Delving into the Latest Updates on GSK-3128349 with Synapse

Overview

Basic Info

Drug Type

Radiolabeled antibody, Diagnostic radiopharmaceuticals

Synonyms

89Zr-AlbudAb™, 89Zr-labeled albumin-binding domain antibody, GSK-3128349

Target

albumin

Action

modulators

Mechanism

albumin modulators(Serum albumin modulators)

Therapeutic Areas-

Active Indication-

Inactive Indication-

Originator Organization

GSK Plc

Active Organization-

Inactive Organization

GSK Plc

License Organization-

Drug Highest PhasePendingPhase 1

First Approval Date-

Regulation-

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Structure/Sequence

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An open label positron emission tomography (PET) imaging study using 89-Zirconium labelled GSK3128349 to investigate the biodistribution and clearance of an albumin binding domain<br>antibody (AlbudAb) GSK3128349 following single dose intravenous administration in healthy male subjects. - AlbudAb PET study.

Start Date23 Aug 2016

Sponsor / Collaborator

GlaxoSmithKline Research & Development Ltd.

NCT02829307

/ CompletedPhase 1

An Open Label Positron Emission Tomography (PET) Imaging Study Using 89Zirconium Labeled GSK3128349 to Investigate the Biodistribution and Clearance of an Albumin Binding Domain Antibody (AlbudAb) GSK3128349 Following Single Dose Intravenous Administration in Healthy Male Subjects

GSK3128349 is a small protein molecule (biopharmaceutical) that binds to albumin in the body, and by itself, has no pharmacological action. A pharmacologically active drug can be attached to GSK3128349 with the goal of changing the distribution and/or duration of action of the attached drug. This study will determine the distribution and pharmacokinetics (duration) of GSK3128349 itself after a single intravenous infusion. GSK3128349 has been labeled with and the radioisotope 89Zirconium allowing it to be visualized in the organs of the body using a PET scanner at multiple time points after GSK3128349 dosing. The data from this study will help predict the distribution of future drugs attached to GSK3128349. The total duration of a subject's participation is about approximately 10 weeks, including the screening period.

Start Date23 Aug 2016

Sponsor / Collaborator

GSK Plc

[+1]

100 Clinical Results associated with GSK-3128349

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100 Translational Medicine associated with GSK-3128349

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100 Patents (Medical) associated with GSK-3128349

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2

Literatures (Medical) associated with GSK-3128349

01 Jan 2020·mAbsQ2 · MEDICINE

Cross-species/cross-modality physiologically based pharmacokinetics for biologics: 89Zr-labelled albumin-binding domain antibody GSK3128349 in humans

Q2 · MEDICINE

Article

Author: Sepp, Armin ; Davies, Marie ; Bergström, Mats

Two-pore physiologically-based pharmacokinetics (PBPK) for biologics describes the tissue distribution and elimination kinetics of soluble proteins as a function of their hydrodynamic radius and the physiological properties of the organs. Whilst many studies have been performed in rodents to parameterize the PBPK framework in terms of organ-specific lymph flow rates, similar validation in humans has been limited. This is mainly due to the paucity of the tissue distribution time course data for biologics that is not distorted by target-related binding. Here, we demonstrate that a PBPK model based on rodent data provided good to satisfactory extrapolation to the tissue distribution time course of ⁸⁹Zr-labeled albumin-binding domain antibody (AlbudAb™) GSK3128349 in healthy human volunteers, including correct prediction of albumin-like plasma half-life, volume of distribution, and extravasation half-life. The AlbudAb™ used only binds albumin, and hence it also provides information about the tissue distribution kinetics and turnover of that ubiquitous and multifunctional plasma protein.

01 Dec 2019·EJNMMI Research

The biodistribution and clearance of AlbudAb, a novel biopharmaceutical medicine platform, assessed via PET imaging in humans

Article

Author: Cleveland, Matthew ; Bergstrom, Mats ; Vincent, Veena ; Vugts, Danielle J ; Szapacs, Matt ; van Dongen, Guus ; Zhang, Sean ; Thorneloe, Kevin S ; Elsinga, Phillip ; Galette, Paul ; Wiegers, Johan ; Birchler, Mary ; Sepp, Armin ; Galinanes-Garcia, Laura ; Renaux, Jessica ; Glaudemans, Andor W J M ; Al-Azzam, Wasfi ; Davies, Marie

METHODS:

A non-conjugated AlbudAb (GSK3128349) was radiolabeled with ⁸⁹Zr and a single 1 mg (~ 15 MBq) dose intravenously administered to eight healthy males. ⁸⁹Zr-AlbudAb tissue distribution was followed for up to 7 days with four whole-body PET/CT scans. ⁸⁹Zr-AlbudAb tissue concentrations were quantified in organs of therapeutic significance, measuring standardized uptake value and tissue/plasma ratios. Plasma pharmacokinetics were assessed by gamma counting and LC-MS/MS of blood samples.

RESULTS:

⁸⁹Zr-AlbudAb administration and PET/CT procedures were well tolerated, with no drug-related immunogenicity or adverse events. ⁸⁹Zr-AlbudAb rapidly distributed throughout the vasculature, with tissue/plasma ratios in the liver, lungs, and heart relatively stable over 7 days post-dose, ranging between 0.1 and 0.5. The brain tissue/plasma ratio of 0.025 suggested minimal AlbudAb blood-brain barrier penetration. Slowly increasing ratios in muscle, testis, pancreas, and spleen reflected either slow AlbudAb penetration and/or ⁸⁹Zr residualization in these organs. Across all tissues evaluated, the kidney tissue/plasma ratio was highest (0.5-1.5 range) with highest concentration in the renal cortex. The terminal half-life of the ⁸⁹Zr-AlbudAb was 18 days.

CONCLUSION:

Evaluating the biodistribution of ⁸⁹Zr-AlbudAb in healthy volunteers using a low radioactivity dose was successful (total subject exposure ~ 10 mSv). Results indicated rapid formation of reversible, but stable, complexes between AlbudAb and albumin upon dosing. ⁸⁹Zr-AlbudAb demonstrated albumin-like pharmacokinetics, including limited renal elimination. This novel organ-specific distribution data for AlbudAbs in humans will facilitate a better selection of drug targets to prosecute using the AlbudAb platform and significantly contribute to modeling work optimizing dosing of therapeutic AlbudAbs in the clinic.

100 Deals associated with GSK-3128349

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R&D Status

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Clinical Result

Indication

Phase

Evaluation

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Study	Phase	Population	Analyzed Enrollment	Group	Results	Evaluation	Publication Date


NCT02829307 (CTgov)	Phase 1	Drug-Related Side Effects and Adverse Reactions	8	89Zr-GSK3128349 1 mg	ikojmyavrp(ctvitsloox) = omksaqygse cpxmbnfnpn (ahvlsqzcyu, 0.1387) View more	-	07 Sep 2018
EANM2017	Not Applicable	-	8	AlbudAb™ GSK3128349	gfravejjqz(fbyoelhcav) = hefzfvldct ttihxntmtq (wavczzkvst )	-	11 Sep 2017

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Translational Medicine

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Clinical Trial

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Approval

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Biosimilar

Competitive landscape of biosimilars in different countries/locations. Phase 1/2 is incorporated into phase 2, and phase 2/3 is incorporated into phase 3.

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