To the Editor

I read with interest your December editorial1 concerning international nonproprietary name (INN) rules for the naming of biosimilars and agree with the opinions expressed, especially the last paragraph. I believe the pressure exerted by the Biotechnology Industry Organization (BIO; Washington, DC) and some manufacturers of the original biological therapeutics to promote separate INN naming for biosimilars by the World Health Organization (WHO; Geneva) is part of a strategy to frame biosimilars as different and inferior.

For decades, industry has been producing different, original biological products with different labeling but the same INN: examples include interferon beta 1a and somatotropin. This was apparently never a problem for BIO or manufacturers, so why is it now an issue with biosimilars?

BIO exaggerates the impact of INN naming on the traceability of biosimilar treatment in the case of safety incidents. This is exemplified in the antibody-associated pure red cell aplasia (PRCA) cases occurring after a formulation change of an epoetin product and first reported in 2002. In the cohort of >60 PRCA patients described by Nicole Casadevall, who discovered this side effect, only three received this epoetin only, complicating the linking of the safety issue to the specific product. Relying on INN alone also makes it impossible to identify the relatively common batch-dependent safety issues. Registering the batch given to individual patients is far more logical and is also made relatively easy using the bar codes present on the product packages.

I agree with the editorial that the introduction of biosimilar INN naming implies that originator products should likewise be renamed after major manufacturing changes. In 2011, in this journal, Scheistl et al.2 showed major differences introduced by such changes, exceeding the differences accepted between reference product and biosimilar. None of these changes were mentioned in the product information, and physicians were therefore unaware that they were treating patients with a different product.

There are also some practical problems to solve before the INN system can be applied to biosimilars. It is a passive system, and an INN is only issued by the WHO on request. Transforming this into a mandatory and enforceable system will be virtually impossible. Also, an INN can only be given to a defined chemical structure, whereas biologicals are nearly always mixtures of naturally occurring or process-induced variants. For example, both epoetin alfa and epoetin beta are mixtures of five or six naturally occurring major glycoforms with significant differences in glycan structure. The alfa or beta suffix in the INN designates a defined glycan structure. But the INN of the epoetins has never been attached to a specific glycoform.

The apartheid regime for biosimilars advocated by BIO is only part of its policy to defame these products as inferior and to block their market introduction. Developing countries are currently an important target for BIO, where affordable biosimilars are the only means for most patients to be treated with biologics. Therefore, governments in countries like Colombia are introducing legislation carefully designed to allow safe and effective biosimilars while avoiding having regulatory standards impede accessibility. BIO is lobbying fiercely up to the highest political levels for biosimilar guidelines in developing countries that would make the marketing of many highly needed biosimilars impossible. Your editorial is an important signal for governments and regulators and confirms your journal as the voice of reason in a biotech field increasingly dominated by pseudoscience and marketing slogans.