DOI: 10.1182/blood.v73.7.1842.1842. Pharmacokinetic and distribution analysis of variant forms of tissue- type plasminogen activator with prolonged clearance in rat

Pharmacokinetic and distribution analysis of variant forms of tissue- type plasminogen activator with prolonged clearance in rat

10.1182/blood.v73.7.1842.1842

Crossref journal-article

American Society of Hematology

Blood (234)

Abstract

Abstract Human tissue-type plasminogen activator (t-PA) is a glycoprotein used currently in thrombolytic therapy. Because of its rapid half-life (T1/2) of approximately five minutes, intravenous (IV) infusion of large doses (approximately 100 mg) are required in patients treated for myocardial infarction. To identify the determinant(s) on t-PA responsible for such rapid clearance, metabolically labeled forms of recombinant t-PA were analyzed in rats following IV administration. The following seven forms of t-PA were tested: (a) natural or glycosylated wild-type t-PA; (b) nonglycosylated wild-type t-PA; (c) delta F t-PA, which lacks the fibronectin fingerlike domain; (d) delta E t-PA, which lacks the epidermal growth factor (EGF) domain; (e) delta FE t-PA, which lacks both the finger and EGF domains; (f) delta FE3X t-PA, a form of delta FE t-PA in which Asn-linked glycosylation is prevented at all known glycosylation sites (Asn-117, 184, and 448; replaced by Gln); and (f) delta FE1X t-PA, a form of delta FE t-PA in which high-mannose- type glycosylation is prevented at Asn-117. Both glycosylated and nonglycosylated wild-type t-PA cleared in an exponential biphasic manner, with an initial alpha-phase T1/2 of 0.8 and 1.9 minutes, respectively. This result demonstrates that carbohydrate is not the primary mediator of the rapid clearance of t-PA. The liver was the primary organ responsible for uptake of these molecules. All other proteins tested, except for delta E t-PA, demonstrated primarily monophasic clearance patterns with T1/2 ranging between 12 and 27 minutes, and reduced uptake in the liver. delta E t-PA however, cleared in a biphasic manner with an alpha-phase T1/2 of 2.1 minutes. Results presented suggest that the clearance of t-PA is mediated by two distinct mechanisms. The primary determinant(s) responsible for modulating the rapid clearance of t-PA appears to be resident within the polypeptide sequence encoding the finger and/or EGF domains, with emphasis on the finger domain. A second and less significant contribution to clearance is defined by the presence and type of glycosylation.

Bibliography

Larsen, G., Metzger, M., Henson, K., Blue, Y., & Horgan, P. (1989). Pharmacokinetic and distribution analysis of variant forms of tissue- type plasminogen activator with prolonged clearance in rat. Blood, 73(7), 1842â1850.

Authors 5

GR Larsen (first)
M Metzger (additional)
K Henson (additional)
Y Blue (additional)
P Horgan (additional)

References 0 Referenced 47

None

Dates

Type	When
Created	5 years, 10 months ago (Oct. 13, 2019, 5:22 a.m.)
Deposited	5 years, 9 months ago (Nov. 19, 2019, 4:40 p.m.)
Indexed	2 months, 1 week ago (June 26, 2025, 6:09 a.m.)
Issued	36 years, 3 months ago (May 15, 1989)
Published	36 years, 3 months ago (May 15, 1989)
Published Print	36 years, 3 months ago (May 15, 1989)

Funders 0

None

BibTeX

@article{Larsen_1989, title={Pharmacokinetic and distribution analysis of variant forms of tissue- type plasminogen activator with prolonged clearance in rat}, volume={73}, ISSN={1528-0020}, url={http://dx.doi.org/10.1182/blood.v73.7.1842.1842}, DOI={10.1182/blood.v73.7.1842.1842}, number={7}, journal={Blood}, publisher={American Society of Hematology}, author={Larsen, GR and Metzger, M and Henson, K and Blue, Y and Horgan, P}, year={1989}, month=may, pages={1842–1850} }

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