Aggregation of human plasma and of human blood induced in vitro by filgrastim originator product; effect of PEGylation

Tudor Arvinte; Emilie Poirier; Amelia Cudd; Nuri Ersayin; Guillaume Darpin; Jason Dowd; Stephen Brokx

doi:10.1016/j.ejpb.2023.12.004

Aggregation of human plasma and of human blood induced in vitro by filgrastim originator product; effect of PEGylation

Eur J Pharm Biopharm. 2024 Jan:194:148-158. doi: 10.1016/j.ejpb.2023.12.004. Epub 2023 Dec 12.

Authors

Tudor Arvinte¹, Emilie Poirier², Amelia Cudd², Nuri Ersayin², Guillaume Darpin², Jason Dowd³, Stephen Brokx³

Affiliations

¹ Therapeomic Inc., Basel, Switzerland. Electronic address: tudor.arvinte@therapeomic.com.
² Therapeomic Inc., Basel, Switzerland.
³ Apobiologix, Toronto, Ontario, Canada.

PMID: 38097022
DOI: 10.1016/j.ejpb.2023.12.004

Abstract

We herein report that filgrastim product Neupogen® and the filgrastim formulation buffer induced aggregate formation when mixed in vitro with human plasma, and formation of large membranous erythrocyte aggregates when mixed with human blood, similar to the aggregation induced by pegfilgrastim and by pegfilgrastim buffer [T. Arvinte, E. Poirier, N. Ersayin, G. Darpin, A. Cudd, J. Dowd, S. Brokx, Aggregation of human plasma and of human blood induced in vitro by pegfilgrastim originator formulation buffer and pegfilgrastim products, Eur. J. Pharmaceut. Biopharmaceut. (2023), doi: 10.1016/j.ejpb.2023.10.019]. The data identify the filgrastim buffer (which is practically the same in filgrastim and pegfilgrastim products) as the main driver of human plasma and blood aggregation. Kinetic experiments showed differences in the extent of plasma aggregation induced by a filgrastim product manufactured in EU and one manufactured in USA. Human donor variability in the plasma aggregation induced by filgrastim was observed. To study the effect of PEGylation of the filgrastim protein on plasma aggregation we compared filgrastim (Neupogen®) with pegfilgrastim (Neulasta®) solutions at the same protein concentration. These data show that PEGylation has a beneficial effect in inhibiting to an extent plasma aggregation. Interestingly, 20 kDa polyethylene glycol in the filgrastim buffer induced more plasma aggregation compared to the buffer, similar to the aggregation induced by pegfilgrastim. For intravenous infusion filgrastim solutions (300 µg/ml, vials only) may be diluted in 5 % dextrose from a concentration of 300 µg/ml to 5 µg/ml. Aggregation of human plasma was also induced by filgrastim solutions diluted in 5 % dextrose to 50 µg/ml, 15 µg/ml and 5 µg/ml filgrastim, as well as by the filgrastim buffer similarly diluted in 5 % dextrose (1:6, 1:20 and 1:60 dilution). These data show that filgrastim solutions used for intravenous administration in patients induce human plasma aggregation in vitro. Such aggregation phenomena may be related to known infusion side effects of filgrastim therapy.

Keywords: Aggregation; Blood; Erythrocyte; Filgrastim; Kinetics; Lipoprotein; Microscope imaging; PEGylation; Plasma.

MeSH terms

Filgrastim
Glucose
Granulocyte Colony-Stimulating Factor*
Humans
Injections
Polyethylene Glycols*
Recombinant Proteins

Substances

Filgrastim
Granulocyte Colony-Stimulating Factor
Polyethylene Glycols
Glucose
Recombinant Proteins