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Abstract #4472

Superior HyperCEST Performance of Membrane-Anchored Xenon Hosts in Nanocarriers with Variable Membrane Fluidity

Leif Schröder1,2,3, Felix Schnabel1, and Jabadurai Jayapaul1
1Translational Molecular Imaging, German Cancer Research Center, Heidelberg, Germany, 2Department for Physics and Astronomy, Ruprecht Karls University Heidelberg, Heidelberg, Germany, 3German Cancer Consortium (DKTK), Heidelberg, Germany

Synopsis

Keywords: Contrast Agents, Contrast Agent

Motivation: The efficiency of CEST agents for hyperpolarized 129Xe depends on the exchange rate of Xe in/out of tailored host structures. For liposomal designs, this may be influenced by the phospholipid membrane fluidity.

Goal(s): This study investigates how cholesterol, which is often added for liposome stability, impacts the HyperCEST performance.

Approach: We compared the changes in CEST buildup from liposomes with variable cholesterol content and either membrane-anchored (i.e., lipopeptide-based) or freely diffusing Xe host.

Results: The HyperCEST efficiency for membrane-anchored Xe hosts is much less sensitive to membrane stiffening than for unbound hosts. Lipopeptide-based HyperCEST agents are thus a powerful approach for biosensor design.

Impact: The HyperCEST performance of membrane-anchored xenon hosts in liposomal nanocarriers shows reduced susceptibility to membrane stiffening compared to non-functionalized hosts. These less susceptible lipopeptide-based hosts are thus the preferred approach for future in vivo applications.

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