Drugs for a developing world

Diseases affecting the developing world have long been neglected, but new partnerships between governments, charities and pharmaceutical firms could change that, says Sarah Houlton

Many of the diseases that kill the most people disproportionately affect the developing world. Whether they are familiar, such as malaria, HIV/Aids and TB (tuberculosis), or neglected diseases like leishmaniasis and sleeping sickness, there is little incentive for big pharma companies to develop drugs as those affected simply do not have the resources to pay for them. As a result, much of the drug discovery effort is funded by philanthropic organisations such as the Wellcome Trust, the Bill & Melinda Gates Foundation and the Medicines for Malaria Venture. However, pharma companies remain the best able to bring a drug through from biological target to marketed compound. Several companies are now working in partnership with these organisations, and some have set up research sites within countries affected by these diseases.

Novartis, for example, established the Novartis Institute for Tropical Diseases (NITD) in Singapore as a public-private partnership with the country’s Economic Development Board in 2002. Initially its focus was on TB and dengue, and later on malaria was added. But why Singapore? ’Important criteria when deciding where to put a research centre include accessing talent and basic science, academic infrastructure, the legal environment and intellectual property protection,’ explains Paul Herrling, the company’s head of corporate research. ’But if you want to make medicines for patients, you need to know their environment - and these diseases don’t occur in Basel or Cambridge. We felt that if we were going to work on diseases prevalent in the tropics, we should put the research as close to them as possible, and Singapore fits the bill.’

The Institute is a fully integrated research centre, with chemistry, biology and molecular biology, and access to the company’s know-how and technology elsewhere in the world. When it was being set up, the Singapore government was trying to attract biomedical science companies - the country had the research infrastructure for basic sciences, but they wanted to be able to translate it into products. ’They wanted to create biomedical science infrastructure so they could learn from it,’ Herrling says. 

The NITD has also attracted funding from other agencies and charities, such as the Bill & Melinda Gates Foundation. ’Their goal was to foster the creation of new medicines for TB because of resistance, and for dengue as there have never been any,’ he says. The Wellcome Trust then asked them to work on malaria, too, and ultimately provided $20 million (?12.2 million) to run the programme, which began 18 months ago. ’We had not selected malaria initially because we already had Coartem [the artemesinin-based combination therapy] - but resistance was starting to appear, and as drug discovery takes 10 to 15 years we needed to start straight away.’ 

For TB, they are now in the early stage of preclinical development - selecting targets and scaffolds. ’We don’t even start any development if the compounds don’t work on all the resistant strains,’ Herrling says. Things are a little further advanced in dengue, with several projects now in the late stage of preclinical development. ’We found one compound which killed the virus in animal models and still works several days after infection, but the side-effects were prohibitive,’ he adds. ’If we can find one that does not affect the host too much, we should be up and running.’

He believes they made the right choice by setting up the NITD in Singapore. ’We assumed it would be easy to recruit brilliant scientists to work there, and we were right,’ he says. ’We have about 100 people from 24 nations, and about half of them are locals. And the scientific environment is great - we have many very good collaborations with academic institutions and hospitals which gives us access to patients.’

Drug discovery culture   

AstraZeneca also has a research site in the developing world - in Bangalore, India. It was originally an Astra site working on tropical diseases, and after the Astra-Zeneca merger in 2000, they decided to focus on tuberculosis. ’We’ve got about a quarter of the world’s population of TB patients in India, and we really should do something about it,’ says the site’s head of R&D, Balganesh Tanjore. ’We looked at the unmet medical need globally, our own infrastructure and expertise, and we had been working in both malaria and tuberculosis as well as parasitic disease, but in 2000 the entire genome sequence of Mycobacterium tuberculosis  became available, and that of the malaria parasite was still in its infancy. We looked at this as a clear and breaking science, and that made the decision for us.’ 

India has many advantages for research, he says. ’There is a lot of competence in the scientific base, people are coming back to India because they believe there are now opportunities for them there, the universities are globally competitive, the cost of research is cheaper and, perhaps most importantly, there is access to clinical materials. But it’s not just because it’s cheaper - building a culture of drug discovery takes time.’ 

Like the Novartis operation in Singapore, the site can carry out the entire drug discovery process from target identification through to candidate drug, and has access to other AstraZeneca technology such as the central screening facility. ’Our mandate was to have something in the clinic for safety trials by 2010, and we believe we’re on schedule,’ Tanjore says. ’We have a lead compound in early safety work; it is a new protein synthesis inhibitor which works on drug resistant TB, is orally bioavailable and is compatible with HIV treatment. So it meets the basic requirements we believe are critical for getting a drug into the patient, and we hope it will immediately bring some sort of relief for multi-drug resistant patients.’ There is another project in lead optimisation, and he hopes that in the next two years at least two programmes will be in this optimisation stage at any one time.  

Therapeutics for a rainbow nation   

South Africa is another country with great unmet medical need and a good science base. This was the rationale behind the decision of a group of chemistry academics - Tony Barrett from Imperial College London, UK, and Steve Ley from the University of Cambridge, UK, and Dennis Liotta from Emory University in Atlanta, Georgia, US - plus George Painter from US anti-viral drug company Chimerix, to set up a start-up company, iThemba Pharmaceuticals, in Johannesburg. As Julian Walsh, director of external affairs for the chemical biology centre at Imperial College and another of the founders, explains, Barrett had started consultancy work in South Africa and had come back impressed at the quality of the people the universities were turning out, and the whole spirit of change in the country.  

’The initial idea had been to set up a scholarship scheme, but the penny dropped that even if a fantastic scholarship system could be set up, there would be nothing for these people to come back to, at least from the point of view of medicinal chemistry - most decent chemists who stay in chemistry end up working in the oil industry,’ he says. ’South Africa’s pharma industry was essentially a pills and powders operation. Yet there are huge and growing health needs, particularly because of AIDS, but there was no research-based biotech emerging so the best of the talent was likely to leave the country. We had a Damascene conversion at Cape Town airport over some good wine, and realised that the biggest contribution we could make to South Africa was to found a research-based company.’ 

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