inhibitor (TFPI), preventing it from hindering the action of FXa and thrombin, necessary for clot initiation and formation. Baxter’s BAX513 uses fucoidan, a seaweed extract being tested on healthy volunteers without hemophilia.

“If you block the proteins that are slowing down coagulation, you can actually restore normal clotting in hemophilic plasma without replacing the missing clotting factor,” says Pipe. For some patients, the adjunctive therapy may become the primary therapy, reducing the number of infusions needed, he says. A bonus is that some TFPI antagonists could be taken orally, such as the capsule form that delivered fucoidan to trial subjects.

“Compliance with bleeding disorders’ treatment is always an issue,” says Bias. “A drug that works better, faster and that you have to take less often can only improve that.”

Innovations for Inhibitors

An estimated 25% of patients with severe hemophilia A develop antibodies, called inhibitors, to the infused factor. Currently, patients undergo immune tolerance therapy to desensitize their immune systems or take a bypassing agent, such as FVIIa. The main drawbacks of the recombinant FVIIa product are that its half-life is only two hours and it is very expensive.

Inspiration Biopharmaceuticals is developing a recombinant porcine (pig) FVIII product for patients with inhibitors. “You can give a dose and get the measurable level of FVIII. That’s a distinct advantage when there’s a life-threatening­ bleed, like a head bleed (intracranial hemorrhage), or a limb-threatening bleed in someone with a compartment syndrome (increased pressure in a muscle in an enclosed space),” Koerper says. But because 80% of patients developed antibodies to plasma-derived pig factor within five days or after five doses, it is possible that a similar scenario might occur with the recombinant product. Results of the clinical trials will provide more data, but its use will probably be restricted.

The longer-lasting products may have an added benefit for inhibitor patients. “Some forms of PEGylation strategy and possibly even some of the fusion proteins may result in reduced risk for inhibitors,” says Pipe. Another product now being tested, Octapharma’s recombinant human-cl rhFVIII, may reduce the rate of inhibitor development because it uses proteins from human cells, not the typical hamster cells.

Recombinant VWD Product at Last

Recombinant products to treat FVIII and FIX were approved in 1992 and 1998, respectively; not so for von Willebrand factor (VWF). “It has bothered me for almost 20 years that I couldn’t offer a recombinant VWF product to my VWD patients,” says Koerper. That need will be fulfilled once Baxter’s recombinant VWF product goes through FDA approval and licensure. It will be targeted to patients with type 3 VWD, the most severe form, and those unresponsive to DDAVP, a synthetic hormone used to prevent or stop bleeds.

Gene Therapy Revisited

Researchers can now create precision drugs that treat diseases caused by specific genetic mutations. One such drug in phase 2 trials is Ataluren (PTC 124^®), manufactured by PTC Therapeutics Inc. It will be used for the approximately 10%–15% of patients with hemophilia A and B with a nonsense mutation, which halts factor production early. Ataluren introduces a molecule that allows the cell to read through the stop signal, making more clotting factor. It comes in a powder that is mixed in water. “Something that you can swallow is going to be a huge advantage because there are no needles involved,” Koerper says. (See sidebar “The Allure of Ataluren” in “What’s Your Genotype?” HemAware Spring 2010, p. 29.)

Rare Bleeding Disorders on the Radar

Patients with rare factor deficiencies know that being one in a million is hardly a cause for celebration. “People forget that there are other clotting factor deficiencies that, in some cases, have no treatment,” says Bias.

But hope is on the horizon. Companies that fractionate, or separate, plasma are interested in getting as many products out of it as they can, says Pipe. “Developing new markets for new plasma derivatives, such as the new FXIII product Corifact™ (approved by the FDA in March 2011), and RiaSTAP^®, a fibrinogen concentrate to treat FI deficiency (indicated for patients with congenital fibrinogen deficiency including afibrinogenemia and hypofibrinogenemia only), increases the sustainability and viability of the plasma fractionation industry.” Both products are manufactured by CSL Behring. Currently, Novo Nordisk has applied for a license for its recombinant FXIII product. British Plasma Laboratories has a plasma-derived FX product in phase 3 clinical trials.

“NHF is most supportive of new products for rare disorders or categories where products don’t currently exist, like the recombinant VWD product,” Bias says. “It’s important that people have access to a product that’s made for them.”

Time Frame for Trials

For drugs now in clinical trials, that access may take a few years. “From initiation of clinical trials to approval, it’s about a five-year window,” says Pipe. Drugs nearing the finish line—those in phase 3 or moving to FDA licensing—still have between 18 and 30 months, he says.

New Era of Optimism

Patients awaiting better, more effective or first-time products to treat their bleeding disorders have many reasons to be optimistic. “For the first time we’re now going to be offering agents that clearly behave differently. We’re not going to be faced with just a single-breed entity to choose from,” Pipe says.

The idea of having more distinct options may be foreign to some, but should be very welcome. New products with different mechanisms mean that treatments may soon be given in a more targeted, personalized manner. “When you have multiple choices it’s going to take some time for the clinicians and families to figure out what’s best for individual patients,” Pipe says.

When recombinant FVIII and FIX drugs came out two decades ago, Koerper thought they were the “ultimate products.” But with all of these recent innovations, she’s changed her thinking. “Now I realize there is so much more that can be done.”

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Clinical Trial Phases

A drug must go through several stages of testing, called “phases” in clinical trials, before it can seek approval review by the Food and Drug Administration (FDA) for use in the US. Depending on how well things go in each phase, the drug progresses from one phase to the next. However, some drug trials are halted voluntarily or by the FDA at certain stages because of concerns about safety or efficacy, for instance. It can take up to five years or more for a new drug to pass muster and make it to the marketplace.

Phase 1

An experimental drug is given to a small number of people (20–100*) to test its safety, tolerability, pharmacokinetics (absorption, distribution, metabolism and excretion) and pharmacodynamics (biochemistry and physiology). Dose-escalating studies are done during this phase to find the optimal dosage.

Phase 2

The drug is given to a larger number of people (100–300*) to evaluate its effectiveness and safety.

Phase 3

The drug is tested in an even larger group of people (1,000–3,000*) at multiple centers across the country to confirm its effectiveness and safety compared with current treatments. During this phase, side effects are also monitored. The studies are randomized and controlled, meaning some patients receive the drug and others get a placebo. Once this “pivotal phase” is successfully completed, the manufacturer can apply for licensing review by the FDA.

Phase 4

Once a drug is licensed for sale, post-marketing surveillance trials are required by the FDA. These trials provide important information on risks, including less common side effects, benefits and optimal use.

*Note: these figures are for standard clinical trials. For bleeding disorders products, the number of trial subjects is often much smaller.

Information partially adapted from clinicaltrials.gov.

Bleeding Disorders Drugs in Human Clinical Trials*

Bleeding Disorder	Drug Name	Company	Clinical Trial
Hemophilia A	Recombinant FVIII-Fc Fusion	Biogen Idec	Phase 3
	NN7088 Recombinant FVIII, third generation	Novo Nordisk	Phase 3
	Human-cl rhFVIII (recomb FVIII, human cell line)	Octapharma	Phase 3
	OBI-1 Recombinant Porcine FVIII	Inspiration	Phase 2/3
	ARC 19499 PEG-conjugated aptamer	Archemix	Phase 1/2
	BAX499 FVIII, subcutaneous	Baxter	Phase 1
	CSL627 Recombinant FVIII-single chain	CSL Behring	Phase 1
Hemophilia B	BAX326 Recombinant FIX	Baxter	Phase 3
	Recombinant FIX-Fc Fusion	Biogen Idec	Phase 3
	OB1001 Recombinant FIX	Inspiration	Phase 2/3
	NN7999 Glyco-PEGylated Recombinant FIX	Novo Nordisk	Phase 3
	ARC 19499 PEG-conjugated aptamer	Archemix	Phase 1/2
	BAX499 FIX, subcutaneous	Baxter	Phase 1
	CSL654 Recombinant FIX-Albumin Fusion	CSL Behring	Phase 1/2
Hemophilia A & B Nonsense mutation	PTC 124 Ataluren	PTC	Phase 2
Inhibitors	rFVII analog	Novo Nordisk	Phase 3
	CSL689 Recombinant FVII-Albumin Fusion	CSL Behring	Phase 2
	GlycoPEG-rFVIIa	Novo Nordisk	Phase 2
	SQ GlycoPEG-rFVIIa	Novo Nordisk	Phase 1
Von Willebrand Disease	BAX 111, rVWF	Baxter	Phase 3
Rare Factor Deficiencies	Recombinant FXIII	Novo Nordisk	License applied for
	Plasma-derived FX	BPL	Phase 3

*This table provides a sampling of drugs now in clinical trials to treat various bleeding disorders. It is by no means comprehensive. NHF does not endorse or recommend any of the products or manufacturers listed. To check the status of drugs now in clinical trials, visit clinicaltrials.gov.

Search this blog for more information on individual press releases form Baxter, Novo Nordisk, CSL Behring,  OctaPharma, Biogen Idec, and Isporation Biopharmaceuticals.

Mobile App to Improve Bleeding Disorder Diagnosis

Novo Nordisk announced in February 2011 the creation of the first mobile application, available on both the iPhone and online, to aid in the diagnosis of bleeding disorders. Coags Uncomplicated features a Lab Value Analyzer allowing physicians to input test results and receive a list of possible diagnoses to consider, including a description of each bleeding disorder and the possible meanings of test results. The application also provides step-by-step suggestions for suitable lab tests to narrow potential diagnoses.

Coags Uncomplicated was developed in partnership with Craig Kessler, MD, Professor of Medicine and Pathology and Director of the Coagulation Laboratory, Georgetown University Hospital, Lombardi Comprehensive Cancer Center.

Coags Uncomplicated was created to meet a need identified by U.S. market research that some specialists do not diagnose the presence of a bleeding disorder in patients with abnormal clotting activity. The failure to recognize a possible bleeding disorder often leads to an overemphasis on the location of the bleed and too little focus on the cause. These findings were presented at the American Society of Hematology Annual Meeting in Orlando, FL, on December 6, 2010.

“While physicians are increasingly using hand-held devices to access medical information, no such tool has existed to help with the diagnosis of bleeding disorders, especially when getting to the correct diagnosis quickly may be critical,” said Eddie Williams, Vice President, Biopharmaceuticals at Novo Nordisk, Inc. “Novo Nordisk was pleased to collaborate with Dr. Kessler on this innovative approach to addressing an unmet need, further demonstrating our commitment to the bleeding disorder community.”

The Coags Uncomplicated app is available for free download at www.coagsuncomplicated.com. The application tools and additional information can also be accessed online.

Source: PRNewswire, February 4, 2011

Safety of Recombinant Activated Factor VII in Randomized Clinical Trials

Marcel Levi, M.D., Jerrold H. Levy, M.D., Henning Friis Andersen, M.Sc., and David Truloff, D.V.M.

N Engl J Med 2010; 363:1791-1800 November 4, 2010

Background

The use of recombinant activated factor VII (rFVIIa) on an off-label basis to treat life-threatening bleeding has been associated with a perceived increased risk of thromboembolic complications. However, data from placebo-controlled trials are needed to properly assess the thromboembolic risk. To address this issue, we evaluated the rate of thromboembolic events in all published randomized, placebo-controlled trials of rFVIIa used on an off-label basis.

Methods

We analyzed data from 35 randomized clinical trials (26 studies involving patients and 9 studies involving healthy volunteers) to determine the frequency of thromboembolic events. The data were pooled with the use of random-effects models to calculate the odds ratios and 95% confidence intervals.

Results

Among 4468 subjects (4119 patients and 349 healthy volunteers), 498 had thromboembolic events (11.1%). Rates of arterial thromboembolic events among all 4468 subjects were higher among those who received rFVIIa than among those who received placebo (5.5% vs. 3.2%, P=0.003). Rates of venous thromboembolic events were similar among subjects who received rFVIIa and those who received placebo (5.3% vs. 5.7%). Among subjects who received rFVIIa, 2.9% had coronary arterial thromboembolic events, as compared with 1.1% of those who received placebo (P=0.002). Rates of arterial thromboembolic events were higher among subjects who received rFVIIa than among subjects who received placebo, particularly among those who were 65 years of age or older (9.0% vs. 3.8%, P=0.003); the rates were especially high among subjects 75 years of age or older (10.8% vs. 4.1%, P=0.02).

Conclusions

In a large and comprehensive cohort of persons in placebo-controlled trials of rFVIIa, treatment with high doses of rFVIIa on an off-label basis significantly increased the risk of arterial but not venous thromboembolic events, especially among the elderly. (Funded by Novo Nordisk.)

Dr. Levy reports serving on a steering committee for Novo Nordisk, and Drs. Andersen and Truloff report being employees of and having equity interest in Novo Nordisk.

Disclosure forms provided by the authors are available with the full text of this article at NEJM.org.

Source Information

From the Academic Medical Center, University of Amsterdam, Amsterdam (M.L.); the Emory University School of Medicine, Atlanta (J.H.L.); and Novo Nordisk, Bagsværd, Denmark (H.F.A., D.T.).

Address reprint requests to Dr. Levi at the Department of Medicine (F-4), Academic Medical Center, University of Amsterdam, Meibergdreef 9, 1105 AZ Amsterdam, the Netherlands, or at m.m.levi@amc.uva.nl.

____________________________

Off-Label Use of rFVIIa Linked to Arterial Thromboembolic Events

Taken From: internalmedicinenews.com
By: MARY ANN MOON, Internal Medicine News Digital Network
11/03/2010

Patients who received off-label recombinant activated factor VII for bleeding episodes had higher rates of arterial thromboembolic events than did those who received placebo, according to a pooled analysis of data from 35 clinical trials published Nov. 4 in the New England Journal of Medicine.

In particular, the rate of coronary arterial thromboembolic events was nearly three times higher in patients randomly assigned to receive rFVIIa off-label than in those assigned to placebo. The rate of adverse events also increased with advancing patient age and with higher doses of the drug, said Dr. Marcel Levi of the University of Amsterdam and his associates.

rFVIIa, marketed as NovoSeven by Novo Nordisk, is approved for the prevention or treatment of bleeding in patients with hemophilia or factor VII deficiency, but an increasing number of small studies have shown its usefulness for severe bleeding in other clinical conditions, including severe trauma, transplant surgery, intracerebral hemorrhage, and overreaction to anticoagulation therapy.

“Most of the safety data on off-label indications are retrospective and involve subjects [who already have] a relatively high risk of adverse events, including thrombosis, making interpretation of these findings difficult,” Dr. Levi and his colleagues noted.

To better assess the drug’s thromboembolic profile, they pooled the data from 26 randomized, placebo-controlled trials involving 4,119 patients with a variety of clinical conditions and 9 randomized, placebo-controlled trials involving 349 healthy volunteers. A total of 29 of these 35 trials were sponsored by Novo Nordisk.

Most of these patients had spontaneous CNS bleeding (31%), advanced liver disease (28%), or trauma (19%). The mean age was approximately 51 years; some of the studies included children, including one that included infants.

Overall, the rate of thromboembolic events was 10.2% in subjects who received rFVIIa – significantly higher than the 8.7% rate in subjects who received placebo (N. Engl. J. Med. 2010;363:1791-1800).

Further analysis showed that almost all of this difference was caused by an excess of arterial thromboembolic events in those who received active treatment (5.5%), compared with those who received placebo (3.2%). There was no significant difference between the two groups in venous thromboembolic events.

Approximately 54% of the arterial thromboembolic events were coronary in nature. In this large subgroup of subjects, the rate of such events was almost three times higher in patients who received active drug, compared with those who received placebo.

The rate of arterial thromboembolic events increased with advancing patient age. In those older than 65 years the rate was 9% with the active drug, compared with 3.8% with placebo. In those older than 75 years the rate was 10.8% with the active drug and 4.1% with placebo. There also was a significant dose-dependent effect.

“This article should serve as a template for pharmaceutical companies to report all studies involving the use of a given drug, on-label and off-label, so that physicians can fully appreciate the benefit and risks when making therapeutic decisions,” Dr. Louis M. Aledort wrote in an accompanying editorial (N. Engl. J. Med. 2010;363:1853-4).

“The authors appropriately warn readers that these data warrant scrutiny when rFVIIa is used on an off-label basis. The thrombolic sequelae reported here are not inconsequential,” noted Dr. Aledort, professor of medicine, hematology, and medical oncology at Mount Sinai School of Medicine, New York.

The thrombotic risks associated with labeled indications for rFVIIa are low. In this study, the risks in healthy volunteers also were low. But for all other study subjects, the risks are substantially higher, even after adjusting for age and different types of bleeding, he wrote.

This pooled analysis was funded by Novo Nordisk, maker of NovoSeven. Dr. Levi’s associates in this study have ties to Norvo Nordisk or are employees and have equity interest in the company. Dr. Aledort reported ties to Baxter, CSL Behring, Grifols, Octapharma, Inspiration, GlaxoSmithKline, and Amgen.

Vitals

Major Finding: The rate of arterial thromboembolic events, particularly coronary arterial thromboembolic events, is approximately three times higher in patients given rFVIIa for off-label indications than in those given placebo.

Data Source: A pooled analysis of 35 randomized, placebo-controlled studies of off-label use of rFVIIa in 4,468 subjects; 29 of these trials were conducted by Novo Nordisk.

Disclosures: This analysis was funded by Novo Nordisk, maker of NovoSeven. Dr. Levi’s associates in this study have ties to Norvo Nordisk or are employees and have equity interest in the company.

FDA Approves 8 mg Vial of NovoSeven® RT

FDA Approves 8 mg Vial of NovoSeven® RT for the Treatment of Hemophilia A or B with Inhibitors and Enhanced Shelf Life for All Vial Sizes

 New 8 mg vial will save reconstitution time and when treating a bleed, every second counts

PRINCETON, N.J., Aug. 10 /PRNewswire-FirstCall/ — Novo Nordisk announced today that the U.S. Food and Drug Administration (FDA) has approved NovoSeven® RT (Coagulation Factor VIIa [Recombinant] Room Temperature Stable) in an 8 mg vial size, making the hemophilia A or B with inhibitors treatment available in 1, 2, 5 and 8 mg vials. The 8 mg vial allows a rapid initiation and administration of this medication for those patients who need a larger dose. In addition, FDA has also approved the extension of shelf life for all vial sizes from 24 months to 36 months at room temperature (at or below 77 degrees Fahrenheit).

NovoSeven® RT is specially formulated to treat people with hemophilia A or B with inhibitors. Hemophilia, which is typically diagnosed in childhood, is a chronic, inherited bleeding disorder that occurs when certain blood clotting factors are missing or do not work properly, resulting in easy bruising and prolonged bleeding from trauma. Spontaneous internal bleeding can occur as well, particularly in the joints and muscles. Inhibitors, a serious complication that can occur after treatment, develop in as many as 30 percent of those with hemophilia. In these cases, antibodies form that neutralize or attack the blood coagulation agents contained in the treatment, resulting in joint disease and making it more difficult to manage bleeds.

“When I get a bleed, I want to infuse my treatment right away. The faster I treat a bleed, the sooner I can continue with my daily routine,” said Bob Hoyt, a member of the Novo Nordisk Changing Possibilities Coalition. “Using fewer vials will be a positive change for patients.” Hoyt has been living with hemophilia with inhibitors most of his life.

For many people living with hemophilia with inhibitors, the 8 mg vial will allow for faster reconstitution – the time it takes to prepare the injection – than their current NovoSeven® RT regimen. Those who previously had to use three vials to deliver an 8 mg dose will now have to reconstitute only one vial. Though the amount of powder in the 8 mg vial is larger than the 5 mg vial, the vial will be the same size and will have a yellow cap to distinguish it from the smaller dose.

“We have heard from patients and physicians alike that when they are treating a bleed, every second counts. We at Novo Nordisk are committed to improving the lives of people living with hemophilia with inhibitors,” said Eddie Williams, Vice President, Biopharmaceuticals, at Novo Nordisk. “The NovoSeven® RT 8 mg vial will allow patients to get the medicine they need much faster when experiencing a bleed, without having to manage multiple vials. We’re also pleased that it will have a positive environmental impact as well – fewer vials may mean less waste.”

The new vial size is expected to be available by November.

The enhanced stability of all vial sizes will allow for more flexibility when managing treatment supplies – another important aspect of hemophilia treatment.

About NovoSeven® RT

Indications and Usage

NovoSeven® RT (Coagulation Factor VIIa [Recombinant] Room Temperature Stable) is indicated for the treatment of bleeding episodes in hemophilia A or B patients with inhibitors to FVIII or FIX and in patients with acquired hemophilia; prevention of bleeding in surgical interventions or invasive procedures in hemophilia A or B patients with inhibitors to FVIII or FIX and in patients with acquired hemophilia; treatment of bleeding episodes in patients with congenital Factor VII deficiency and prevention of bleeding in surgical interventions or invasive procedures in patients with congenital FVII deficiency.

Important Safety Information

Warning: Serious thrombotic side effects are associated with the use of NovoSeven® RT outside of uses approved by the FDA. These thrombotic side effects are blood clots that form in arteries and veins and can cause harm and may lead to death. Your doctor should discuss the risks and explain the signs and symptoms of thrombotic side effects to you. Your doctor should monitor you for blood clots during treatment with NovoSeven® RT.

Thrombotic side effects following the use of NovoSeven® RT occurred in 0.28% of all bleeds that were treated for FDA-approved uses. The rate of 0.20% was observed in hemophilia patients with inhibitors, and the rate was higher in patients with acquired hemophilia (4%). Thrombotic events (fatal and non-fatal) have been reported following use of NovoSeven® RT for all FDA-approved uses.

Some patients have conditions that may increase the risk of thrombotic events. These include clogged arteries, blood clots that form throughout the body instead of at the place of injury (called disseminated intravascular coagulation), a type of blood poisoning called septicemia, and crush injury, which is when a body part is crushed or squeezed between heavy or immobile objects. Also, people taking aPCCs/PCCs (activated or nonactivated prothrombin complex concentrates) at the same time they are taking NovoSeven® RT may be at increased risk for thrombotic side effects. NovoSeven® RT should be used with caution in patients who have an increased risk for thrombotic side effects. These include, but are not limited to, patients with a history of heart disease, liver disease, patients who have limited movement following surgery, elderly patients, and neonates (babies who are 4 weeks old or younger). In each of these situations, the potential benefit of treatment with NovoSeven® RT should be weighed against the risk of these complications.

Some patients with Factor VII deficiency have developed resistance (antibodies) to Factor VII after treatment with NovoSeven® RT. Factor VII-deficient patients should be monitored for antibody formation before and after administration of NovoSeven® RT.

People who have ever had a bad reaction to NovoSeven® RT or to proteins from mice, hamsters, or “bovines” (such as an ox or cow) should consult their physician prior to using NovoSeven® RT.

The most common side effects during clinical trials in people taking NovoSeven® RT were fever, bleeding, injection site reaction, joint pain, headache, high or low blood pressure, nausea, vomiting, pain, swelling, and rash.

Please visit www.novosevenrt.com for Prescribing Information.

You are encouraged to report negative side effects of prescription drugs to the FDA. Visit www.fda.gov/medwatch, or call 1-800-FDA-1088

NovoSeven® RT is a prescription medicine.

NovoSeven® is a registered trademark of Novo Nordisk Health Care AG.

About Novo Nordisk

Novo Nordisk is a global healthcare company with more than 87 years of innovation and leadership in diabetes care. The company also has leading positions within hemophilia care, growth hormone therapy and hormone therapy for women. Novo Nordisk’s business is driven by the Triple Bottom Line: a commitment to social responsibility to employees and customers, environmental soundness and economic success. Headquartered in Denmark, Novo Nordisk employs more than 29,650 employees in 76 countries, and markets its products in 179 countries. Novo Nordisk’s B shares are listed on the stock exchange in Copenhagen and its ADRs are listed on the New York Stock Exchange (NVO). For more information, visit novonordisk-us.com.

SOURCE Novo Nordisk

RELATED LINKS
http://www.novosevenrt.com