The TPP’s IP Chapter Imposes Longer, Broader, and Stronger Patent Monopolies on Medicines
The TPP’s IP Chapter contains final provisions that (1) weaken standards of patentability, leading to more patents; (2) extend patent terms to compensate for delays in granting patents or registering marketing approval; (3) adopt new exclusive rights relating to undisclosed registration-related/clinical-trial data; (4) prevent or interfere with the registration of generics where patents are claimed; and (5) enhance patent infringement remedies.
In general, weak standards of patentability, the criteria upon which patents are granted, make it easier to get initial patents—the first 20 years of exclusive rights; weak standards also encourage seeking multiple secondary patents that further extend the period of exclusivity. Using weak patent standards, drug companies can obtain “secondary,” 20-year patents on minor variations of an active ingredient, new formulations and dosages, new uses or methods of use (indications), and new processes of synthesis and manufacture. In the pharmaceutical industry, pursuit of secondary patents is positively framed as patent life-cycle management; in the access-to-medicines world it is criticized as manipulative evergreening [
10].
The TPP imposes weakened standard of patentability in two ways. First, it defines “obviousness,” the real meat of the inventiveness inquiry, to eliminate countries’ right to require that an invention have a significant technological advantage as assessed by persons “highly” skilled in the relevant arts. Second, the TPP mandates that countries allow patents on new uses or methods or process of use of known medicines, even though research and development costs are significantly lower for a medicine already known to be safe and even though the search for new indications is more a function of routine, plodding investigation than “inventive-step” science [
11]. The consequences of weak standards of patentability can be quite significant. For example, there are over 800 different families of patents on the antiretroviral booster, ritonavir [
12], and its period of exclusivity had been extended for decades [
13]. Such extended periods of exclusivity can have significant cost implications [
14].
The TPP lengthens pharmaceutical monopolies in other ways. For example, if there is an unreasonable delay in the granting of a patent (within five years of the filing of a patent application or within three years after a request for patent examination) then the patent term must be adjusted to compensate for the delay. In addition, the TPP requires patent terms adjustments to compensate for delays in the marketing approval process. A study from the US on the impact of patent term extensions found that they add an average of 3.6 years to the period of exclusivity and might account for nearly 20% of pharmaceutical sales in the US [
15].
The TPP creates additional forms of monopoly protection by requiring countries to adopt data/marketing exclusivity restrictions like those applied in the US [
16]. Accordingly, when a pharmaceutical product involving a new chemical entity receives marketing approval, the relevant drug regulatory authority and generic applicants cannot refer to or rely on the undisclosed regulatory data submitted by the originator, nor on the fact of the prior registration, to assess the therapeutic equivalence of the follow-on product for a minimum period of five years. This period of exclusivity can be extended by successive three-year periods each time the originator submits additional clinical information for a new use of the medicine. The TPP also imposes US-style patent-registration linkage (blockage of registration by the medicines regulatory authority), or requires notice to patent holders and timely access to judicial or administrative procedures for preventing market approval of a follow-on generic equivalent whenever a product patent is claimed.
An even longer period of data/marketing exclusivity is required for biologics. Although there is no economic evidence justifying longer exclusivity for biologics [
17], the US fought hard for twelve years of exclusivity. The parties settled on eight years of data exclusivity for biologics or five years followed by three years of equivalent market protection. Because biologics are a growing proportion of the market and are often significantly more expensive than small-molecule medicines, expanding exclusivity can have significant cost implications. There are several studies showing that data exclusivity raises prices and negatively impacts access to medicines [
18].
The Enforcement Section of the IP Chapter strengthens private enforcement of IP rights and imposes greater enforcement obligations on governments. It contains provisions requiring deterrent remedies, compelling the use of the rightholder’s retail price as a measure of damages, mandating injunctive relief, and banning reasonable royalties as an infringement remedy. Several of these proposals exceed US law [
19]. TPP governments will also be required to adopt border control measures like those that interrupted lawful passage of generic medicines through Europe in 2008 and 2009 [
20]. Fear of excess liability, injunctions, and border seizures can deter generics from marketing competing equivalents when there is even a slight risk of patent infringement enforcement.
The Investment Chapter Grants Additional Enforcement Powers to IP Rightholders
In the Investment Chapter, IP rights are defined as protected investments, and foreign IP investors are permitted to seek private arbitration through ISDS whenever they feel that their investments have been treated unfairly or inequitably, taken without compensation, or discriminated against. TPP member states can expect an avalanche of IP-related claims from disappointed pharmaceutical companies that think their legitimate expectations of future profits have been thwarted by foreign governments’ IP decisions or policies.
The TPP’s Investment Chapter greatly expands the enforcement rights of foreign pharmaceutical companies, creating substantial risks to countries’ ability to set IP-related policy and to render IP decisions. The Investment Chapter unequivocally defines IP rights as “investments.” It prohibits the following: (1) discrimination against foreign IP investors, (2) unfair and inequitable treatment, and (3) indirect expropriation. More pointedly, it allows ISDS claims directly against governments before unreviewable three-person arbitration panels, even when judicial remedies have not been exhausted or when companies have lost on appeal. Foreign investors can bring ISDS claims that domestic investors cannot. Moreover, companies might claim—correctly or not—a lack of fair and equitable treatment that undermines their well-grounded expectations of profit with respect to many health-related regulatory and judicial decisions, including the following: denials or revocations of pharmaceutical patents; granting of compulsory licenses; denials or restrictions on marketing rights; refusals to list excessively priced, IP-protected products for reimbursement; decisions to establish price controls; and required disclosure of clinical trial data. Foreign companies might claim indirect expropriation following changes in regulatory environments, including changes designed to promote public health [
21].
The dangers of ISDS IP enforcement are highlighted in a US$500 million arbitration claim brought by Eli Lilly against the government of Canada under the North America Free Trade Agreement because it revoked patents on two medicines that Canada’s highest court had found failed to satisfy well-established standards of patentability in Canada [
22]. Canada will have to spend millions of dollars to defend against this claim even if it ultimately wins, which is likely. The even greater danger is that other, poorer countries will be intimidated away from regulating or otherwise acting against the interests of foreign IP investors, even if they are doing so in a non-discriminatory fashion and in the interests of public health.
Discussion
Medical professionals, patients, and others concerned with access to medicines and enhanced generic competition might wonder whether there are justifications for a trade agreement that strengthens IP, investment, and regulatory-participation rights for the originator pharmaceutical industry. They might also wonder what alternative provisions should be in the TPP. The historic justification for longer, stronger, and broader IP protections for medicines is quite simple—they give rise to economic power to charge what the market will bear so that companies can earn extra profits that they thereafter invest to invent the next generation of life-enhancing medicines, including those for currently untreated or undertreated conditions [
23]. As successful as the IP system might be for doing so—and this is highly disputed [
24]—it surely comes at an enormous cost, one that is increasingly intolerable not only to US patients and payers but even more so to poorer populations and poor governments. This analysis concludes, at the very least, that the TPP should not require greater patent, data, and enforcement protections than those prescribed by TRIPS, and instead that it should clarify and endorse greater adoption and use of allowable flexibilities. An even more far-reaching approach, one that cannot be fully developed here, would encourage greater government investment in and regulation of research and development (R&D) with the aim of fully supporting innovation, including clinical trials, while at the same time preserving policy space to ensure competitive access to new medical technologies and their rapid dissemination throughout the world. If one regards medicines as global public goods [
25] and agrees that access to the tools of health create both individual and communal benefits, then one might support trade policies that delink the need for R&D resources from monopoly protections that result in access-prohibitive prices [
26], not only for developing countries but increasingly for rich countries as well.
IP maximization in the TPP will harm access to more affordable medicines in both the US and its trading partners. Policy space on both sides of the Pacific will be reduced while opportunities for excessive pricing will increase dramatically with predictable adverse consequence for the right to health. Armed with knowledge about the details of the TPP’s anti-access provisions, there is still time for health advocates to convince the US Congress and TPP partners that the TPP’s monopoly-enhancing measures must be rejected.
https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4783061/#pmed.1001970.ref015
The Value of Patent Term Extensions to the Pharmaceutical Industry in the USA
In the last 20 or so years various kinds of exclusivity have been introduced in the US, which go beyond the basic patent protection. The most important of these is patent term restoration, but other new incentives introduced include the paediatric extension, exclusivity for drugs with limited patient populations (orphan drugs) and data exclusivity. Since 1988 over 500 products have benefited from patent term restoration and over 130 from the paediatric extension. Of the 40 best selling products in the US in 2006, 26 benefited from patent term restoration and 19 from the paediatric extension, with 29 products benefiting from one or both. The overall impact on these 29 was to increase average effective patent life from 9.2 to 12.8 years, an increase of over three and a half years.
About 39 per cent of the top 40 sales of over US$100bn were contributed by patent extensions. It is estimated that patent extensions could account for about 20 per cent of total US pharmaceutical sales in 2006. Although patent term extensions are currently a sizeable contributor to the gross sales revenues of pharmaceutical companies, the evidence suggests that this contribution will fall significantly in the future, principally as a result of the decline in the number of new chemical entities receiving marketing authorisation. The evidence suggests that the US legislation has been more successful in incentivising the generic market, and that while research-based manufacturers have benefited from patent term extensions, these have not prevented the difficulties they now face which derive from more fundamental economic and technological challenges.
http://journals.sagepub.com/doi/abs/10.1057/jgm.2008.6