Search This Blog

Friday, January 4, 2019

MedImmune chief leaving AstraZeneca and joining the trek into biotech



Six years after AstraZeneca’s then new CEO Pascal Soriot named Bahija Jallal president of the big MedImmune subsidiary in Gaithersburg, MD, putting her at the center of the company’s R&D turnaround plans, the longtime pharma exec is joining the great migration of industry professionals to biotech.

Jallal is taking the helm at Immunocore next week, a prominent TCR player in the UK which has been going through a remarkable shakeup after the original team under CEO Eliot Forster — now chief at F-star — either left or were forced out. Immunocore was able to raise $320 million a little more than 3 years ago — a time when that kind of money was still able to cause astonishment in the industry.
This wasn’t the first such biotech job to come along, Jallal tells me in an exclusive interview ahead of the announcement. “But when the right one is there you jump on it.”
The job starts on Monday, and Jallal says she feels like “a kid in a candy store” when it comes to Immunocore, a company with a broad platform that is built to accommodate oncology as well as infectious diseases and autoimmune conditions.
And Jallal isn’t the only senior AstraZeneca exec heading to new biotech fields. The Wall Street Journal reports today that Mark Mallon — current EVP in charge of portfolio strategy — is on his way to take the CEO job at Ironwood, as that company splits up under pressure and Peter Hecht leaves to run the R&D spinout.

Over the past year-plus Immunocore has run into some severe turbulence after it tried to shop a new round at its old unicorn valuation. Potential investors weren’t ready to buy in, triggering an exodus at the top and a move up for chief commercial officer Andrew Hotchkiss as interim chief.
Jallal says Hotchkiss has done a great job this year, which includes inking a major new pact with Genentech, and he’ll go back to concentrating on his commercial focus with an eye on advancing Immunocore’s late-stage cancer therapy toward the market.
“I can tell you there’s been a lot of progress in the past year,” she adds. “Next week we’re going to JPMorgan and share the story with the investor community and others. My intention is to bring reassurance to investors that I will bring stability to the organization, bring the best team and have the vision we can all work together and show them why I am joining the company.”
Jallal was one of three top R&D execs Soriot picked for the Big Pharma’s turnaround in 2013. Briggs Morrison left several years ago to run Syndax. That leaves Mene Pangalos and his new colleagues to run the show at AstraZeneca’s research and development operations.
There’s no immediate word on who will replace Jallal at Medimmune, where she steered 5 drugs to an approval, including their checkpoint player Imfinzi.
Posted by at No comments:

Stocks to watch into JPMorgan’s upcoming healthcare conference


Noting that biotech has generally outperformed the broader relative market during its Healthcare Conference in previous years, JPMorgan highlighted “can’t miss” presentations expected from 10 companies, including Gilead Sciences (GILD), Sarepta Therapeutics (SRPT), Sage Therapeutics (SAGE) and Celgene (CELG). To note, the firm’s comments on the biotech presentations that should not be missed by investors were released before Bristol-Myers (BMY) and Celgene announced this morning that they have entered into a definitive merger agreement under which the former will acquire the latter in a cash and stock transaction with an equity value of about $74B.
2019 HEALTHCARE CONFERENCE: Biotech has generally outperformed the broader relative market during the JPMorgan Healthcare Conference, driven by a myriad of factors that included clinical, regulatory and strategy updates from the companies themselves and read-through from other events/companies in the same space, JPMorgan analysts said in a note to investors previewing the upcoming event. The firm believes that many will be looking to the 2019 conference as a sentiment check for the year ahead and the potential to reset expectations after “a rocky Q4.” From the about 100 companies in the JPMorgan Biotechnology coverage universe, the firm highlighted the potential Top 10 “can’t miss” presentations, which included Gilead Sciences, Celgene, Regeneron Pharmaceuticals (REGN), Sarepta Therapeutics, Jazz Pharmaceuticals (JAZZ), Sage Therapeutics, Ascendis Pharma (ASND), Ironwood Pharmaceuticals (IRWD), Solid Biosciences (SLDB) and Novavax (NVAX).
TOP 10 ‘CAN’T MISS’ PRESENTATIONS: JPMorgan believes Gilead’s presentation this year could be notable in that it is a fireside chat only with multiple members of management going into an important year with a new CEO poised to take the helm, multiple near-term Phase 3 readouts, and multiple ongoing launches. Regarding Regeneron, the firm believes investors could get some initial launch metrics for dupilumab in asthma and more commentary around the strategy in immuno-oncology, among other things. Looking at Sarepta, JPMorgan pointed out that the company could potentially provide initial Limb-Girdle data, a micro-dystrophin DMD regulatory update, and competitive micro-dystrophin data. JPMorgan is also looking forward Jazz Pharmaceuticals’ latest Vyxeos comments, insights into 2019 Xyrem volume growth, and more color on the recent Solriamfetol delay as well as the aggressive share repurchases it believes were made in the fourth quarter. Meanwhile, Sage has announced that they will be disclosing top-line data from the highly anticipated Phase 3 trial of SAGE-217 in PPD in January, and JPMorgan suspects this could occur before or during the conference. The firm also expects Ascendis to disclose a new therapeutic vertical, with rationale and the unmet medical need/commercial opportunity, and Ironwood to pre-announce Linzess sales and outlook for out-year/peak sales. During the conference, the firm also expects possible initial expression data for Solid Biosciences’ SGT-001 micro-dystrophin program, and Novavax’s NanoFlu Phase 2 immunogenicity data in older adults.
Posted by at No comments:

How Should Doctors Determine Brain Death?


The American Academy of Neurology (AAN) called for uniform brain death laws, policies, and practices in a new position statement.
The position paper, published in Neurology, defines brain death — otherwise known as death by neurologic criteria — as the individual’s death due to irreversible loss of function of the entire brain in accordance with the Uniform Determination of Death Act (UDDA), a model state law that was approved for the U.S. in 1981.
The statement has three goals, lead author James Russell, DO, MS, of Lahey Hospital and Medical Center in Burlington, Massachusetts, told MedPage Today.
“First, it provides AAN, American Neurological Association, and Child Neurology Society endorsement of the [UDDA’s] conclusion, which identified brain death as equivalent to cardiorespiratory death,” he said.
Second, it provides endorsement from all three organizations that the 2010 guidelines for adults and 2011 guidelines for children are “the currently and widely recognized medical standards for brain death determination,” Russell added.
And third, it offers guidance about how to “reconcile requests to abstain from brain death testing or to continue organ-sustaining technology after a diagnosis of brain death has been rendered,” he said.
To the AAN’s knowledge, no cases have occurred in which the adult or pediatric guidelines led to inaccurate determination of death with return of any brain function, including consciousness, brainstem reflexes, or breathing. But so far, only Nevada has adopted legislation that requires using the guidelines as the medical standard for determining brain death.
Every state has accepted the UDDA definition of brain death as legal death, but in most states, medical standards for determining brain death are unspecified. This lack of specificity, coupled with inconsistencies within institutions, has led to differing interpretations in high-profile legal cases.
“The AAN statement was prompted by several recent medicolegal cases that highlighted controversies in brain death and questioned whether it should be considered an accepted and valid medical standard,” said James Bernat, MD, of the Geisel School of Medicine at Dartmouth College in Hanover, New Hampshire, who helped develop the conceptual foundation of brain death that formed the basis of the UDDA.
The AAN’s position provides an “authoritative consensus declaration on the practice of brain death determination,” Bernat told MedPage Today. “It clarifies that, despite legitimate areas of controversy, physicians conducting a brain death determination can feel secure that it represents the medical standard of care.”
The problem is not just uncertainty about what constitutes brain death, noted Arthur Caplan, PhD, director of medical ethics at NYU Langone Hospital in New York City, who was not involved with the AAN paper.
“It’s uncertainties about what power family members have to compel the continuation of treatment, even in the face of death,” Caplan told MedPage Today. “We see a swinging of the pendulum toward patient autonomy. Some doctors have become nervous and think they have to listen to patients, even when they’re asking for things that are impossible, or outside the standard of care, or simply wrong.”
“This paper affirms that parental and family rights have limits, and family members shouldn’t be allowed to coerce treatments, while recognizing they do need accommodation in terms of explanations or meetings with ethics committees,” Caplan continued. “But death is not a state that requires continuation of treatment, and this paper says that pretty clearly.”
The AAN position statement provides guidance for clinicians when families do not accept a determination of death and request continued life support. It also supports legislation modeled after the Nevada statute in every state, uniform policies in medical facilities that comply with brain death guidelines, and programs to credential physicians to determine death by neurological criteria.
The Brain Death Summit, subsequent meetings, and conference calls of the Brain Death Working Group have been financially supported by the American Academy of Neurology.
Authors report no disclosures relevant to the manuscript.
Posted by at No comments:

Prospects Cloudy for Part B Drug Payments


The issue of skyrocketing drug prices has placed Big Pharma squarely in the crosshairs of Congress and the president for the last few years, making Martin Shkreliand Mylan household names (and not in a good way).
In 2018, the Trump administration took multiple steps to address the matter, beginning with the announcement of a blueprint for lowering drug pricing, “American Patients First.” One of President Trump’s aims was to “end global freeloading” — the often dramatically higher prices for drugs sold in the U.S. versus other markets. And one particular target has been Medicare Part B drugs — those administered by physicians and typically among the most expensive therapies.
Click here to read MedPage Today‘s story from Oct. 25, 2018, about a proposed overhaul. In the follow-up story below, we explore the Trump administration’s broader efforts to address drug pricing, including experts’ opinions regarding how such changes might affect the pharmaceutical market and patients.
An End to ‘Global Freeloading’
In October, President Trump announced a plan to adopt a new “International Pricing Index” model, which specifically hones in on drugs paid for through the Medicare Part B drug program. The plan would replace the “average sales price” (ASP) that determines what Medicare and beneficiaries pay for Part B drugs with a payment scheme based partly on prices charged in other countries (which in most cases are lower than in the U.S.) through a mechanism known as “reference pricing.”
Broadly speaking, reference pricing involves establishing a maximum amount that a payer will reimburse for a product based on a certain benchmark. In this case, the payer is the government and the target price would be tied to an international price index, based, in part, on prices paid in other economically similar countries.
Over the course of 5 years, the share of the drug’s price tied to the international price versus the ASP would grow, until overall prices for Part B drugs would drop, the administration projected, by 30%.
More specifically, in the first year of the model, the Part B payment would be 80% based on the current ASP and 20% based on the international pricing index, with the share of ASP in the index progressively declining each year. After 5 years, Medicare Part B payments would be targeted at about 126% of the average international price, explained Health and Human Services Secretary Alex Azar during a briefing with reporters in late October.
While many specifics were absent from the plan, an October HHS press release estimated that the index would save taxpayers and patients $17.2 billion over 5 years.
The new model also aims to pilot significant changes to payment mechanisms for distributors and providers.
Instead of a “buy and bill” operation, where doctors’ offices contract with wholesalers and group purchasing organizations that buy drugs from manufacturers and then resell them to providers, physicians would have the option to use private vendors who “retain ownership”and distribute the drugs to hospitals and doctors offices. These third-party vendors would also be responsible for billing Medicare themselves.
According to the proposal, the program would be piloted in half the country — although the specific geographic regions remain unnamed — in the first year and involve only biologics and drugs made by a single manufacturer. Over the ensuing 5-year period, Medicare would phase in additional products to ultimately include 90% of all Part B drugs, said Azar.
Experts Weigh In
“A lot of people have looked at the fact that drugs are cheaper in almost every country in the world than they are in the U.S.,” said Jack Hoadley, PhD, research professor emeritus at the Georgetown University Health Policy Institute here.
But if drug prices in the U.S. are somehow “magically” linked to prices paid in Europe, causing prices to fall in the U.S., “manufacturers are not going to sit there and say, ‘That’s fine. We’ll just see a drop in our revenue… They’re going to find a way to make that up,” which could mean raising prices in those other countries, he said.
Curiously, raising prices abroad would impact prices in the U.S. if U.S. prices are tied to those of other developed nations, he noted.
Until the administration clearly defines what it means by “reference pricing,” and until modeling is done on what manufacturers’ behavioral response could be, the impact of the new proposal is hard to measure, Hoadley said.
“I think the international reference pricing [proposal] makes complete sense, because we’re just not able to negotiate effectively,” said Gerard Anderson, PhD, of Johns Hopkins Bloomberg School of Public Health in Baltimore.
And the fact that a Republican administration introduced such a radical proposal reflects a “watershed moment,” as the ideas in it are “antithetical” to many conservatives, he added.
But the administration could go further in its changes to Part B, Anderson said. It could eliminate the incentive for doctors to choose the most expensive treatments. Under the current payment system, physicians are paid the ASP plus a percentage add-on fee. The higher the cost of the drug, the higher the add-on fee, and the stronger the incentive to choose the higher-cost drug, Anderson explained.
Doctors are used to earning substantial profits on dispensing these drugs, as much as “several hundred thousand dollars” he said, and while the Trump administration’s proposal reduces the amount physicians would receive for administering Part B drugs, it doesn’t entirely do away with that incentive, he said.
Anderson also questioned the idea of involving a third-party vendor, between the doctors and the government, adding “another level of bureaucracy and burden” and creating unnecessary administrative costs, he said.
Will it Happen?
Prospects for the International Pricing Index are uncertain, noted several of the experts MedPage Today interviewed.
Stacie Dusetzina, PhD, associate professor of health policy at Vanderbilt University School of Medicine in Nashville, said the proposal isn’t “realistic.”
“In essence, this plan relies on other countries to do our negotiating for us. To be able to index our price to other countries, we would need to know what prices they pay, which can be difficult to obtain now and will likely be harder to get in the future if pharmaceutical companies know these prices will be used against them in negotiations,” Dusetzina wrote in an email to MedPage Today.
Regarding the changes to how physicians are paid for administering Part B drugs, Dusetzina noted that it “seems obvious” that the percentage-based payment (and the perverse incentives that come with it) “is not the best way to pay physicians for their services.”
But the Obama administration encountered “fierce resistance” from professional organizations when it attempted to change how physicians are paid for Part B drugs.
“I imagine the [Trump] administration would face similar hurdles,” she said.
The idea of involving a third-party vendor as a substitute for physicians buying and billing Part B drugs seems dubious, Dusetzina suggested.
“The vendor that they describe… sounds a lot like a [pharmacy benefit manager], which makes it unclear how much they will help reduce spending (versus adding additional administrative costs to the system),” Dusetzina wrote.
While the concepts of the plan are “admirable” she wrote, the administration faces an “uphill battle” in implementing them.
Also, “[w]e should do more to negotiate for drug prices in the U.S., not merely piggyback on other countries’ efforts. We should also make sure that physicians are paid the same for delivering both high- and low-priced drugs,” Dusetzina concluded.
Other policy experts shared similar doubts about the proposal’s chances for success.
“It’s going to be a herculean task to get it through Congress,” Marsha Simon, PhD, president of Simon & Co., a healthcare consulting firm here, told MedPage Today.
She pointed to the recently tabled IMPROVE Act, a bill focused on coordinating care for children in the Medicaid program, which Simon said she believes failed to pass because of the unpopularity of the “pay-fors.” In this case, the bill would have been funded through penalties on drug companies that misclassified their drugs as generic instead of brand drugs in the Medicaid Drug Rebate Program.
When a drug is classified as a brand, manufacturers pay higher rebates than if the same drug is classified as a generic product, she explained. In the past, drugmakers have gotten away with categorizing their drugs as generics or “misbranding” them. Famously, Mylan, the maker of the EpiPen epinephrine auto-injector is accused of misbranding them as generic products and overcharging the Medicaid program more than $1 billion, Simon said.
The IMPROVE Act, elements of which had been pending for far longer under the ACE KIDS Act, which was part of IMPROVE, passed in the House but stalled in the Senate — because of drug company influence, Simon suggested.
In other words, if Big Pharma doesn’t like a proposal it won’t get passed in congress, and the international reference pricing proposal is no exception, Simon argued.
That said, the Center for Medicare and Medicaid Innovation (CMMI) has the authority to pilot the proposed model on its own and if it’s successful, make compliance mandatory without passing any legislation.
According to CMMI criteria, the model has to improve the healthcare program and not reduce access to be considered successful, Simon said.
And if it were implemented, Simon said she feels strongly that the index should also be applied to the initial price of drugs in Medicaid, in the 340B Drug program and in the Department of Veterans Affairs.
“It would have an enormous impact on our public programs,” she said.
Hoadley, who was also skeptical about the feasibility of an overhaul of Part B drugs, said it was difficult to say whether or not the plan would be implemented.
“The good news is that a lot of the options that are being talked about are not currently dividing people along ideological or partisan lines,” he said, and at a minimum, there is consensus on making changes to the Part B program.
On the other hand, there have been signs already of “hard pushback” from stakeholders, he said.
When the Obama administration put forward its own Part B proposal was “shut down”after oncologists, physician organizations, and certain disease groups argued that the changes would make drugs unaffordable and restrict access. (In December 2016, the administration announced it would halt the demonstration project.)
That proposal had two phases, Hoadley said. The first phase, which focused on shifting from paying physicians ASP plus 6% to a reduced add-on payment of 2.5% as well as a flat fee of $16.80, was the part that created all “the noise” from stakeholders.
However, the second phase of the Obama administration’s plan, related to value-based pricing — paying more for improved patient outcomes — while not entirely fleshed out, has re-emerged under the Trump administration, Hoadley noted. This suggests there may be a chance for a “longer conversation” about value-based pricing.
“Past precedent gives you reason to be skeptical about bipartisan compromise, particularly on some of the more out-of-the-box solutions, but it’s a new day in 2019,” Hoadley said, and it’s always possible that partnerships can be forged across the aisle.
Posted by at No comments:

Ablative Solutions bags $77M to complete hypertension device trials


Ablative Solutions raised $77 million from the likes of Gilde Healthcare and BioStar Ventures to bankroll clinical trials of its minimally invasive treatment for uncontrolled hypertension.
Specifically, the new capital will support clinical trials for Ablative’s alcohol-mediated renal denervation technology in support of regulatory filings in the U.S. and Europe, the company said in a statement. The procedure is performed using the company’s Peregrine system and is intended to reduce blood pressure in people with hypertension for whom antihypertensive drugs do not work.
The Peregrine System Kit targets sympathetic nerves that run to and from the kidneys along renal arteries and play a key role in the regulation of blood pressure. The system delivers small doses of dehydrated alcohol to the space outside the renal artery to block overactive signaling of the sympathetic nerves. It does so via the Peregrine System Infusion Catheter, which has FDA clearance to infuse diagnostic and therapeutic agents to the perivascular space that surrounds blood vessels. The system is being studied both in patients taking antihypertensive medication and in those who are not.
Michigan Accelerator Fund, Novus Biotechnology and other individual investors joined Gilde and BioStar in the series D round.
“Hypertension creates a significant burden on the healthcare system, increasing the risk of serious cardiovascular events and stroke,” said Geoff Pardo of Gilde Healthcare in the statement. “We see tremendous potential for Ablative Solutions’ approach and believe the team has a solid plan for building the clinical data through the TARGET BP clinical program.”
Ablative Solutions isn’t the only player using renal denervation to attack high blood pressure. Last July, Otsuka announced it would acquire ReCor Medical and its ultrasound ablation system. ReCor’s device is designed to treat hypertension the same way Ablative’s does—by downregulating the activity of the sympathetic nerves.
Posted by at No comments:

Verily pockets $1B with eyes on partnerships, M&A


Six weeks after canning its Novartis-partnered glucose-sensing contact lens project, Verily is raising a $1 billion round that will power new partnerships, “global business development opportunities” and potential acquisitions.
Silver Lake led the mammoth round and was joined in the investment by Ontario Teachers’ Pension Plan and “other global investment management firms.” The company did not disclose financial terms of the transaction.
“We are taking external funding to increase flexibility and optionality as we expand on our core strategic focus areas,” said Verily CEO Andrew Conrad in a statement. “Adding a well-rounded group of seasoned investors, led by Silver Lake, will further prepare us to execute as healthcare continues the shift towards evidence generation and value-based reimbursement models.”

The financing comes after a year during which Verily inked multiple partnerships. In May, the company joined forces with Gilead Sciences to analyze the effect the latter’s drugs have on the immune cells of patients with inflammatory diseases. In June, Sanofi, Sensile Medical and Verily teamed up to develop an “all-in-one” insulin patch pump, primarily aimed at patients with Type 2 diabetes—nearly two years after Verily and Sanofi created Onduo, their diabetes-focused joint venture. In July, Verily set up a joint venture with ResMed to apply big data analytics to sleep apnea by developing connected software to assist healthcare providers in identifying and managing patients.

Further, despite halting its smart contact lens project—the device was ultimately unable to consistently measure glucose levels in tears that correlated with blood glucose readings—Verily’s partnership with Novartis continues. The pair is working on a responsive, accommodating contact lens for presbyopia—age-related farsightedness—and a smart intraocular lens for improving sight following cataract surgery.
Posted by at No comments:

Vaccine for Type 1 diabetes? Provention Bio says a human trial is in sight


Type 1 diabetes, in which the immune system attacks insulin-producing beta cells of the pancreas, is caused by both genetic susceptibility and environmental factors, researchers believe. Biotech startup Provention Bio is trying to reduce the environmental risk by way of a vaccine scientists believe can prevent up to 50% of new Type 1 diabetes cases.
Previous epidemiological studies and experiments on animals and human tissues have suggested a possible link between enterovirus (EV) infections and Type 1 diabetes, according to a summary co-authored by Provention’s co-founder and chief scientific officer, Francisco Leon, M.D., Ph.D., which appeared recently in the journal Expert Review of Vaccines. EVs are known to infect the pancreas and cause a diabetes-like disease in animals. Additionally, scientists have prevented diabetes in mice with attenuated virus vaccines or recombinant VP1 viral proteins.
Based on those findings and with proceeds from an initial public offering, Provention is now advancing a multivalent group B coxsackieviruses (CVBs) vaccine candidate dubbed PRV-101 into the clinic for Type 1 diabetes, it announced.

Researcher Heikki Hyöty of the University of Tampere in Finland, who co-authored the current review, had previously found that people with markers of EV infections had an increased risk of Type 1 diabetes. He published that evidence in a 2017 paper in the journal Diabetologia.
In that study, Finnish scientists examined 1,673 longitudinal stool samples from 129 children who turned positive for autoantibodies against pancreatic islets—which is known as a pre-symptom phase of Type 1 diabetes—and compared them with 3,108 samples from 282 matched control children. The researchers observed an increased frequency of EV RNA in the children long before the emergence of autoimmunity.
What’s more, Hyöty and colleagues found that CVB1 antibodies in the mothers of the study subjects were associated with about 50% lower rate of autoimmunity in the children.
“This important observation suggests that a vaccine against CVB could prevent a substantial subset of T1D cases,” wrote the authors in the current study.
Still, there isn’t enough evidence to prove the observed CVB-diabetes link is indeed causal. That key question will likely only be answered by a clinical trial. That’s where Provention Bio comes in.
The company has developed PRV-101, a multivalent CVB vaccine made with the same formalin-inactivated whole-virus vaccine technology used in a polio inoculation. In a preclinical proof-of-concept study done by a team at the University of Tampere, a prototype of the vaccine successfully protected against virus-induced diabetes in a mouse model of Type 1 diabetes, the team reported in a Diabetologia paper.
Provention is on track to start human trials of PRV-101 soon, and its executives hope it will be the first vaccine to prevent up to 50% of Type 1 diabetes cases. “In addition to the potential prevention of T1D, this vaccine could have other important beneficial health effects generated by protection against acute CVB infections, which are frequent and cause significant morbidity particularly in young children,” Leon said in the announcement.
Posted by at No comments:
Subscribe to: Posts (Atom)