Wednesday, February 10, 2010

FDA meeting on pirfenidone
FDA Advisory Committee is meeeting on March 9 2010 to consider approval of pirfenidone for the treatment of pulmonary fibrosis. I am submitting the following opinion to FDA to be considered at this meeting:

My Experience with Idiopathic Pulmonary Fibrosis (IPF)

I am a retired MD pharmacologist and for the last 9 years an IPF patient.

As a patient I experienced an unusually slow progression of the disease: a gradual suffocation leading to a loss of my ability to run, climb stairs and now even walk without oxygen. Attacks of a severe unproductive cough have made the life particularly miserable. I am a patient at Yale pulmonary clinic but the best pulmonary physicians cannot cure me. I am not eligible for lung transplantation and my therapy consists only of oxygen, since there are no drugs capable of alleviating my suffering. In the clinic I am having annual pulmonary function tests to document a gradual decline in most parameters. There is also a support group of patients with IPF to share experiences. I am learning that some of the patients are in worse shape than I am. They are in wheelchairs and can no longer dress or take a shower without the help of a caregiver. I can see myself in a similar situation in the near future.

As a scientist I am deeply disturbed by our failure to recognize the medical need and to develop drugs for the treatment of IPF. Very little research is ongoing in this field at either academic institutions or the pharmaceutical industry. I spent a good portion of the last year researching IPF and the approaches to its therapy. My research culminated in an extensive review article published last December (Scriabine A and Rabin D.U.. New developments in the therapy of pulmonary fibrosis. In: Contemporary aspects of biomedical research: drug discovery. Enna S.J. and Williams, M. Eds. Academic Press 2009; 419-464). Targets for antifibrotic drugs have been proposed and models of fibrotic diseases are available, but only pirfenidone offers some hope for IPF patients in the near future. IPF is probably not a single disease, but a group of pulmonary diseases with similar pathology, but different etiology. If so, one drug is not likely to help every patient diagnosed with IPF and clinical trials will not demonstrate uniform efficacy in a heterogeneous population. Under these circumstances safety should be the major consideration for drug approval.

Alexander Scriabine, MD
ascriabine@comcast.net
435 Colonial Road
Guilford, CT 06437