Fatty acid-binding proteins 5 and 7 gene deletion increases sucrose consumption and diminishes forced swim immobility time

Abstract: Inhibition and genetic deletion of fatty acid-binding proteins (FABPs) 5 and 7 have been shown to increase the levels of the endocannabinoid anandamide as well as the related N-acylethanolamine's palmitoylethanolamide and oleoylethanolamide. This study examined the role of these FABPs on forced-swim (FS) behavior and on sucrose consumption in two experiments: (experiment 1) using wild-type (WT) mice treated with the FABP inhibitor SBFI26 or vehicle and (experiment 2) using WT and FABP5/7 deficient mice. Result… Show more

“…In summary, given that there are noted neurochemical changes reported in the present study as well as behavioral differences in FABP5-deficient mice in related cognitive/addiction disease-modeling studies [ 1 , 4 – 6 , 9 , 72 ], and there is an existing modulatory relationship between endocannabinoid signaling and DA content within the midbrain [ 3 , 58 ], further research is needed to investigate FABP5’s neuropathophysiological role in shaping DA circuits.…”

“…The epidermal/brain FABP type 5 (FABP5) has been specifically implicated in the cellular uptake of the central endocannabinoid neurotransmitter, anandamide, as well as its hydrolysis into arachidonic acid [ 1 , 2 ] and, finally, its transportation to the nucleus where multiple cellular cascades take place—some of which subsequently alter behavior and dopaminergic functioning [ 3 ]. Recent pre-clinical studies have investigated FABP5 in the context of various dopamine (DA)-linked neuropathophysiological phenotypes; these include studies on depression-, anxiety-, and drug addiction-like behaviors [ 4 – 7 ] as well as neurochemical changes relating to memory functioning, stress, pain sensation, and neuroinflammation [ 5 , 8 – 11 ].…”

“…The DA system is well known to be associated with the neuromodulation of depression- and addiction-like phenotypes [ 12 – 16 ]. Hamilton and colleagues showed that transgenic FABP5−/− (knockout) mice significantly increased sucrose consumption and reduced immobility times in the forced-swim test compared with their wild-type counterparts [ 4 ]. In related behavioral evidence, pharmacological administration of DA type 2 (D2) agonists has been shown to reduce immobility time in the forced swim test, indicating that greater D2 activation exerts an antidepressant effect [ 17 ].…”

“…In two similar studies, antagonism of DA type 1 (D1) or D2 in the nucleus accumbens selectively decreased sucrose cue-evoked excitation, predicted the animal’s movement, and preceded their movement onset [ 18 ]; additionally, antagonism of D2 has been shown to decrease intake of sucrose as a function of its concentration [ 19 ]. Therefore, dopamine signaling is important for both reward-seeking behavior and orosensory stimulation of sucrose, and the FABP5 gene has been implicated in these DA-linked behaviors of consuming/seeking rewarding sucrose [ 15 , 20 ] and mediating immobility time in the forced swim test [ 4 , 17 , 21 ].…”

Fatty acid-binding protein 5 differentially impacts dopamine signaling independent of sex and environment

“…In summary, given that there are noted neurochemical changes reported in the present study as well as behavioral differences in FABP5-deficient mice in related cognitive/addiction disease-modeling studies [ 1 , 4 – 6 , 9 , 72 ], and there is an existing modulatory relationship between endocannabinoid signaling and DA content within the midbrain [ 3 , 58 ], further research is needed to investigate FABP5’s neuropathophysiological role in shaping DA circuits.…”

“…The epidermal/brain FABP type 5 (FABP5) has been specifically implicated in the cellular uptake of the central endocannabinoid neurotransmitter, anandamide, as well as its hydrolysis into arachidonic acid [ 1 , 2 ] and, finally, its transportation to the nucleus where multiple cellular cascades take place—some of which subsequently alter behavior and dopaminergic functioning [ 3 ]. Recent pre-clinical studies have investigated FABP5 in the context of various dopamine (DA)-linked neuropathophysiological phenotypes; these include studies on depression-, anxiety-, and drug addiction-like behaviors [ 4 – 7 ] as well as neurochemical changes relating to memory functioning, stress, pain sensation, and neuroinflammation [ 5 , 8 – 11 ].…”

“…The DA system is well known to be associated with the neuromodulation of depression- and addiction-like phenotypes [ 12 – 16 ]. Hamilton and colleagues showed that transgenic FABP5−/− (knockout) mice significantly increased sucrose consumption and reduced immobility times in the forced-swim test compared with their wild-type counterparts [ 4 ]. In related behavioral evidence, pharmacological administration of DA type 2 (D2) agonists has been shown to reduce immobility time in the forced swim test, indicating that greater D2 activation exerts an antidepressant effect [ 17 ].…”

“…In two similar studies, antagonism of DA type 1 (D1) or D2 in the nucleus accumbens selectively decreased sucrose cue-evoked excitation, predicted the animal’s movement, and preceded their movement onset [ 18 ]; additionally, antagonism of D2 has been shown to decrease intake of sucrose as a function of its concentration [ 19 ]. Therefore, dopamine signaling is important for both reward-seeking behavior and orosensory stimulation of sucrose, and the FABP5 gene has been implicated in these DA-linked behaviors of consuming/seeking rewarding sucrose [ 15 , 20 ] and mediating immobility time in the forced swim test [ 4 , 17 , 21 ].…”

Fatty acid-binding protein 5 differentially impacts dopamine signaling independent of sex and environment

“…Регулируемая при участии SREBP-1a (sterol regulatory element-binding protein 1) Acss2 способствует увеличению жировых запасов и отягощению ожирения [30]. Кодируемый Fabp5 переносчик жирных кислот препятствует апоптозу адипоцитов [31] посредством системы эндоканнабиноидов и GIP, повышает потребление пищи и на высококалорийных рационах, чем способствует развитию диет-индуцированного ожирения [32,33]. Характерно, что у мышей db/db контрольной группы экспрессия обоих этих генов была, по-видимому, изначально повышена по сравнению с контрольными C57Bl/6J.…”

Full transcriptome analysis of gene expression in liver of mice in a comparative study of quercetin efficiency on two obesity models

Overview of the Endocannabinoid System and Endocannabinoidome