TY - JOUR
T1 - Nucleus accumbens deep brain stimulation improves depressive-like behaviors through BDNF-mediated alterations in brain functional connectivity of dopaminergic pathway
AU - Li, Ssu Ju
AU - Lo, Yu Chun
AU - Tseng, Hsin Yi
AU - Lin, Sheng Huang
AU - Kuo, Chao Hung
AU - Chen, Ting Chieh
AU - Chang, Ching Wen
AU - Liang, Yao Wen
AU - Lin, Yi Chen
AU - Wang, Chih Yu
AU - Cho, Tsai Yu
AU - Wang, Mu Hua
AU - Chen, Ching Te
AU - Chen, You Yin
N1 - Funding Information:
This work is financially supported by Taiwan National Science and Technology Council under contract numbers of 112-2622-8-A49-010-TE2 , 112-2321-B-A49-009 , 110-2314-B-038-074 , 111-2731-M-002-001 , 111-2314-B-038-059-MY3 , 111-2221-E-A49-049-MY2 , 111-2321-B-A49-005 . This research also is supported by the “Key and Novel Therapeutics Development Program for Major Diseases” project of Academia Sinica, Taiwan, R.O.C . under the grant number of AS-KPQ-111-KNT .
Funding Information:
In our study, MRI was used to exclude animals with incorrect probe placement. This step was crucial as incorrect placement could result in ineffective treatment. By using MRI to accurately determine whether the probe placement was correct, we were able to assess the therapeutic effect of NAc-DBS more precisely on the CSDS model. To confirm this, we added a negative control group to our study. We found that animals with incorrect probe placement but still receiving electrical stimulation did not show significant therapeutic effects in behavioral performance and FC. The use of MRI also circumvents radiation exposure associated with CT and can readily identify complications related to electrode implantation (Cole et al., 2009). By using MRI to confirm electrode placement after implantation, we can reduce costs and save time in academic research. If the initial surgical implantation is incorrect, there will be no effective treatment. Relevant literature can also be found to support our perspective. One study investigated the clinical safety of intracranial EEG electrodes in MRI at 1.5 T and 3 T (Guo et al., 2015). A study also provided a pictorial review of pre- and post-operative imaging of cochlear implants (Sanchez et al., 2016). Another study discussed the design of a robotic system for MRI-guided deep brain stimulation electrode placement (Cole et al., 2009). Our experimental results are consistent with these studies and support the use of MRI to confirm electrode placement after implantation.This work is financially supported by Taiwan National Science and Technology Council under contract numbers of 112-2622-8-A49-010-TE2, 112-2321-B-A49-009, 110-2314-B-038-074, 111-2731-M-002-001, 111-2314-B-038-059-MY3, 111-2221-E-A49-049-MY2, 111-2321-B-A49-005. This research also is supported by the “Key and Novel Therapeutics Development Program for Major Diseases” project of Academia Sinica, Taiwan, R.O.C. under the grant number of AS-KPQ-111-KNT.The authors thank 7T animal MRI Core Lab of the Neurobiology and Cognitive Science Center, National Taiwan University for technical and facility support, and Dr. Jyh-Horng Chen and Dr. Chao-Hsien Hsieh of Instrumentation Center for MRI experiments at National Taiwan University.
Publisher Copyright:
© 2023
PY - 2023/9
Y1 - 2023/9
N2 - Major depressive disorder (MDD), a common psychiatric condition, adversely affects patients’ moods and quality of life. Despite the development of various treatments, many patients with MDD remain vulnerable and inadequately controlled. Since anhedonia is a feature of depression and there is evidence of leading to metabolic disorder, deep brain stimulation (DBS) to the nucleus accumbens (NAc) might be promising in modulating the dopaminergic pathway. To determine whether NAc-DBS alters glucose metabolism via mitochondrial alteration and neurogenesis and whether these changes increase neural plasticity that improves behavioral functions in a chronic social defeat stress (CSDS) mouse model. The Lab-designed MR-compatible neural probes were implanted in the bilateral NAc of C57BL/6 mice with and without CSDS, followed by DBS or sham stimulation. All animals underwent open-field and sucrose preference testing, and brain resting-state functional MRI analysis. Meanwhile, we checked the placement of neural probes in each mouse by T2 images. By confirming the placement location, mice with incorrect probe placement (the negative control group) showed no significant therapeutic effects in behavioral performance and functional connectivity (FC) after receiving electrical stimulation and were excluded from further analysis. Western blotting, seahorse metabolic analysis, and electron microscopy were further applied for the investigation of NAc-DBS. We found NAc-DBS restored emotional deficits in CSDS-subjected mice. Concurrent with behavioral amelioration, the CSDS DBS-on group exhibited enhanced FC in the dopaminergic pathway with increased expression of BDNF- and NeuN-positive cells increased dopamine D1 receptor, dopamine D2 receptors, and TH in the medial prefrontal cortex, NAc, ventral hippocampus, ventral tegmental area, and amygdala. Increased pAMPK/total AMPK and PGC-1α levels, functions of oxidative phosphorylation, and mitochondrial biogenesis were also observed after NAc-DBS treatment. Our findings demonstrate that NAc-DBS can promote BDNF expression, which alters FC and metabolic profile in the dopaminergic pathway, suggesting a potential strategy for ameliorating emotional processes in individuals with MDD.
AB - Major depressive disorder (MDD), a common psychiatric condition, adversely affects patients’ moods and quality of life. Despite the development of various treatments, many patients with MDD remain vulnerable and inadequately controlled. Since anhedonia is a feature of depression and there is evidence of leading to metabolic disorder, deep brain stimulation (DBS) to the nucleus accumbens (NAc) might be promising in modulating the dopaminergic pathway. To determine whether NAc-DBS alters glucose metabolism via mitochondrial alteration and neurogenesis and whether these changes increase neural plasticity that improves behavioral functions in a chronic social defeat stress (CSDS) mouse model. The Lab-designed MR-compatible neural probes were implanted in the bilateral NAc of C57BL/6 mice with and without CSDS, followed by DBS or sham stimulation. All animals underwent open-field and sucrose preference testing, and brain resting-state functional MRI analysis. Meanwhile, we checked the placement of neural probes in each mouse by T2 images. By confirming the placement location, mice with incorrect probe placement (the negative control group) showed no significant therapeutic effects in behavioral performance and functional connectivity (FC) after receiving electrical stimulation and were excluded from further analysis. Western blotting, seahorse metabolic analysis, and electron microscopy were further applied for the investigation of NAc-DBS. We found NAc-DBS restored emotional deficits in CSDS-subjected mice. Concurrent with behavioral amelioration, the CSDS DBS-on group exhibited enhanced FC in the dopaminergic pathway with increased expression of BDNF- and NeuN-positive cells increased dopamine D1 receptor, dopamine D2 receptors, and TH in the medial prefrontal cortex, NAc, ventral hippocampus, ventral tegmental area, and amygdala. Increased pAMPK/total AMPK and PGC-1α levels, functions of oxidative phosphorylation, and mitochondrial biogenesis were also observed after NAc-DBS treatment. Our findings demonstrate that NAc-DBS can promote BDNF expression, which alters FC and metabolic profile in the dopaminergic pathway, suggesting a potential strategy for ameliorating emotional processes in individuals with MDD.
KW - Deep brain stimulation
KW - Depression
KW - Dopaminergic pathway
KW - Functional connectivity (FC)
KW - Mitochondrial biogenesis
KW - Nucleus accumbens
UR - http://www.scopus.com/inward/record.url?scp=85168742759&partnerID=8YFLogxK
UR - http://www.scopus.com/inward/citedby.url?scp=85168742759&partnerID=8YFLogxK
U2 - 10.1016/j.ynstr.2023.100566
DO - 10.1016/j.ynstr.2023.100566
M3 - Article
AN - SCOPUS:85168742759
SN - 2352-2895
VL - 26
JO - Neurobiology of Stress
JF - Neurobiology of Stress
M1 - 100566
ER -