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Development of a surrogate marker for P-glycoprotein expression in drug-resistant epilepsy using the (R)-[11C]-Verapamil PET/MR with cyclosporine : 난치성 뇌전증에서 사이클로스포린과 (R)-[11C]-Verapamil PET/MR을 이용한 P-glycoprotein 발현의 대리표지자 개발

DC Field Value Language
dc.contributor.advisor이상건-
dc.contributor.author신정원-
dc.date.accessioned2017-07-14T01:16:39Z-
dc.date.available2017-07-14T01:16:39Z-
dc.date.issued2016-02-
dc.identifier.other000000132875-
dc.identifier.urihttps://hdl.handle.net/10371/121791-
dc.description학위논문 (박사)-- 서울대학교 대학원 : 의과대학협동과정 임상약리학전공, 2016. 2. 이상건.-
dc.description.abstractBackground and Purpose: The development of resistance to antiepileptic drugs is explained well by the transporter hypothesis, which suggests that drug resistance is caused by inadequate penetration of drugs into the brain barrier as a result of increased levels of efflux transporter such as p-glycoprotein. To evaluate the brain expression of p-glycoprotein (Pgp) in patients with drug-resistant epilepsy (DRE), including neocortical epilepsy, we developed a non-invasive quantitative analysis including asymmetry indices (AIs) based on (R)-[11C]-verapamil PET/MRI with cyclosporine (CS)-
dc.description.abstracta Pgp inhibitor.
Materials and Methods: Nine patients with DRE, five patients with drug-sensitive epilepsy (DSE), and eight healthy subjects underwent dynamic (R)-[11C]-verapamil PET/MRI with an intravenous infusion of CS. AIs [(right region – left region)/(right region + left region) ×200%] of the standard uptake values in each of the paired lobes were calculated.
Results: All DRE patients, except for patients with parietal lobe epilepsy, had significantly different asymmetry from the healthy subjects, whereas all DSE patients had asymmetry similar to healthy subjects. In the temporal lobe, the AIs of patients with left temporal lobe DRE were more positive than those of healthy subjects (healthy subjects: 4.0413 ± 1.7452
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dc.description.abstractpatients: 7.2184 ± 1.8237-
dc.description.abstractp = 0.048), and those of patients with right temporal DRE were more negative (patients: -1.6496 ± 3.4136-
dc.description.abstractp = 0.044). In addition, specific regions which had significant asymmetry were different between lateral and medial temporal lobe epilepsy groups. In the frontal lobe, the AI of patient with right frontal lobe DRE was more negative than healthy subjects.
Conclusions: We confirmed that Statistical Parametric Mapping analysis using AIs of (R)-[11C]-verapamil PET/MRI with CS could be used as a surrogate marker for DRE, and this approach might be helpful for localizing or lateralizing the epileptic zone. ClinicalTrials.gov number: NCT02144792
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dc.description.tableofcontentsINTRODUCTION 1

METHODS 4
1. Subjects 4
2. PET/MRI and Experimental Procedures 5
3. Synthesis of (R)-[11^C]-verapamil 6
4. PET Data Analysis and Acquisition of Asymmetry Indices 7
5. Genotyping Methods 8
6. Statistical Analyses 9

RESULTS 10
1. Basal demographics 10
2. Characteristics of VPM-PET/MR–CS 11
3. Comparing uptake of (R)-[11^C] - verapamil between two kinds of Pgp inhibitors 12
4. Different Values of AIs in DRE Patients and Healthy Subjects 12
5. Possibility of localization using VPM-PET/MR–CS 13

DISCUSSION 15

CONCLUSION 20

REFERENCES 21

TABLES 25

FIGURES 31

국문요약 40
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dc.formatapplication/pdf-
dc.format.extent1519219 bytes-
dc.format.mediumapplication/pdf-
dc.language.isoen-
dc.publisher서울대학교 대학원-
dc.subjectP-glycoprotein-
dc.subjectDrug-resistant epilepsy-
dc.subjectSurrogate marker-
dc.subjectPET/MR-
dc.subject(R)-[11C]-verapamil-
dc.subject.ddc615-
dc.titleDevelopment of a surrogate marker for P-glycoprotein expression in drug-resistant epilepsy using the (R)-[11C]-Verapamil PET/MR with cyclosporine-
dc.title.alternative난치성 뇌전증에서 사이클로스포린과 (R)-[11C]-Verapamil PET/MR을 이용한 P-glycoprotein 발현의 대리표지자 개발-
dc.typeThesis-
dc.description.degreeDoctor-
dc.citation.pages42-
dc.contributor.affiliation의과대학 협동과정임상약리학전공-
dc.date.awarded2016-02-
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