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Orphan drug

April 12, 2024

An orphan drug is a pharmaceutical agent that is developed to treat certain rare medical conditions. An orphan drug would not be profitable to produce without government assistance, due to the small population of patients affected by the conditions. The conditions that orphan drugs are used to treat are referred to as orphan diseases. The assignment of orphan status to a disease and to drugs developed to treat it is a matter of public policy that depends on the legislation (if there is any) of the country.

Designation of a drug as an orphan drug has yielded medical breakthroughs that might not otherwise have been achieved, due to the economics of drug research and development.[1] Examples of this can be that in the U.S. and the EU, it is easier to gain marketing approval for an orphan drug. There may be other financial incentives, such as an extended period of exclusivity, during which the producer has sole rights to market the drug. All are intended to encourage development of drugs which would otherwise lack sufficient profit motive to attract corporate research budgets and personnel.[2][3]

Definition edit

United States edit

According to the US Food and Drug Administration (FDA), an orphan drug is defined as one "intended for the treatment, prevention or diagnosis of a rare disease or condition, which is one that affects less than 200,000 persons in the US" (which equates to approximately 6 cases per 10,000 population) "or meets cost recovery provisions of the act".[4][5]

Europe edit

In the European Union (EU), the European Medicines Agency (EMA) defines a drug as "orphan" if it is intended for the diagnosis, prevention or treatment of a life-threatening or chronically and seriously debilitating condition affecting not more than 5 in 10,000 EU people.[6] EMA also qualifies a drug as orphan if – without incentives – it would be unlikely that marketing the drug in the EU would generate sufficient benefit for the affected people and for the drug manufacturer to justify the investment.[6]

Japan edit

In Japan, drugs and medical devices are given the designation as an orphan drug or device based on the Act of Securing Quality, Efficacy, Safety of Pharmaceuticals, Medical Devices, Regenerative or Cellular Therapy Products, Gene Therapy Products, and Cosmetics if they are intended for use in less than 50,000 patients in Japan for which there is a high medical need.[7]

Global statistics edit

As of 2014, there were 281 marketed orphan drugs and more than 400 orphan-designated drugs in clinical trials. More than 60% of orphan drugs were biologics. The U.S. dominated development of orphan drugs, with more than 300 trials, followed by Europe. Cancer treatment was the indication in more than 30% of orphan drug trials.[8]

  • Number of orphan drugs in clinical trials: 40[8]
  • Number of orphan drugs in phase 2 trial: 231[8]
  • Number of orphan drugs in U.S. clinical trials: 350 in the pipeline from research until registration[8]

Effect on investment, sales and profit edit

According to Thomson Reuters in their 2012 publication "The Economic Power of Orphan Drugs", there has been increased investment in orphan drug research and development, partly due to the U.S. Orphan Drug Act of 1983 (ODA) and similar acts in other regions of the world driven by "high-profile philanthropic funding".[9][10]

According to Drug Discovery Today, the years 2001 to 2011 were the "most productive period in the history of orphan drug development, in terms of average annual orphan drug designations and orphan drug approvals".[10]: 660  For the same decade the compound annual growth rate (CAGR) of the orphan drugs was an "impressive 25.8%, compared to only 20.1% for a matched control group of non-orphan drugs".[9]: 6  By 2012, the market for orphan drugs was worth US$637 million, compared with US$638 million for a control group of non-orphan drugs.[9]

By 2012,

the revenue-generating potential of orphan drugs [was] as great as for non-orphan drugs, even though patient populations for rare diseases are significantly smaller. Moreover, we suggest that orphan drugs have greater profitability when considered in the full context of developmental drivers, including government financial incentives, smaller clinical trial sizes, shorter clinical trial times and higher rates of regulatory success.

— Gaze and Breen 2012

According to a 2014 report, the orphan drug market has become increasingly lucrative for a number of reasons. The cost of clinical trials for orphan drugs is substantially lower than for other diseases because trial sizes are naturally much smaller than for more diseases with larger numbers of patients. Small clinical trials and minimal competition place orphan agents at an advantage in regulatory review.[2]

Tax incentives reduce the cost of development. On average the cost per patient for orphan drugs is "six times that of non-orphan drugs, a clear indication of their pricing power". The cost of per-person outlays are large and are expected to increase with wider use of public subsidies.[2]

The 2014 Orphan Drug report stated that the percentage of orphan drug sales as part of all prescription drug sales had been increasing at a rapid rate. The report projected a total of US$176 billion by 2020.[2] Although orphan disease populations are the smallest, the cost of per-patient outlays among them are the largest and are expected to increase as more people with rare diseases become eligible for subsidies – in the U.S., for example, through the Affordable Care Act.[2]

Legislation edit

Orphan drugs generally follow the same regulatory development path as any other pharmaceutical product, in which testing focuses on pharmacokinetics and pharmacodynamics, dosing, stability, safety and efficacy. However, some statistical burdens are lessened to maintain development momentum. For example, orphan drug regulations generally acknowledge the fact that it may not be possible to test 1,000 patients in a phase III clinical trial if fewer than that number are affected by the disease.

Government intervention on behalf of orphan drug development takes several forms:

  • Tax incentives
  • Exclusivity (enhanced patent protection and marketing rights)
  • Research subsidies
  • Creating a government-run enterprise to engage in research and development as in a Crown corporation

A 2015 study of "34 key Canadian stakeholders, including drug regulators, funders, scientists, policy experts, pharmaceutical industry representatives, and patient advocates" investigated factors behind the pharmaceutical industry growing interest in "niche markets" such as orphan drugs.[11]

United States edit

The Orphan Drug Act (ODA) of January 1983, passed in the United States, with lobbying from the National Organization for Rare Disorders and many other organizations,[12] is meant to encourage pharmaceutical companies to develop drugs for diseases that have a small market.[13] Under the ODA drugs, vaccines, and diagnostic agents would qualify for orphan status if they were intended to treat a disease affecting fewer than 200,000 American citizens. Under the ODA orphan drug sponsors qualify for seven-year FDA-administered market Orphan Drug Exclusivity (ODE), "tax credits of up to 50% of R&D costs, R&D grants, waived FDA fees, protocol assistance[10]: 660  and may get clinical trial tax incentives.[13]

In the U.S., orphan drug designation means that the sponsor qualifies for certain benefits, but it does not mean the drug is safe, effective or legal.

In 2002, the Rare Diseases Act was signed into law. It amended the Public Health Service Act to establish the Office of Rare Diseases. It also increased funding for the development of treatments for people with rare diseases.[14]

European Union edit

In 2000, the European Union (EU) enacted similar legislation, Regulation(EC) No 141/2000, which refers to drugs developed to treat rare diseases to as "orphan medicinal products". The EU's definition of an orphan condition is broader than that of the US, in that it also covers some tropical diseases that are primarily found in developing nations.[15] Orphan drug status granted by the European Commission gives marketing exclusivity in the EU for 10 years after approval.[16] The EU's legislation is administered by the Committee on Orphan Medicinal Products of the European Medicines Agency (EMA).

In late 2007 the FDA and EMA agreed to use a common application process for both agencies to make it easier for manufacturers to apply for orphan drug status but, while continuing two separate approval processes.[17]

Other countries edit

Legislation has been implemented by Japan, Singapore, and Australia that offers subsidies and other incentives to encourage the development of drugs that treat orphan diseases.[18]

Numbers of new drugs edit

Under the ODA and EU legislation, many orphan drugs have been developed, including drugs to treat glioma, multiple myeloma, cystic fibrosis, phenylketonuria, snake venom poisoning, and idiopathic thrombocytopenic purpura.[citation needed][19]

The Pharmaceutical Executive opines, that the "ODA is nearly universally acknowledged to be a success".[1]

Before the US Congress enacted the ODA in 1983, only 38 drugs were approved in the US specifically to treat orphan diseases.[3] In the US, from January 1983 to June 2004, 249 orphan drugs received marketing authorization and 1,129 received different orphan drug designations, compared to fewer than ten such products in the decade prior to 1983. From 1983 until May 2010, the FDA approved 353 orphan drugs and granted orphan designations to 2,116 compounds. As of 2010, 200 of the roughly 7,000 officially designated orphan diseases have become treatable.[1]

Critics have questioned whether orphan drug legislation was the real cause of this increase, claiming that many of the new drugs were for disorders which were already being researched anyway, and would have had drugs developed regardless of the legislation, and whether the ODA has truly stimulated the production of non-profitable drugs; the act also has been criticised for allowing some pharmaceutical companies to make a large profit off drugs which have a small market but sell for a high price.[13]

While the European Medicines Agency grants orphan drugs market access in all member states, in practice, they only reach the market when a member state decides that its national health system will reimburse for the drug. For example, in 2008, 44 orphan drugs reached the market in the Netherlands, 35 in Belgium, and 28 in Sweden, while in 2007, 35 such drugs reached the market in France and 23 in Italy.[20]

Though not technically an orphan disease, research and development into the treatment for AIDS has been heavily linked to the Orphan Drug Act. In the beginning of the AIDS epidemic the lack of treatment for the disease was often accredited to a believed lack of commercial base for a medication linked to HIV infection. This encouraged the FDA to use the Orphan Drug Act to help bolster research in this field, and by 1995 13 of the 19 drugs approved by the FDA to treat AIDS had received orphan drug designation, with 10 receiving marketing rights. These are in addition to the 70 designated orphan drugs designed to treat other HIV related illnesses.[21]

Examples for selected diseases edit

Cystic fibrosis edit

In the 1980s, people with cystic fibrosis rarely lived beyond their early teens. Drugs like Pulmozyme and tobramycin, both developed with aid from the ODA, revolutionized treatment for cystic fibrosis patients by significantly improving their quality of life and extending their life expectancies. Now, cystic fibrosis patients often survive into their thirties and some into their fifties.[14]

Familial hypercholesterolemia edit

The 1985 Nobel Prize for medicine went to two researchers for their work related to familial hypercholesterolemia, which causes large and rapid increases in cholesterol levels. Their research led to the development of statin drugs which are now commonly used to treat high cholesterol.[18]

Wilson's disease edit

Penicillamine was developed to treat Wilson's disease, a rare hereditary disease that can lead to a fatal accumulation of copper in the body. This drug was later found to be effective in treating arthritis.[18] Bis-choline tetrathiomolybdate is currently under investigation as a therapy against Wilson's disease.

Phospholipase 2G6-associated neurodegeneration edit

In 2017, FDA granted RT001 orphan drug designation in the treatment of phospholipase 2G6-associated neurodegeneration (PLAN).[22]

Transthyretin-related hereditary amyloidosis edit

The FDA granted Patisiran (Onpattro) orphan drug status and breakthrough therapy designation due to its novel mechanism involving RNA therapy to block the production of an abnormal form of transthyretin. Patisiran received full FDA approval in 2018[23] and its RNA lipid nanoparticle drug delivery system was later used in the Pfizer–BioNTech COVID-19 vaccine and Moderna RNA vaccines.

Activism, research centers edit

The Center for Orphan Drug Research at the University of Minnesota College of Pharmacy helps small companies with insufficient in-house expertise and resources in drug synthesis, formulation, pharmacometrics, and bio-analysis.[24] The Keck Graduate Institute Center for Rare Disease Therapies (CRDT) in Claremont, California, supports projects to revive potential orphan drugs whose development has stalled by identifying barriers to commercialization, such as problems with formulation and bio-processing.[24]

Numerous advocacy groups such as the National Organization for Rare Disorders, Global Genes Project, Children's Rare Disease Network, Abetalipoproteinemia Collaboration Foundation, Zellweger Baby Support Network, and the Friedreich's Ataxia Research Alliance have been founded in order to advocate on behalf of patients with rare diseases with a particular emphasis on diseases that affect children.[1]

Cost edit

According to a 2015 report published by EvaluatePharma, the economics of orphan drugs mirrors the economics of the pharmaceutical market as a whole but has a few very large differences.[25] The market for orphan drugs is by definition very small, but while the customer base is drastically smaller the cost of research and development is very much the same as for non orphan drugs. This, the producers have claimed, causes them to charge extremely high amounts for treatment, sometimes as high as $700,000 a year, as in the case of Spinraza (Biogen), FDA approved in December 2016 for spinal muscular atrophy,[26] placing a large amount of stress on insurance companies and patients. An analysis of 12 orphan drugs that were approved in the US between 1990 and 2000 estimated a price reduction of on average 50% upon loss of marketing exclusivity, with a range of price reductions from 14% to 95%.[27]

Governments have implemented steps to reduce high research and development cost with subsidies and other forms of financial assistance. The largest assistance are tax breaks which can be as high as 50% of research and development costs.[28] Orphan drug manufacturers are also able to take advantage of the small customer base to cut cost on clinical trials due to the small number of cases to have smaller trials which reduces cost. These smaller clinical trials also allow orphan drugs to move to market faster as the average time to receive FDA approval for an orphan drug is 10 months compared to 13 months for non-orphan drugs. This is especially true in the market for cancer drugs, as a 2011 study found that between 2004 and 2010 orphan drug trials were more likely to be smaller and less randomized than their non-orphan counterparts, but still had a higher FDA approval rate, with 15 orphan cancer drugs being approved, while only 12 non-orphan drugs were approved.[29] This allows manufactures to get cost to the point that it is economically feasible to produce these treatments.[28] The subsidies can total up to $30 million per fiscal year in the United States alone.[citation needed]

By 2015, industry analysts and academic researchers agreed, that the sky-high price of orphan drugs, such as eculizumab, was not related to research, development and manufacturing costs. Their price is arbitrary and they have become more profitable than traditional medicines.[30]

Public resources went into understanding the molecular basis of the disease, public resources went into the technology to make antibodies and finally, Alexion, to their credit, kind of picked up the pieces.

— Sachdev Sidhu 2015

Public funding edit

Evaluation criteria edit

By 2007 the use of economic evaluation methods regarding public-funding of orphan drugs, using estimates of the incremental cost-effectiveness, for example, became more established internationally.[31] The QALY has often been used in cost-utility analysis to calculate the ratio of cost to QALYs saved for a particular health care intervention.[32][33] By 2008 the National Institute for Health and Care Excellence (NICE) in England and Wales, for example, operated with a threshold range of £20,000–30,000 per quality-adjusted life year (QALY).[34] By 2005 doubts were raised about the use of economic evaluations in orphan drugs.[31] By 2008 most of the orphan drugs appraised had cost-effectiveness thresholds "well in excess of the 'accepted' level and would not be reimbursed according to conventional criteria".[34] As early as 2005 McCabe et al. argued[35][36] that rarity should not have a premium and orphan drugs should be treated like other pharmaceuticals in general.[35][36] Drummond et al.[36] argued that the social value of health technologies should also be included in the assessment along with the estimation of the incremental cost-effectiveness ratio.

Abuse potential edit

 
Rosuvastatin (brand name Crestor) is an example of a drug that received Orphan Drug funding but was later marketed to a large consumer base.

The very large incentives given to pharmaceutical companies to produce orphan drugs have led to the impression that the financial support afforded to make these drugs possible is akin to abuse.[37] Because drugs can be used to treat multiple conditions, companies can take drugs that were filed with their government agency as orphan drugs to receive financial assistance, and then market it to a wide population to increase their profit margin. For example AstraZeneca's cholesterol drug Crestor was filed as a treatment for the rare disease pediatric familial hypercholesterolemia. After the drug was approved for orphan drug designation, and AstraZeneca had received tax breaks and other advantages, AstraZeneca later applied and received FDA approval for the drug to be used to treat cholesterol in all diabetics.[18]

NICE edit

The UK's National Institute for Health and Care Excellence (NICE) can pay from £100,000 to £300,000 per QALY (Quality Adjusted Life Year) for treatments of "very rare conditions". This is compared to under £20,000 for non-orphan drugs.[38]

In 2015, NICE held consultations with "patient groups, the Department of Health, companies, learned societies, charities and researchers" regarding the appraisal of medicines and other technologies. There was a call for more research into new processes, including:[39]

the model of pharmaceutical research and development, the expectations that companies and patient groups have about how risk and reward is shared between the industry and a publicly funded NHS, and in the arrangements for commissioning expensive new treatments.

— NICE 2014

See also edit

References edit

  1. ^ a b c d Armstrong, Walter (May 2010). "Pharma's Orphans". Pharmaceutical Executive.
  2. ^ a b c d e Hadjivasiliou, Andreas (October 2014), "Orphan Drug Report 2014" (PDF), EvaluatePharma, retrieved 28 June 2015
  3. ^ a b Rich Daly (5 September 2002). "House Offers Incentives For Development of 'Orphan' Drugs". Congressional Quarterly Daily Monitor.
  4. ^ "Developing Products for Rare Diseases & Conditions". US Food and Drug Administration. 20 December 2018. Retrieved 28 December 2019.
  5. ^ Hall, Anthony K; Carlson, Marilyn R (2014). "The current status of orphan drug development in Europe and the US". Intractable and Rare Diseases Research. 3 (1): 1–7. doi:10.5582/irdr.3.1. ISSN 2186-3644. PMC 4204542. PMID 25343119.
  6. ^ a b Giannuzzi, Viviana; Conte, Rosa; Landi, Annalisa; Ottomano, Serena Antonella; Bonifazi, Donato; Baiardi, Paola; Bonifazi, Fedele; Ceci, Adriana (3 April 2017). "Orphan medicinal products in Europe and United States to cover needs of patients with rare diseases: an increased common effort is to be foreseen". Orphanet Journal of Rare Diseases. 12 (1): 64. doi:10.1186/s13023-017-0617-1. ISSN 1750-1172. PMC 5376695. PMID 28372595.
  7. ^ "Ministry of Health, Labour and Welfare: Pharmaceuticals and Medical Devices". www.mhlw.go.jp. Retrieved 2023-01-11.
  8. ^ a b c d Global orphan drug market to reach US$120 billion by 2018 (press release), New Delhi: Kuick Research, 7 Feb 2014, retrieved 20 March 2014
  9. ^ a b c Laura Gaze; Jennifer Breen (2012), (PDF), Thomson Reuters, archived from the original (PDF) on 13 May 2015, retrieved 29 June 2015
  10. ^ a b c Meeking, Kiran N.; Williams, Cory S. M.; Arrowsmith, John E. (15 August 2012), "Orphan drug development: an economically viable strategy for biopharma R&D", Drug Discovery Today, 17 (13–14): 660–664, doi:10.1016/j.drudis.2012.02.005, PMID 22366309, retrieved 29 June 2015
  11. ^ Shannon Gibson; Hamid R Raziee; Trudo Lemmens (19 March 2015). "Why the Shift? Taking a Closer Look at the Growing Interest in Niche Markets and Personalized Medicine". World Medical & Health Policy. 7 (1): 3–27. doi:10.1002/wmh3.131. PMC 4405057. PMID 25914853.
  12. ^ Henkel, John (1999). "Orphan Drug Law Matures into Medical Mainstay". FDA Consumer. U.S. Food and Drug Administration. Retrieved 14 February 2009.
  13. ^ a b c Pollack, Andrew (30 April 1990). "Orphan Drug Law Spurs Debate". The New York Times. Retrieved 15 February 2009.
  14. ^ a b Illingworth, Patricia; Cohen, Jillian; Illingworth, P (2004). "Orphan Drug Policies: Implications for the United States, Canada, and Developing Countries". Health Law Journal. 12: 183–200. PMID 16539081.
  15. ^ "Orphan disease definition - Medical Dictionary definitions of popular medical terms easily defined on MedTerms". Medterms.com. 2002-08-25. Retrieved 2010-06-07.
  16. ^ Gerke, Sara; Pattinson, Shaun D. (2017-02-09). "EU Marketing Authorisation of Orphan Medicinal Products and Its Impact on Related Research" (PDF). European Journal of Health Law. 24 (5): 541–564. doi:10.1163/15718093-12341439.
  17. ^ Donna Young (2007-11-28). "U.S., EU Will Use Same Orphan Drug Application". BioWorld News. Washington. Retrieved 2008-01-06. In an attempt to simplify the process for obtaining orphan status for medications targeting rare diseases, the FDA and the European Medicines Agency (EMA) have created a common application. ... U.S. and European regulators still will conduct independent reviews of application submissions to ensure the data submitted meet the legal and scientific requirements of their respective jurisdictions, the agencies said. Alt URL 2008-03-09 at the Wayback Machine
  18. ^ a b c d Andrew Duffy (23 February 2002). "ORPHAN DISEASES A RARE OCCURRENCE: A desperate search for help; County family joins long list with rare diseases in seeking a miracle". Windsor Star (Ontario).
  19. ^ https://www0.gsb.columbia.edu/mygsb/faculty/research/pubfiles/4716/Lichtenberg%20Orphan%20drugs%20SSRN%202011-01-10.pdf [bare URL PDF]
  20. ^ Denis, Alain; Mergaert, Lut; Fostier, Christel; et al. (2010). "Issues Surrounding Orphan Disease and Orphan Drug Policies in Europe". Applied Health Economics and Health Policy. 8 (5): 343–50. doi:10.2165/11536990-000000000-00000. PMID 20804226. S2CID 27388954.
  21. ^ Arno, Peter S.; Bonuck, Karen; Davis, Michael (1995-01-01). "Rare Diseases, Drug Development, and AIDS: The Impact of the Orphan Drug Act". The Milbank Quarterly. 73 (2): 231–252. doi:10.2307/3350258. JSTOR 3350258. PMID 7776947.
  22. ^ . Global Newswire. 2 November 2017. Archived from the original on 1 April 2019. Retrieved 12 March 2019.
  23. ^ Brooks, Megan (10 August 2018). "FDA approves first-of-its kind targeted RNA-based therapy to treat a rare disease". fda.gov. US Federal Drug Administration. Retrieved 5 May 2021.
  24. ^ a b Wechsler, Jill (July 2008). "Celebrating 25 Years of Orphan Drugs". Pharmaceutical Technology.
  25. ^ Hadjivasiliou, Andreas (2015). EvaluatePharma Orphan Drug Report 2015. EvaulatePharma.
  26. ^ Thomas, Katie (30 December 2016). "Costly Drug for Fatal Muscular Disease Wins F.D.A. Approval". The New York Times. Retrieved 12 April 2017.
  27. ^ Schey, Carina; Milanova, Tsveta; Hutchings, Adam (2011). "Estimating the budget impact of orphan medicines in Europe: 2010 - 2020". Orphanet Journal of Rare Diseases. 6 (62): 62. doi:10.1186/1750-1172-6-62. PMC 3191371. PMID 21951518.
  28. ^ a b Meekings, Kiran N.; Williams, Cory S. M.; Arrowsmith, John E. (2012-07-01). "Orphan drug development: an economically viable strategy for biopharma R&D". Drug Discovery Today. 17 (13–14): 660–664. doi:10.1016/j.drudis.2012.02.005. PMID 22366309.
  29. ^ Kesselheim, A. S.; Myers, J. A.; Avorn, J. (2011-06-08). "Characteristics of clinical trials to support approval of orphan vs nonorphan drugs for cancer". JAMA. 305 (22): 2320–2326. doi:10.1001/jama.2011.769. ISSN 0098-7484. PMID 21642684.
  30. ^ Crowe, Kelly (25 June 2015), "How pharmaceutical company Alexion set the price of the world's most expensive drug: Cost of one of world's most expensive drugs shrouded in corporate secrecy", CBC News, retrieved 25 June 2015
  31. ^ a b Drummond, M. F.; Grubert, N. (2007), International Trends in the Use of Health Economic Data, Spectrum Report, Decision Resources, Waltham, Mass.{{citation}}: CS1 maint: location missing publisher (link)
  32. ^ "Measuring effectiveness and cost effectiveness: the QALY" (Press release). NICE. 20 April 2010. Retrieved 15 Jun 2015.
  33. ^ . NICE. 2013. Archived from the original on 7 May 2015. Retrieved 15 Jun 2015.
  34. ^ a b Drummond, Michael F. (2008). "Challenges in the economic evaluation of orphan drugs". Eurohealth. 14 (2): 16–257.
  35. ^ a b McCabe, C; Claxton, K; Tsuchiya, A. (2005). "Orphan drugs and the NHS". British Medical Journal. 331 (4): 1016–19. doi:10.1136/bmj.331.7523.1016. PMC 1273462. PMID 16254305.
  36. ^ a b c McCabe, C; Tsuchiya, A; Claxton, K; Raftery, J. (2007). "Assessing the economic challenges posed by orphan drugs: a comment on Drummond et al". International Journal of Technology Assessment in Health Care. 23 (3): 397–404. doi:10.1017/s0266462307071012. PMID 17579945. S2CID 29572982.
  37. ^ Simoens, Steven (2011-06-17). "Pricing and reimbursement of orphan drugs: the need for more transparency". Orphanet Journal of Rare Diseases. 6 (1): 42. doi:10.1186/1750-1172-6-42. PMC 3132155. PMID 21682893.
  38. ^ "Our charter | Who we are | About". NICE. Retrieved 2021-03-29.
  39. ^ "NICE calls for a new approach to managing the entry of drugs into the NHS" (Press release). NICE. 18 September 2014. Retrieved 29 June 2015.

External links edit

 
Look up orphan drug in Wiktionary, the free dictionary.
 
Wikimedia Commons has media related to Orphan drugs.
  • Drug Information Association (DIA)
  • EVENT: DIA/FDA Orphan Drug Designation Workshop November 2010
  • European Commission - The Orphan drugs strategy
  • USA Food and Drug Administration: The Orphan Drug Act (as amended)
  • US FDA List of Orphan Designations and Approvals

April 12, 2024
orphan, drug, orphan, drug, pharmaceutical, agent, that, developed, treat, certain, rare, medical, conditions, orphan, drug, would, profitable, produce, without, government, assistance, small, population, patients, affected, conditions, conditions, that, orpha. An orphan drug is a pharmaceutical agent that is developed to treat certain rare medical conditions An orphan drug would not be profitable to produce without government assistance due to the small population of patients affected by the conditions The conditions that orphan drugs are used to treat are referred to as orphan diseases The assignment of orphan status to a disease and to drugs developed to treat it is a matter of public policy that depends on the legislation if there is any of the country Designation of a drug as an orphan drug has yielded medical breakthroughs that might not otherwise have been achieved due to the economics of drug research and development 1 Examples of this can be that in the U S and the EU it is easier to gain marketing approval for an orphan drug There may be other financial incentives such as an extended period of exclusivity during which the producer has sole rights to market the drug All are intended to encourage development of drugs which would otherwise lack sufficient profit motive to attract corporate research budgets and personnel 2 3 Contents 1 Definition 1 1 United States 1 2 Europe 1 3 Japan 2 Global statistics 3 Effect on investment sales and profit 4 Legislation 4 1 United States 4 2 European Union 4 3 Other countries 4 4 Numbers of new drugs 5 Examples for selected diseases 5 1 Cystic fibrosis 5 2 Familial hypercholesterolemia 5 3 Wilson s disease 5 4 Phospholipase 2G6 associated neurodegeneration 5 5 Transthyretin related hereditary amyloidosis 6 Activism research centers 7 Cost 8 Public funding 8 1 Evaluation criteria 8 2 Abuse potential 8 3 NICE 9 See also 10 References 11 External linksDefinition editUnited States edit According to the US Food and Drug Administration FDA an orphan drug is defined as one intended for the treatment prevention or diagnosis of a rare disease or condition which is one that affects less than 200 000 persons in the US which equates to approximately 6 cases per 10 000 population or meets cost recovery provisions of the act 4 5 Europe edit In the European Union EU the European Medicines Agency EMA defines a drug as orphan if it is intended for the diagnosis prevention or treatment of a life threatening or chronically and seriously debilitating condition affecting not more than 5 in 10 000 EU people 6 EMA also qualifies a drug as orphan if without incentives it would be unlikely that marketing the drug in the EU would generate sufficient benefit for the affected people and for the drug manufacturer to justify the investment 6 Japan edit In Japan drugs and medical devices are given the designation as an orphan drug or device based on the Act of Securing Quality Efficacy Safety of Pharmaceuticals Medical Devices Regenerative or Cellular Therapy Products Gene Therapy Products and Cosmetics if they are intended for use in less than 50 000 patients in Japan for which there is a high medical need 7 Global statistics editAs of 2014 update there were 281 marketed orphan drugs and more than 400 orphan designated drugs in clinical trials More than 60 of orphan drugs were biologics The U S dominated development of orphan drugs with more than 300 trials followed by Europe Cancer treatment was the indication in more than 30 of orphan drug trials 8 Number of orphan drugs in clinical trials 40 8 Number of orphan drugs in phase 2 trial 231 8 Number of orphan drugs in U S clinical trials 350 in the pipeline from research until registration 8 Effect on investment sales and profit editAccording to Thomson Reuters in their 2012 publication The Economic Power of Orphan Drugs there has been increased investment in orphan drug research and development partly due to the U S Orphan Drug Act of 1983 ODA and similar acts in other regions of the world driven by high profile philanthropic funding 9 10 According to Drug Discovery Today the years 2001 to 2011 were the most productive period in the history of orphan drug development in terms of average annual orphan drug designations and orphan drug approvals 10 660 For the same decade the compound annual growth rate CAGR of the orphan drugs was an impressive 25 8 compared to only 20 1 for a matched control group of non orphan drugs 9 6 By 2012 the market for orphan drugs was worth US 637 million compared with US 638 million for a control group of non orphan drugs 9 By 2012 the revenue generating potential of orphan drugs was as great as for non orphan drugs even though patient populations for rare diseases are significantly smaller Moreover we suggest that orphan drugs have greater profitability when considered in the full context of developmental drivers including government financial incentives smaller clinical trial sizes shorter clinical trial times and higher rates of regulatory success Gaze and Breen 2012 According to a 2014 report the orphan drug market has become increasingly lucrative for a number of reasons The cost of clinical trials for orphan drugs is substantially lower than for other diseases because trial sizes are naturally much smaller than for more diseases with larger numbers of patients Small clinical trials and minimal competition place orphan agents at an advantage in regulatory review 2 Tax incentives reduce the cost of development On average the cost per patient for orphan drugs is six times that of non orphan drugs a clear indication of their pricing power The cost of per person outlays are large and are expected to increase with wider use of public subsidies 2 The 2014 Orphan Drug report stated that the percentage of orphan drug sales as part of all prescription drug sales had been increasing at a rapid rate The report projected a total of US 176 billion by 2020 2 Although orphan disease populations are the smallest the cost of per patient outlays among them are the largest and are expected to increase as more people with rare diseases become eligible for subsidies in the U S for example through the Affordable Care Act 2 Legislation editOrphan drugs generally follow the same regulatory development path as any other pharmaceutical product in which testing focuses on pharmacokinetics and pharmacodynamics dosing stability safety and efficacy However some statistical burdens are lessened to maintain development momentum For example orphan drug regulations generally acknowledge the fact that it may not be possible to test 1 000 patients in a phase III clinical trial if fewer than that number are affected by the disease Government intervention on behalf of orphan drug development takes several forms Tax incentives Exclusivity enhanced patent protection and marketing rights Research subsidies Creating a government run enterprise to engage in research and development as in a Crown corporationA 2015 study of 34 key Canadian stakeholders including drug regulators funders scientists policy experts pharmaceutical industry representatives and patient advocates investigated factors behind the pharmaceutical industry growing interest in niche markets such as orphan drugs 11 United States edit The Orphan Drug Act ODA of January 1983 passed in the United States with lobbying from the National Organization for Rare Disorders and many other organizations 12 is meant to encourage pharmaceutical companies to develop drugs for diseases that have a small market 13 Under the ODA drugs vaccines and diagnostic agents would qualify for orphan status if they were intended to treat a disease affecting fewer than 200 000 American citizens Under the ODA orphan drug sponsors qualify for seven year FDA administered market Orphan Drug Exclusivity ODE tax credits of up to 50 of R amp D costs R amp D grants waived FDA fees protocol assistance 10 660 and may get clinical trial tax incentives 13 In the U S orphan drug designation means that the sponsor qualifies for certain benefits but it does not mean the drug is safe effective or legal In 2002 the Rare Diseases Act was signed into law It amended the Public Health Service Act to establish the Office of Rare Diseases It also increased funding for the development of treatments for people with rare diseases 14 European Union edit In 2000 the European Union EU enacted similar legislation Regulation EC No 141 2000 which refers to drugs developed to treat rare diseases to as orphan medicinal products The EU s definition of an orphan condition is broader than that of the US in that it also covers some tropical diseases that are primarily found in developing nations 15 Orphan drug status granted by the European Commission gives marketing exclusivity in the EU for 10 years after approval 16 The EU s legislation is administered by the Committee on Orphan Medicinal Products of the European Medicines Agency EMA In late 2007 the FDA and EMA agreed to use a common application process for both agencies to make it easier for manufacturers to apply for orphan drug status but while continuing two separate approval processes 17 Other countries edit Legislation has been implemented by Japan Singapore and Australia that offers subsidies and other incentives to encourage the development of drugs that treat orphan diseases 18 Numbers of new drugs edit Under the ODA and EU legislation many orphan drugs have been developed including drugs to treat glioma multiple myeloma cystic fibrosis phenylketonuria snake venom poisoning and idiopathic thrombocytopenic purpura citation needed 19 The Pharmaceutical Executive opines that the ODA is nearly universally acknowledged to be a success 1 Before the US Congress enacted the ODA in 1983 only 38 drugs were approved in the US specifically to treat orphan diseases 3 In the US from January 1983 to June 2004 249 orphan drugs received marketing authorization and 1 129 received different orphan drug designations compared to fewer than ten such products in the decade prior to 1983 From 1983 until May 2010 the FDA approved 353 orphan drugs and granted orphan designations to 2 116 compounds As of 2010 200 of the roughly 7 000 officially designated orphan diseases have become treatable 1 Critics have questioned whether orphan drug legislation was the real cause of this increase claiming that many of the new drugs were for disorders which were already being researched anyway and would have had drugs developed regardless of the legislation and whether the ODA has truly stimulated the production of non profitable drugs the act also has been criticised for allowing some pharmaceutical companies to make a large profit off drugs which have a small market but sell for a high price 13 While the European Medicines Agency grants orphan drugs market access in all member states in practice they only reach the market when a member state decides that its national health system will reimburse for the drug For example in 2008 44 orphan drugs reached the market in the Netherlands 35 in Belgium and 28 in Sweden while in 2007 35 such drugs reached the market in France and 23 in Italy 20 Though not technically an orphan disease research and development into the treatment for AIDS has been heavily linked to the Orphan Drug Act In the beginning of the AIDS epidemic the lack of treatment for the disease was often accredited to a believed lack of commercial base for a medication linked to HIV infection This encouraged the FDA to use the Orphan Drug Act to help bolster research in this field and by 1995 13 of the 19 drugs approved by the FDA to treat AIDS had received orphan drug designation with 10 receiving marketing rights These are in addition to the 70 designated orphan drugs designed to treat other HIV related illnesses 21 Examples for selected diseases editCystic fibrosis edit In the 1980s people with cystic fibrosis rarely lived beyond their early teens Drugs like Pulmozyme and tobramycin both developed with aid from the ODA revolutionized treatment for cystic fibrosis patients by significantly improving their quality of life and extending their life expectancies Now cystic fibrosis patients often survive into their thirties and some into their fifties 14 Familial hypercholesterolemia edit The 1985 Nobel Prize for medicine went to two researchers for their work related to familial hypercholesterolemia which causes large and rapid increases in cholesterol levels Their research led to the development of statin drugs which are now commonly used to treat high cholesterol 18 Wilson s disease edit Penicillamine was developed to treat Wilson s disease a rare hereditary disease that can lead to a fatal accumulation of copper in the body This drug was later found to be effective in treating arthritis 18 Bis choline tetrathiomolybdate is currently under investigation as a therapy against Wilson s disease Phospholipase 2G6 associated neurodegeneration edit In 2017 FDA granted RT001 orphan drug designation in the treatment of phospholipase 2G6 associated neurodegeneration PLAN 22 Transthyretin related hereditary amyloidosis edit The FDA granted Patisiran Onpattro orphan drug status and breakthrough therapy designation due to its novel mechanism involving RNA therapy to block the production of an abnormal form of transthyretin Patisiran received full FDA approval in 2018 23 and its RNA lipid nanoparticle drug delivery system was later used in the Pfizer BioNTech COVID 19 vaccine and Moderna RNA vaccines Activism research centers editThe Center for Orphan Drug Research at the University of Minnesota College of Pharmacy helps small companies with insufficient in house expertise and resources in drug synthesis formulation pharmacometrics and bio analysis 24 The Keck Graduate Institute Center for Rare Disease Therapies CRDT in Claremont California supports projects to revive potential orphan drugs whose development has stalled by identifying barriers to commercialization such as problems with formulation and bio processing 24 Numerous advocacy groups such as the National Organization for Rare Disorders Global Genes Project Children s Rare Disease Network Abetalipoproteinemia Collaboration Foundation Zellweger Baby Support Network and the Friedreich s Ataxia Research Alliance have been founded in order to advocate on behalf of patients with rare diseases with a particular emphasis on diseases that affect children 1 Cost editAccording to a 2015 report published by EvaluatePharma the economics of orphan drugs mirrors the economics of the pharmaceutical market as a whole but has a few very large differences 25 The market for orphan drugs is by definition very small but while the customer base is drastically smaller the cost of research and development is very much the same as for non orphan drugs This the producers have claimed causes them to charge extremely high amounts for treatment sometimes as high as 700 000 a year as in the case of Spinraza Biogen FDA approved in December 2016 for spinal muscular atrophy 26 placing a large amount of stress on insurance companies and patients An analysis of 12 orphan drugs that were approved in the US between 1990 and 2000 estimated a price reduction of on average 50 upon loss of marketing exclusivity with a range of price reductions from 14 to 95 27 Governments have implemented steps to reduce high research and development cost with subsidies and other forms of financial assistance The largest assistance are tax breaks which can be as high as 50 of research and development costs 28 Orphan drug manufacturers are also able to take advantage of the small customer base to cut cost on clinical trials due to the small number of cases to have smaller trials which reduces cost These smaller clinical trials also allow orphan drugs to move to market faster as the average time to receive FDA approval for an orphan drug is 10 months compared to 13 months for non orphan drugs This is especially true in the market for cancer drugs as a 2011 study found that between 2004 and 2010 orphan drug trials were more likely to be smaller and less randomized than their non orphan counterparts but still had a higher FDA approval rate with 15 orphan cancer drugs being approved while only 12 non orphan drugs were approved 29 This allows manufactures to get cost to the point that it is economically feasible to produce these treatments 28 The subsidies can total up to 30 million per fiscal year in the United States alone citation needed By 2015 industry analysts and academic researchers agreed that the sky high price of orphan drugs such as eculizumab was not related to research development and manufacturing costs Their price is arbitrary and they have become more profitable than traditional medicines 30 Public resources went into understanding the molecular basis of the disease public resources went into the technology to make antibodies and finally Alexion to their credit kind of picked up the pieces Sachdev Sidhu 2015Public funding editEvaluation criteria edit By 2007 the use of economic evaluation methods regarding public funding of orphan drugs using estimates of the incremental cost effectiveness for example became more established internationally 31 The QALY has often been used in cost utility analysis to calculate the ratio of cost to QALYs saved for a particular health care intervention 32 33 By 2008 the National Institute for Health and Care Excellence NICE in England and Wales for example operated with a threshold range of 20 000 30 000 per quality adjusted life year QALY 34 By 2005 doubts were raised about the use of economic evaluations in orphan drugs 31 By 2008 most of the orphan drugs appraised had cost effectiveness thresholds well in excess of the accepted level and would not be reimbursed according to conventional criteria 34 As early as 2005 McCabe et al argued 35 36 that rarity should not have a premium and orphan drugs should be treated like other pharmaceuticals in general 35 36 Drummond et al 36 argued that the social value of health technologies should also be included in the assessment along with the estimation of the incremental cost effectiveness ratio Abuse potential edit nbsp Rosuvastatin brand name Crestor is an example of a drug that received Orphan Drug funding but was later marketed to a large consumer base The very large incentives given to pharmaceutical companies to produce orphan drugs have led to the impression that the financial support afforded to make these drugs possible is akin to abuse 37 Because drugs can be used to treat multiple conditions companies can take drugs that were filed with their government agency as orphan drugs to receive financial assistance and then market it to a wide population to increase their profit margin For example AstraZeneca s cholesterol drug Crestor was filed as a treatment for the rare disease pediatric familial hypercholesterolemia After the drug was approved for orphan drug designation and AstraZeneca had received tax breaks and other advantages AstraZeneca later applied and received FDA approval for the drug to be used to treat cholesterol in all diabetics 18 NICE edit The UK s National Institute for Health and Care Excellence NICE can pay from 100 000 to 300 000 per QALY Quality Adjusted Life Year for treatments of very rare conditions This is compared to under 20 000 for non orphan drugs 38 In 2015 NICE held consultations with patient groups the Department of Health companies learned societies charities and researchers regarding the appraisal of medicines and other technologies There was a call for more research into new processes including 39 the model of pharmaceutical research and development the expectations that companies and patient groups have about how risk and reward is shared between the industry and a publicly funded NHS and in the arrangements for commissioning expensive new treatments NICE 2014See also editRare disease Drug development European Organization for Rare Diseases Supplementary protection certificateReferences edit a b c d Armstrong Walter May 2010 Pharma s Orphans Pharmaceutical Executive a b c d e Hadjivasiliou Andreas October 2014 Orphan Drug Report 2014 PDF EvaluatePharma retrieved 28 June 2015 a b Rich Daly 5 September 2002 House Offers Incentives For Development of Orphan Drugs Congressional Quarterly Daily Monitor Developing Products for Rare Diseases amp Conditions US Food and Drug Administration 20 December 2018 Retrieved 28 December 2019 Hall Anthony K Carlson Marilyn R 2014 The current status of orphan drug development in Europe and the US Intractable and Rare Diseases Research 3 1 1 7 doi 10 5582 irdr 3 1 ISSN 2186 3644 PMC 4204542 PMID 25343119 a b Giannuzzi Viviana Conte Rosa Landi Annalisa Ottomano Serena Antonella Bonifazi Donato Baiardi Paola Bonifazi Fedele Ceci Adriana 3 April 2017 Orphan medicinal products in Europe and United States to cover needs of patients with rare diseases an increased common effort is to be foreseen Orphanet Journal of Rare Diseases 12 1 64 doi 10 1186 s13023 017 0617 1 ISSN 1750 1172 PMC 5376695 PMID 28372595 Ministry of Health Labour and Welfare Pharmaceuticals and Medical Devices www mhlw go jp Retrieved 2023 01 11 a b c d Global orphan drug market to reach US 120 billion by 2018 press release New Delhi Kuick Research 7 Feb 2014 retrieved 20 March 2014 a b c Laura Gaze Jennifer Breen 2012 The Economic Power of Orphan Drugs PDF Thomson Reuters archived from the original PDF on 13 May 2015 retrieved 29 June 2015 a b c Meeking Kiran N Williams Cory S M Arrowsmith John E 15 August 2012 Orphan drug development an economically viable strategy for biopharma R amp D Drug Discovery Today 17 13 14 660 664 doi 10 1016 j drudis 2012 02 005 PMID 22366309 retrieved 29 June 2015 Shannon Gibson Hamid R Raziee Trudo Lemmens 19 March 2015 Why the Shift Taking a Closer Look at the Growing Interest in Niche Markets and Personalized Medicine World Medical amp Health Policy 7 1 3 27 doi 10 1002 wmh3 131 PMC 4405057 PMID 25914853 Henkel John 1999 Orphan Drug Law Matures into Medical Mainstay FDA Consumer U S Food and Drug Administration Retrieved 14 February 2009 a b c Pollack Andrew 30 April 1990 Orphan Drug Law Spurs Debate The New York Times Retrieved 15 February 2009 a b Illingworth Patricia Cohen Jillian Illingworth P 2004 Orphan Drug Policies Implications for the United States Canada and Developing Countries Health Law Journal 12 183 200 PMID 16539081 Orphan disease definition Medical Dictionary definitions of popular medical terms easily defined on MedTerms Medterms com 2002 08 25 Retrieved 2010 06 07 Gerke Sara Pattinson Shaun D 2017 02 09 EU Marketing Authorisation of Orphan Medicinal Products and Its Impact on Related Research PDF European Journal of Health Law 24 5 541 564 doi 10 1163 15718093 12341439 Donna Young 2007 11 28 U S EU Will Use Same Orphan Drug Application BioWorld News Washington Retrieved 2008 01 06 In an attempt to simplify the process for obtaining orphan status for medications targeting rare diseases the FDA and the European Medicines Agency EMA have created a common application U S and European regulators still will conduct independent reviews of application submissions to ensure the data submitted meet the legal and scientific requirements of their respective jurisdictions the agencies said Alt URL Archived 2008 03 09 at the Wayback Machine a b c d Andrew Duffy 23 February 2002 ORPHAN DISEASES A RARE OCCURRENCE A desperate search for help County family joins long list with rare diseases in seeking a miracle Windsor Star Ontario https www0 gsb columbia edu mygsb faculty research pubfiles 4716 Lichtenberg 20Orphan 20drugs 20SSRN 202011 01 10 pdf bare URL PDF Denis Alain Mergaert Lut Fostier Christel et al 2010 Issues Surrounding Orphan Disease and Orphan Drug Policies in Europe Applied Health Economics and Health Policy 8 5 343 50 doi 10 2165 11536990 000000000 00000 PMID 20804226 S2CID 27388954 Arno Peter S Bonuck Karen Davis Michael 1995 01 01 Rare Diseases Drug Development and AIDS The Impact of the Orphan Drug Act The Milbank Quarterly 73 2 231 252 doi 10 2307 3350258 JSTOR 3350258 PMID 7776947 US FDA Grants Orphan Drug Designation for Retrotope s RT001 in the Treatment of Phospholipase 2G6 PLA2G6 Associated Neurodegeneration Global Newswire 2 November 2017 Archived from the original on 1 April 2019 Retrieved 12 March 2019 Brooks Megan 10 August 2018 FDA approves first of its kind targeted RNA based therapy to treat a rare disease fda gov US Federal Drug Administration Retrieved 5 May 2021 a b Wechsler Jill July 2008 Celebrating 25 Years of Orphan Drugs Pharmaceutical Technology Hadjivasiliou Andreas 2015 EvaluatePharma Orphan Drug Report 2015 EvaulatePharma Thomas Katie 30 December 2016 Costly Drug for Fatal Muscular Disease Wins F D A Approval The New York Times Retrieved 12 April 2017 Schey Carina Milanova Tsveta Hutchings Adam 2011 Estimating the budget impact of orphan medicines in Europe 2010 2020 Orphanet Journal of Rare Diseases 6 62 62 doi 10 1186 1750 1172 6 62 PMC 3191371 PMID 21951518 a b Meekings Kiran N Williams Cory S M Arrowsmith John E 2012 07 01 Orphan drug development an economically viable strategy for biopharma R amp D Drug Discovery Today 17 13 14 660 664 doi 10 1016 j drudis 2012 02 005 PMID 22366309 Kesselheim A S Myers J A Avorn J 2011 06 08 Characteristics of clinical trials to support approval of orphan vs nonorphan drugs for cancer JAMA 305 22 2320 2326 doi 10 1001 jama 2011 769 ISSN 0098 7484 PMID 21642684 Crowe Kelly 25 June 2015 How pharmaceutical company Alexion set the price of the world s most expensive drug Cost of one of world s most expensive drugs shrouded in corporate secrecy CBC News retrieved 25 June 2015 a b Drummond M F Grubert N 2007 International Trends in the Use of Health Economic Data Spectrum Report Decision Resources Waltham Mass a href Template Citation html title Template Citation citation a CS1 maint location missing publisher link Measuring effectiveness and cost effectiveness the QALY Press release NICE 20 April 2010 Retrieved 15 Jun 2015 Guide to the methods of technology appraisal 2013 NICE 2013 Archived from the original on 7 May 2015 Retrieved 15 Jun 2015 a b Drummond Michael F 2008 Challenges in the economic evaluation of orphan drugs Eurohealth 14 2 16 257 a b McCabe C Claxton K Tsuchiya A 2005 Orphan drugs and the NHS British Medical Journal 331 4 1016 19 doi 10 1136 bmj 331 7523 1016 PMC 1273462 PMID 16254305 a b c McCabe C Tsuchiya A Claxton K Raftery J 2007 Assessing the economic challenges posed by orphan drugs a comment on Drummond et al International Journal of Technology Assessment in Health Care 23 3 397 404 doi 10 1017 s0266462307071012 PMID 17579945 S2CID 29572982 Simoens Steven 2011 06 17 Pricing and reimbursement of orphan drugs the need for more transparency Orphanet Journal of Rare Diseases 6 1 42 doi 10 1186 1750 1172 6 42 PMC 3132155 PMID 21682893 Our charter Who we are About NICE Retrieved 2021 03 29 NICE calls for a new approach to managing the entry of drugs into the NHS Press release NICE 18 September 2014 Retrieved 29 June 2015 External links edit nbsp Look up orphan drug in Wiktionary the free dictionary nbsp Wikimedia Commons has media related to Orphan drugs Drug Information Association DIA EVENT DIA FDA Orphan Drug Designation Workshop November 2010 European Commission The Orphan drugs strategy List of European Orphan Drugs USA Food and Drug Administration The Orphan Drug Act as amended US FDA List of Orphan Designations and Approvals Retrieved from https en wikipedia org w index php title Orphan drug amp oldid 1177176464, wikipedia, wiki, book, books, library,

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