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	<title>drug seeking &#8211; schmidtlab.org</title>
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		<title>Administration of a Novel High Affinity PICK1 PDZ Domain Inhibitor Attenuates Cocaine Seeking in Rats</title>
		<link>https://schmidtlab.org/2020/03/31/administration-of-a-novel-high-affinity-pick1-pdz-domain-inhibitor-attenuates-cocaine-seeking-in-rats/</link>
		
		<dc:creator><![CDATA[suditir]]></dc:creator>
		<pubDate>Tue, 31 Mar 2020 18:08:04 +0000</pubDate>
				<category><![CDATA[Publications & News]]></category>
		<category><![CDATA[Published Studies]]></category>
		<category><![CDATA[cocaine]]></category>
		<category><![CDATA[drug seeking]]></category>
		<category><![CDATA[pick1]]></category>
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					<description><![CDATA[Schmidt Lab alumni Christopher Turner, Jordan Wolfheimer, and Dr. Nicole Hernandez, in collaboration with Drs. De Luca and Madsen of the University of Copenhagen, recently published a paper in Neuropharmacology . Find the abstract below: Protein interacting with C kinase-1 &#8230; <a class="kt-excerpt-readmore more-link" href="https://schmidtlab.org/2020/03/31/administration-of-a-novel-high-affinity-pick1-pdz-domain-inhibitor-attenuates-cocaine-seeking-in-rats/">Read More</a>]]></description>
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<p class="wp-block-paragraph">Schmidt Lab alumni Christopher Turner, Jordan Wolfheimer, and Dr. Nicole Hernandez, in collaboration with Drs. De Luca and Madsen of the University of Copenhagen, recently published a paper in Neuropharmacology . Find the <a href="https://pubmed.ncbi.nlm.nih.gov/31805281/?from_term=Madsen+KL&amp;from_cauthor_id=31805281&amp;from_pos=1">abstract</a> below:</p>



<blockquote class="wp-block-quote is-layout-flow wp-block-quote-is-layout-flow"><p>Protein interacting with C kinase-1 (PICK1) regulates intra-cellular trafficking of GluA2-containing AMPA receptors, a process known to play a critical role in cocaine-seeking behavior. This suggests that PICK1 may represent a molecular target for developing novel pharmacotherapies to treat cocaine craving-induced relapse. Emerging evidence indicates that inhibition of PICK1 attenuates the reinstatement of cocaine-seeking behavior, an animal model of relapse. Here, we show that systemic administration of TAT-P<sub>4</sub>-(DATC5)<sub>2</sub>, a novel high-affinity peptide inhibitor of the PICK1 PDZ domain, dose-dependently attenuated the reinstatement of cocaine seeking in rats at doses that did not produce operant learning deficits or suppress locomotor activity. We also show that systemic TAT-P<sub>4</sub>-(DATC5)<sub>2</sub>&nbsp;penetrated the brain where it was visualized in the nucleus accumbens shell. Consistent with these effects, infusions of TAT-P<sub>4</sub>-(DATC5)<sub>2</sub>&nbsp;directly into the accumbens shell reduced cocaine, but not sucrose, seeking. The effects of TAT-P<sub>4</sub>-(DATC5)<sub>2</sub>&nbsp;on cocaine seeking are likely due, in part, to inhibition of PICK1 in medium spiny neurons (MSNs) of the accumbens shell as TAT-P<sub>4</sub>-(DATC5)<sub>2</sub>&nbsp;was shown to accumulate in striatal neurons and bind PICK1. Taken together, these findings highlight a novel role for PICK1 in the reinstatement of cocaine seeking and support future studies examining the efficacy of peptide inhibitors of PICK1 in animal and human models of cocaine relapse.</p></blockquote>



<p class="wp-block-paragraph">Congratulations! </p>
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