Full metadata record
| DC Field | Value | Language |
|---|---|---|
| dc.contributor.advisor | Yu, Seong Woon | - |
| dc.contributor.author | Shim, Hyun Jung | - |
| dc.date.accessioned | 2017-05-10T08:52:23Z | - |
| dc.date.available | 2016-02-12T00:00:00Z | - |
| dc.date.issued | 2016 | - |
| dc.identifier.uri | http://dgist.dcollection.net/jsp/common/DcLoOrgPer.jsp?sItemId=000002229068 | en_US |
| dc.identifier.uri | http://hdl.handle.net/20.500.11750/1443 | - |
| dc.description.abstract | Neuroinflammation has relevance to many neurodegenerative diseases. Although certain aspects of inflammatory responses have beneficial effects, uncontrolled inflammation may impair the maintenance of homeostasis and exacerbate disease states. Microglia, the major resident brain immune cells, are mainly associated with neuroinflammatory responses in the central nervous system. Under normal condition, deactivated microglia produce anti-inflammatory and neurotrophic factors. However, under exposure of invaded pathogen or tissue damage, microglia are activated and promote a pro-inflammatory response. The translocator protein 18 kDa (TSPO) is a five transmembrane protein localized in the outer mitochondrial membrane. The expression level of TSPO is increased by neuroinflammation in activated microglia and astrocytes. Although there is a close correlation between a high expression level of TSPO and neuroinflammation, it is not known how TSPO is involved in the regulation of neuroinflammation and microglia activation. To reveal the role of TSPO in the regulation of inflammation and the related mechanisms through which TSPO regulates neuroinflammation, we examined the effects of two TSPO ligands, PK11195 and Ro5-4864, and TSPO overexpression on the signaling molecules important in mediation of microglia activation. Lipopolysaccharide (LPS) treatment induced a robust increase in the production of inflammatory factors, such as nitric oxide (NO), tumor necrosis factors (TNF) -α and interlukin (IL) -6. TSPO overexpression significantly attenuated the production of pro-inflammatory cytokines. TSPO ligands inhibited mitogen-activated protein kinases (MAPK) pathway, especially Jun N-terminal kinase (JNK) and p38, but not Erk. In addition, TSPO overexpression or pretreatment with TSPO ligands reduced LPS-induced NF-κB transcriptional activity. These results demonstrate that TSPO negatively regulates neruroinflammation and microglia activation through the suppression of NF-κB and MAPK signaling pathways. Recently, the role and mechanisms of parkin in the regulation of inflammation has been reported. Because Parkin was recruited to mitochondria following LPS treatment, we confirmed the relationship between TSPO and Parkin in inflammation in microglia. Although Parkin has anti-inflammatory effects, TSPO knockdown blocked the inhibitory effects of Parkin against the production of pro-inflammatory cytokines. Futhermore, TSPO and Parkin suppressed inflammation via autophagy. However, TSPO knock-down increased p62 aggregation that reduced by Parkin. This study was aimed to investigate whether TSPO negatively regulates neuroinflammation and microglia activation via the regulation of parkin and p62 in microglia. The results obtained from this study will unveil the regulatory mechanisms of TSPO in neuroinflammation, thereby contribute to the anti-inflammatory therapeutic design for the treatment of neurodegernative diseases ⓒ 2016 DGIST |
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| dc.description.tableofcontents | 1. INTRODUCTION 1-- 1.1 Microglia 1-- 1.1.1Origin and distribution 1-- 1.1.2Microglia morphology and activation 2-- 1.2 Neuroinflammation 2-- 1.2.1 Microglia in neuroinflammation 2-- 1.2.2Neuroinflammation in neurodegenerative disease 3-- 1.3 TSPO 4-- 1.3.1Historical perspective and recent controversial topics 5-- 1.3.2 Structure and distribution 5-- 1.3.3 Function 5-- 1.3.4 Ligands 6-- 1.3.5 TSPO in neuroinflammation and neurodegenerative disease 6-- 1.4 Parkin 7-- 1.4.1 Parkin Structure and Function 7-- 1.4.2 Parkin and neuroinflammation in neurodegenerative diseases 8-- 2. Methods and Materials 9-- 2.1 Chemicals and reagents 9-- 2.2 Cell cultures 9-- 2.3 Nitrite assay 9-- 2.4 Enzyme-Linked Immunosorbent Assay (ELISA) 10-- 2.5 NF-κB luciferase reporter assay 10-- 2.6 Western blot Analysis 10-- 2.7 Immunoprecipitation 11-- 2.8 DNA transfection and knockdown 11-- 2.9 Statistical Analyses 12-- 3. Results 13-- 3.1 Translocator Protein 18 kDa (TSPO) is a negative regulator in neuroinflammation in microglia 13-- 3.2 TSPO suppresses MAPK activation and NF-κB activity in microglia 13-- 3.3 Parkin suppresses neuroinflammation in microglia 14-- 3.4 TSPO modulates neuroinflammation via Parkin in microglia 15-- 3.5 TSPO and Parkin regulate inflammation via autophagy 16-- 3.6 Parkin R275W mutant is associated with the regulation of inflammation in microglia 16-- 4. Discussion 18-- 5. Figure legends 21-- 6. Figures 26-- References 44-- |
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| dc.format.extent | 53 | - |
| dc.language | eng | - |
| dc.publisher | DGIST | - |
| dc.subject | Neuroinflammation | - |
| dc.subject | Microglia | - |
| dc.subject | TSPO | - |
| dc.subject | Parkin | - |
| dc.subject | p62 | - |
| dc.subject | 신경 | - |
| dc.subject | 염증 | - |
| dc.subject | 반응 | - |
| dc.subject | 미세아교세포 | - |
| dc.title | TSPO mediates neuroinflammation via Parkin and p62 regulation in microglia | - |
| dc.title.alternative | 미세아교세포에서의 Parkin 및 p62를 통한 TSPO의 신경 염증 반응 조절 | - |
| dc.type | Thesis | - |
| dc.identifier.doi | 10.22677/thesis.2229068 | - |
| dc.description.alternativeAbstract | 신경염증반응은 많은 신경퇴행성 뇌질환과 관련이 있다. 비록 염증 반응이 유익한 측면도 있지만, 잘못 조절된 염증 반응은 항상성을 파괴하고, 병의 진행을 더욱 빠르게 한다. 주요한 뇌신경계 면역 세포인 미세아교세포는 이러한 신경 염증 반응에서 중요한 역할을 한다. 정상적인 상태에서 미세아교세포는 활성화 되지 않은 상태로 존재하며, 신체에 이로운 신경영양인자들을 분비하지만, 병원체의 침입 및 조직의 손상이 유발된 경우, 미세아교세포는 활성화 상태로 변화하여 염증반응을 유발한다. Translocator protein 18 kDa (TSPO)는 미토콘드리아 바깥쪽 막에 있는 five transmembrane protein 이다. TSPO 는 정상 상태에서는 낮은 발현을 보이나, 신경염증 반응에 의해 미세아교세포가 활성화 되면 TSPO 의 발현이 증가된다. 비록 신경 염증에 의한 TSPO 발현의 증가양상은 알려졌으나, TSPO 가 신경염증반응에서 어떤 역할을 하는지는 명확히 알려진 바가 없었다. 본 연구에서는 TSPO 의 리간드 및 과발현 실험을 통해 염증반응에서의 TSPO 의 역할과 조절기작을 밝혔다. TSPO 의 과발현은 신경염증반응에 의한 염증성 사이토카인의 분비를 억제시켰으며, MAKP (JNK 와 p38)와 NF-κB 에 의한 염증반응 유발 경로 또한 효과적으로 줄이는 양상을 보여주었다. 이러한 결과들은 TSPO 가 신경염증반응을 억제하는 조절자라는 것을 입증하였다. 최근 Parkin 에 의한 신경염증반응 조절에 대한 연구가 활발히 보고되고 있다. Parkin 은 LPS 에 의해 세포질에서 미토콘드리아로 이동하여 염증반응에 관여한다고 보고되었기 때문에, 신경염증반응 조절에 있어서 TSPO 와 Parkin 의 연관성에 대해 연구하였다. Parkin 의 과발현은 항염증 효과를 보여주었으나, TSPO 의 발현을 억제할 경우 Parkin 에 의한 항염증 효과도 줄어드는 것을 확인할 수 있었다. 뿐만 아니라, TSPO 및 Parkin 은 autophagy marker 인 p62 의 응집을 완화시키는 것이 관찰 되었다. 하지만, TSPO 의 발현을 억제한 경우 parkin 에 의한 p62 의 응집이 완화되는 현상은 줄어드는 것으로 보아, TSPO 가 Parkin 을 통해 p62 의 증가된 응집을 완화시키고, autophagy 를 통해 염증반응을 줄여주는 것으로 사료된다. 본 연구는 뇌신경염증반응에 있어서 TSPO 의 역할 및 조절기작을 밝혀, 항염증 약물의 개발에 도움을 줄 것이며, 나아가 신경퇴행성 뇌질환의 치료의 발판을 마련할 것으로 기대된다. ⓒ 2016 DGIST | - |
| dc.description.degree | Master | - |
| dc.contributor.department | Brain and Cognitive Sciences | - |
| dc.contributor.coadvisor | Choi, Ji Woong | - |
| dc.date.awarded | 2016. 2 | - |
| dc.publisher.location | Daegu | - |
| dc.description.database | dCollection | - |
| dc.date.accepted | 2016-02-12 | - |
| dc.contributor.alternativeDepartment | 대학원 뇌인지과학전공 | - |
| dc.contributor.affiliatedAuthor | Shim, Hyun Jung | - |
| dc.contributor.affiliatedAuthor | Yu, Seong Woon | - |
| dc.contributor.affiliatedAuthor | Choi, Ji Woong | - |
| dc.contributor.alternativeName | 심현정 | - |
| dc.contributor.alternativeName | 유성운 | - |
| dc.contributor.alternativeName | 최지웅 | - |
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