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PET Imaging of GPR44 by Antagonist [11C]MK-7246 in Pigs.


ABSTRACT: A validated imaging marker for beta-cell mass would improve understanding of diabetes etiology and enable new strategies in therapy development. We previously identified the membrane-spanning protein GPR44 as highly expressed and specific to the beta cells of the pancreas. The selective GPR44 antagonist MK-7246 was radiolabeled with carbon-11 and the resulting positron-emission tomography (PET) tracer [11C]MK-7246 was evaluated in a pig model and in vitro cell lines. The [11C]MK-7246 compound demonstrated mainly hepatobiliary excretion with a clearly defined pancreas, no spillover from adjacent tissues, and pancreatic binding similar in magnitude to the previously evaluated GPR44 radioligand [11C]AZ12204657. The binding could be blocked by preadministration of nonradioactive MK-7246, indicating a receptor-binding mechanism. [11C]MK-7246 showed strong potential as a PET ligand candidate for visualization of beta-cell mass (BCM) and clinical translation of this methodology is ongoing.

SUBMITTER: Cheung P 

PROVIDER: S-EPMC8073488 | biostudies-literature | 2021 Apr

REPOSITORIES: biostudies-literature

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PET Imaging of GPR44 by Antagonist [<sup>11</sup>C]MK-7246 in Pigs.

Cheung Pierre P   Zhang Bo B   Puuvuori Emmi E   Estrada Sergio S   Amin Mohammad A MA   Ye Sofie S   Korsgren Olle O   Odell Luke R LR   Eriksson Jonas J   Eriksson Olof O  

Biomedicines 20210416 4


A validated imaging marker for beta-cell mass would improve understanding of diabetes etiology and enable new strategies in therapy development. We previously identified the membrane-spanning protein GPR44 as highly expressed and specific to the beta cells of the pancreas. The selective GPR44 antagonist MK-7246 was radiolabeled with carbon-11 and the resulting positron-emission tomography (PET) tracer [<sup>11</sup>C]MK-7246 was evaluated in a pig model and in vitro cell lines. The [<sup>11</sup  ...[more]

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