GM-CSF was first cloned in 1985, and soon afterwards three potential drug products were being made using
recombinant DNA technology:
molgramostim was made in
Escherichia coli and is not glycosylated,
sargramostim was made in yeast, has a leucine instead of proline at position 23 and is somewhat glycosylated, and
regramostim was made in Chinese hamster ovary cells (CHO) and has more glycosylation than sargramostim. The amount of glycosylation affects how the body interacts with the drug and how the drug interacts with the body. At that time,
Genetics Institute, Inc. was working on molgramostim,
Immunex was working on
sargramostim (Leukine), and
Sandoz was working on regramostim. Molgramostim was eventually co-developed and co-marketed by Novartis and Schering-Plough under the trade name Leucomax for use in helping white blood cell levels recover following chemotherapy, and in 2002 Novartis sold its rights to Schering-Plough. Sargramostim was approved by the US FDA in 1991 to accelerate white blood cell recovery following autologous
bone marrow transplantation under the trade name Leukine, and passed through several hands, ending up with
Genzyme, which was subsequently acquired by
Sanofi. Leukine is now owned by Partner Therapeutics (PTx). Imlygic was approved by the US FDA in October 2015, and in December 2015 by the EMA, as an oncolytic virotherapy, commercialized by Amgen Inc. This
oncolytic herpes virus, named
Talimogene laherparepvec, has been genetically engineered to express human GM-CSF using the tumor cells machinery. ==Clinical significance==