Sustained effects of repeated levodopa (L-DOPA) administration on reward circuitry, effort-based motivation, and anhedonia in depressed patients with higher inflammation

Sustained effects of repeated levodopa (L-DOPA) administration on reward circuitry, effort-based motivation, and anhedonia in depressed patients with higher inflammation

•Higher CRP has been associated with lower reward circuit FC and anhedonia in MDD.•Evidence shows these relationships may be due to inflammation effects on dopamine.•L-DOPA increased VS-vmPFC FC in MDD with CRP > 2 but not ≤ 2 mg/L in our prior work.•Herein, MDD with CRP > 2 mg/L received repe...

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Hauptverfasser: Mandakh, Bekhbat, Zhihao, Li, Dunlop, Boadie W., Treadway, Michael T., Mehta, Neeti D., Revill, Kate P., Lucido, Michael J., Changdo, Hong, Andrea, Ashchi, Wommack, Evanthia C., Goldsmith, David R., Ebrahim, Haroon, Miller, Andrew H., Felger, Jennifer C.
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Anhedonia
C-reactive protein
Depression
Dopamine
Functional connectivity
Inflammation
Motivation
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container_title Brain, behavior, and immunity
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creator Mandakh, Bekhbat
Zhihao, Li
Dunlop, Boadie W.
Treadway, Michael T.
Mehta, Neeti D.
Revill, Kate P.
Lucido, Michael J.
Changdo, Hong
Andrea, Ashchi
Wommack, Evanthia C.
Goldsmith, David R.
Ebrahim, Haroon
Miller, Andrew H.
Felger, Jennifer C.
description •Higher CRP has been associated with lower reward circuit FC and anhedonia in MDD.•Evidence shows these relationships may be due to inflammation effects on dopamine.•L-DOPA increased VS-vmPFC FC in MDD with CRP > 2 but not ≤ 2 mg/L in our prior work.•Herein, MDD with CRP > 2 mg/L received repeated L-DOPA (150–450 mg/day/week) and placebo.•L-DOPA caused sustained improvements in VS-vmPFC FC and effort-based motivation. Inflammatory biomarkers like C-reactive protein (CRP) are elevated in a subset of patients with depression and associated with lower functional connectivity (FC) in a ventral striatum (VS) to ventromedial prefrontal cortex (vmPFC) reward circuit and symptoms of anhedonia. Evidence linking these relationships to the effects of inflammation on dopamine is consistent with our recent findings that acute levodopa (L-DOPA) increased VS-vmPFC FC in association with deceased anhedonia in depressed patients with higher but not lower CRP (>2 versus ≤ 2 mg/L). To determine whether repeated L-DOPA administration caused sustained effects on FC and behavior in these patients, medically stable depressed outpatients with CRP > 2 mg/L and anhedonia (n = 18) received one week of three doses of L-DOPA (150–450 mg/day/week with carbidopa) or placebo in a randomized order. Resting-state (rs) and task-based (tb; monetary incentive delay) fMRI, effort-based motivation, and exploratory measures of anhedonia and depression severity were assessed at baseline and after one week of placebo and each dose of L-DOPA. Responses to individual doses of L-DOPA varied across outcomes. For example, VS-vmPFC rs-FC was significantly increased by L-DOPA at 150 and 450 mg/day/week (p 
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Inflammatory biomarkers like C-reactive protein (CRP) are elevated in a subset of patients with depression and associated with lower functional connectivity (FC) in a ventral striatum (VS) to ventromedial prefrontal cortex (vmPFC) reward circuit and symptoms of anhedonia. Evidence linking these relationships to the effects of inflammation on dopamine is consistent with our recent findings that acute levodopa (L-DOPA) increased VS-vmPFC FC in association with deceased anhedonia in depressed patients with higher but not lower CRP (&gt;2 versus ≤ 2 mg/L). To determine whether repeated L-DOPA administration caused sustained effects on FC and behavior in these patients, medically stable depressed outpatients with CRP &gt; 2 mg/L and anhedonia (n = 18) received one week of three doses of L-DOPA (150–450 mg/day/week with carbidopa) or placebo in a randomized order. Resting-state (rs) and task-based (tb; monetary incentive delay) fMRI, effort-based motivation, and exploratory measures of anhedonia and depression severity were assessed at baseline and after one week of placebo and each dose of L-DOPA. Responses to individual doses of L-DOPA varied across outcomes. For example, VS-vmPFC rs-FC was significantly increased by L-DOPA at 150 and 450 mg/day/week (p &lt; 0.01), whereby approximately half of patients responded optimally to 150 mg/day L-DOPA and approximately half required higher doses for maximum effect. While effort-based motivation was only significantly increased by L-DOPA at 150 mg/day (p &lt; 0.05), it correlated with VS-vmPFC rs-FC at this dose (r = 0.64, p = 0.024), and all L-DOPA doses met a clinically significant threshold of ≥ 10 % increase versus placebo. When comparing the maximum response at any L-DOPA dose to placebo, high effect sizes were observed for these primary outcomes and tb-FC during reward anticipation (dz = 0.82–0.98, p &lt; 0.01), as well as secondary and exploratory measures of anhedonia and depression severity (dz = 0.48–0.97, p &lt; 0.05). 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Inflammatory biomarkers like C-reactive protein (CRP) are elevated in a subset of patients with depression and associated with lower functional connectivity (FC) in a ventral striatum (VS) to ventromedial prefrontal cortex (vmPFC) reward circuit and symptoms of anhedonia. Evidence linking these relationships to the effects of inflammation on dopamine is consistent with our recent findings that acute levodopa (L-DOPA) increased VS-vmPFC FC in association with deceased anhedonia in depressed patients with higher but not lower CRP (&gt;2 versus ≤ 2 mg/L). To determine whether repeated L-DOPA administration caused sustained effects on FC and behavior in these patients, medically stable depressed outpatients with CRP &gt; 2 mg/L and anhedonia (n = 18) received one week of three doses of L-DOPA (150–450 mg/day/week with carbidopa) or placebo in a randomized order. Resting-state (rs) and task-based (tb; monetary incentive delay) fMRI, effort-based motivation, and exploratory measures of anhedonia and depression severity were assessed at baseline and after one week of placebo and each dose of L-DOPA. Responses to individual doses of L-DOPA varied across outcomes. For example, VS-vmPFC rs-FC was significantly increased by L-DOPA at 150 and 450 mg/day/week (p &lt; 0.01), whereby approximately half of patients responded optimally to 150 mg/day L-DOPA and approximately half required higher doses for maximum effect. While effort-based motivation was only significantly increased by L-DOPA at 150 mg/day (p &lt; 0.05), it correlated with VS-vmPFC rs-FC at this dose (r = 0.64, p = 0.024), and all L-DOPA doses met a clinically significant threshold of ≥ 10 % increase versus placebo. When comparing the maximum response at any L-DOPA dose to placebo, high effect sizes were observed for these primary outcomes and tb-FC during reward anticipation (dz = 0.82–0.98, p &lt; 0.01), as well as secondary and exploratory measures of anhedonia and depression severity (dz = 0.48–0.97, p &lt; 0.05). Sustained effects on reward circuitry, effort-based motivation, and anhedonia by repeated L-DOPA administration support the therapeutic potential of agents that increase dopamine in depressed patients with higher inflammation.</description><subject>Anhedonia</subject><subject>C-reactive protein</subject><subject>Depression</subject><subject>Dopamine</subject><subject>Functional connectivity</subject><subject>Inflammation</subject><subject>Motivation</subject><issn>0889-1591</issn><issn>1090-2139</issn><issn>1090-2139</issn><fulltext>true</fulltext><rsrctype>article</rsrctype><creationdate>2024</creationdate><recordtype>article</recordtype><recordid>eNp9kdFqFDEUhoNY7Lb6AN5ILlvojDmZmZ0Er0qtWliooF6HzOTEzTIzGZPMlj6Sb2m2W70UEgLh-_9D8hHyFlgJDNbvd2XXuZIzXpfAS8bXL8gKmGQFh0q-JCsmhCygkXBKzmLcMcaaCsQrclrJtayrmq_I729LTNpNaChai32K1FsacEad8t2Ae2_8rOnFpvh4__X6kmozusnFFHRyfqJ5BXzQwdDehX5xKTxeHZp8SEWnY64YfXL7J_iK6snkvUXjJ6epm6jBOWA8YHNGcMrjH1za0q37ucWQCTvocXxKvyYnVg8R3zyf5-THp9vvN1-Kzf3nu5vrTdFDw3iBEsAIqPm6bpq2qy1vWyGgaoxg2rQgsdVaSsZ6IbjtrLa2403NrW6NBdNU5-Ti2DsH_2vBmNToYo_DoCf0S1QV1C1w2QqZUTiiffAxBrRqDm7U4VEBUwdDaqeyIXUwpICrbChn3j3XL92I5l_ir5IMfDgCmB-5dxhU7PPP9GhcyH6U8e4_9X8AU7OkGw</recordid><startdate>20241216</startdate><enddate>20241216</enddate><creator>Mandakh, Bekhbat</creator><creator>Zhihao, Li</creator><creator>Dunlop, Boadie W.</creator><creator>Treadway, Michael T.</creator><creator>Mehta, Neeti D.</creator><creator>Revill, Kate P.</creator><creator>Lucido, Michael J.</creator><creator>Changdo, Hong</creator><creator>Andrea, Ashchi</creator><creator>Wommack, Evanthia C.</creator><creator>Goldsmith, David R.</creator><creator>Ebrahim, Haroon</creator><creator>Miller, Andrew H.</creator><creator>Felger, Jennifer C.</creator><general>Elsevier Inc</general><scope>NPM</scope><scope>AAYXX</scope><scope>CITATION</scope><scope>7X8</scope></search><sort><creationdate>20241216</creationdate><title>Sustained effects of repeated levodopa (L-DOPA) administration on reward circuitry, effort-based motivation, and anhedonia in depressed patients with higher inflammation</title><author>Mandakh, Bekhbat ; 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Inflammatory biomarkers like C-reactive protein (CRP) are elevated in a subset of patients with depression and associated with lower functional connectivity (FC) in a ventral striatum (VS) to ventromedial prefrontal cortex (vmPFC) reward circuit and symptoms of anhedonia. Evidence linking these relationships to the effects of inflammation on dopamine is consistent with our recent findings that acute levodopa (L-DOPA) increased VS-vmPFC FC in association with deceased anhedonia in depressed patients with higher but not lower CRP (&gt;2 versus ≤ 2 mg/L). To determine whether repeated L-DOPA administration caused sustained effects on FC and behavior in these patients, medically stable depressed outpatients with CRP &gt; 2 mg/L and anhedonia (n = 18) received one week of three doses of L-DOPA (150–450 mg/day/week with carbidopa) or placebo in a randomized order. Resting-state (rs) and task-based (tb; monetary incentive delay) fMRI, effort-based motivation, and exploratory measures of anhedonia and depression severity were assessed at baseline and after one week of placebo and each dose of L-DOPA. Responses to individual doses of L-DOPA varied across outcomes. For example, VS-vmPFC rs-FC was significantly increased by L-DOPA at 150 and 450 mg/day/week (p &lt; 0.01), whereby approximately half of patients responded optimally to 150 mg/day L-DOPA and approximately half required higher doses for maximum effect. While effort-based motivation was only significantly increased by L-DOPA at 150 mg/day (p &lt; 0.05), it correlated with VS-vmPFC rs-FC at this dose (r = 0.64, p = 0.024), and all L-DOPA doses met a clinically significant threshold of ≥ 10 % increase versus placebo. When comparing the maximum response at any L-DOPA dose to placebo, high effect sizes were observed for these primary outcomes and tb-FC during reward anticipation (dz = 0.82–0.98, p &lt; 0.01), as well as secondary and exploratory measures of anhedonia and depression severity (dz = 0.48–0.97, p &lt; 0.05). Sustained effects on reward circuitry, effort-based motivation, and anhedonia by repeated L-DOPA administration support the therapeutic potential of agents that increase dopamine in depressed patients with higher inflammation.</abstract><cop>Netherlands</cop><pub>Elsevier Inc</pub><pmid>39694342</pmid><doi>10.1016/j.bbi.2024.12.026</doi></addata></record>
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source ScienceDirect Journals (5 years ago - present)
subjects Anhedonia
C-reactive protein
Depression
Dopamine
Functional connectivity
Inflammation
Motivation
title Sustained effects of repeated levodopa (L-DOPA) administration on reward circuitry, effort-based motivation, and anhedonia in depressed patients with higher inflammation
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