Design of a surrogate Anticalin protein directed against CD98hc for preclinical studies in mice

Friedrich Christian Deuschle; André Schiefner; Corinna Brandt; Arne Skerra

doi:10.1002/pro.3894

Design of a surrogate Anticalin protein directed against CD98hc for preclinical studies in mice

Friedrich Christian Deuschle, André Schiefner, Corinna Brandt, Arne Skerra

Chair of Biological Chemistry

Technical University of Munich

Research output: Contribution to journal › Article › peer-review

2 Scopus citations

Abstract

The human CD98 heavy chain (CD98hc) offers a promising biomedical target both for tumor therapy and for drug delivery to the brain. We have previously developed a cognate Anticalin protein with picomolar affinity and demonstrated its effectiveness in a xenograft animal model. Due to the lack of cross-reactivity with the murine ortholog, we now report the development and X-ray structural analysis of an Anticalin with high affinity toward CD98hc from mouse. This binding protein recognizes the same protruding epitope loop—despite distinct structure—in the membrane receptor ectodomain as the Anticalin selected against human CD98hc. Thus, this surrogate Anticalin should be useful for the preclinical assessment of CD98hc targeting in vivo and support the translational development for medical application in humans.

Original language	English
Pages (from-to)	1774-1783
Number of pages	10
Journal	Protein Science
Volume	29
Issue number	8
DOIs	https://doi.org/10.1002/pro.3894
State	Published - Aug 2020

Keywords

CD98hc
cancer theranostics
lipocalin
mouse model
protein engineering

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.1002/pro.3894

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title = "Design of a surrogate Anticalin protein directed against CD98hc for preclinical studies in mice",

abstract = "The human CD98 heavy chain (CD98hc) offers a promising biomedical target both for tumor therapy and for drug delivery to the brain. We have previously developed a cognate Anticalin protein with picomolar affinity and demonstrated its effectiveness in a xenograft animal model. Due to the lack of cross-reactivity with the murine ortholog, we now report the development and X-ray structural analysis of an Anticalin with high affinity toward CD98hc from mouse. This binding protein recognizes the same protruding epitope loop—despite distinct structure—in the membrane receptor ectodomain as the Anticalin selected against human CD98hc. Thus, this surrogate Anticalin should be useful for the preclinical assessment of CD98hc targeting in vivo and support the translational development for medical application in humans.",

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author = "Deuschle, {Friedrich Christian} and Andr{\'e} Schiefner and Corinna Brandt and Arne Skerra",

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AU - Deuschle, Friedrich Christian

AU - Schiefner, André

AU - Brandt, Corinna

AU - Skerra, Arne

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KW - mouse model

KW - protein engineering

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Design of a surrogate Anticalin protein directed against CD98hc for preclinical studies in mice

Abstract

Keywords

UN SDGs

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