First-in-human study with new recombinant agalsidase beta (ISU303) in healthy subjects.

[fabry disease]

ISU 303 is a new recombinant agalsidase beta (Agal ) enzyme replacement therapy under investigation for Fabry disease , caused by a deficiency in α-galactosidase A activity that leads to fatty deposits in tissues . We evaluated the pharmacokinetic (PK ) parameters , safety and tolerability of ISU 303 in healthy adult volunteers . The study was a dose block-randomized , double -blinded , placebo-controlled , single -dosing , and dose escalation phase 1 clinical trial . A total of 18 healthy subjects were enrolled (0 .3 mg /kg , n = 6 ; 1 .0 mg /kg , n = 6 ; placebo , n = 6 ). Blood samples for PK analysis were collected according to planned time . The PK parameters in each 0 .3 and 1 .0 mg /kg Agal group were as follows : Cmax (mU /mL ) 43 .19 ± 5 .9 and 195 .86 ± 32 .3 ; AUClast (h ·mU /mL ) 207 .91 ± 25 .1 and 939 .96 ± 158 .3 ; t 1 /2 (hours ) 1 .13 ± 0 .3 and 1 .46 ± 0 .2 ; Cl (mL /min /kg ) 1 .79 ± 0 .2 and 1 .34 ± 0 .2 , respectively . There were seven adverse events (AE ) overall . All AEs were resolved without any complications . None were related to the study drug . There were no immunogenicity or any significant infusion-related reactions . The new Agal product exhibited a dose-dependent PK and was well tolerated with no significant AEs in healthy adult volunteers .