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Synthesis of 5, 10, 15, 20-Tetrakis(7-sulfanatobenzo[b]thiophene) Porphyrin for Mitochondria and DNA Targeted Photodynamic Therapy : 미토콘드리아 및 DNA 타겟 광역동 치료를 위한 술폰산벤조티오핀 포피린 합성

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dc.contributor.advisorJoon Myong Song-
dc.contributor.authorRangasamy Sabarinathan-
dc.date.accessioned2017-07-13T16:38:00Z-
dc.date.available2017-07-13T16:38:00Z-
dc.date.issued2016-02-
dc.identifier.other000000133109-
dc.identifier.urihttps://hdl.handle.net/10371/120128-
dc.description학위논문 (박사)-- 서울대학교 대학원 : 약학대학 약학과 약품분석학전공, 2016. 2. 송준명.-
dc.description.abstractPorphyrins are rich in applications and it can be called as the colors of life. From the photosynthetic process in plants, to the red hemoglobin that carries oxygen to the cells in our bodies utilize porphyrin molecules. Thus, without any surprise porphyrins are actively explored as tools for wider applications to improve medicine and other biomedical fields. With the aim of improving photodynamic therapy (PDT) in mind, this thesis work examines new synthetic porphyrins for selective targeting of sub-cellular compartments in cancerous cells and execute apoptotic cell death upon PDT, and causing minimal destruction and irritation to normal tissue.

PDT is a phototherapeutic cancer therapy in which a photosensitizer (PS)—light activated drug—absorbs light of specific wavelength and excites to the singlet state. From the excited singlet state, PSs can undergo an internal transition to the excited triplet state, a relatively long-lived and high-energy species that transfers its excess energy to molecular oxygen. Subsequently, molecular oxygen excites from the stable triplet state to the highly reactive singlet state. With no spin-state restriction, singlet oxygen is cytotoxic, readily reacting with electron-rich biomolecules such as unsaturated lipids, amino acids and DNA consequently destroying the tumor cell. Singlet oxygen has a limited range of diffusion. Therefore, the site of its generation is also the site of initial damage.

Photosensitizers used in PDT are often classified as first, second and third generation PS. This classification is based on the historical development and conceptual approaches. Haematoporphyrin derivative (HpD) or Photofrin are otherwise called as first generation PS enjoyed its success in cancer therapy due to their tumor localizing and photophysical properties yet suffers from its drawbacks (mixture of compounds and less selectivity). Herein, second generation PSs with high purity and improved photophysical properties had been developed. Still there is always room for improver, and current research efforts are aimed at developing third generation PSs where additional biological criteria such as selective targeting of sub-cellular organelles are considered in the design principle.

Herein, this thesis work focused in developing third generation PSs that can target selectively sub-cellular organelles such mitochondria and DNA and effectively induce apoptotic cell death after PDT. In Chapter I, a comprehensive background on history of photodynamic therapy, fundamental aspects, classification and requirements of PSs is presented. In chapter 2, synthesis, structural elucidation, photophysical properties and in vitro photokilling and mechanism of cell death of 5, 10, 15, 20–Tetrakis(7-sulfonatobenzo[b]thiophene)porphyrin (SBTP) is studied.

Keywords: porphyrin
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dc.description.abstractphotosensitizers-
dc.description.abstractphotodynamic therapy-
dc.description.abstractmitochondria-
dc.description.abstractDNA-
dc.description.abstractapoptosis-
dc.description.abstractintrinsic-
dc.description.abstractextrinsic-
dc.description.abstracthigh-content assay.

Student number: 2010-31366
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dc.description.tableofcontentsChapter I Introduction 1
1.0. Cancer 1
1.0.1. Causes of cancer 2
1.0.2. Cancer prevention 2
1.0.3. Cancer Treatments 3
1.2. Photodynamic Therapy 3
1.2.1. History of Photodynamic therapy 3
1.2.1. Basic principles of PDT 7
1.2.2. Mechanisms of tumour destruction 9
1.3. Sensitizers 10
1.3.1. Porphyrinoid photosensitizers 14
1.4. Classification of photosensitizers 17
1.4.1. First Generation Photosensitizers 18
1.4.2. The Second Generation of Photosensitizers 19
1.4.3. The Third Generation Photosensitizers 22
References 25

Chapter II Synthesis and Photodynamic Studies of Novel meso-substituted Benzo[b]thiophene Porphyrins 31
Abstract 31
2.0. Introduction 33
2.1. Results 37
2.1.1. Synthesis and structural characterization of 5, 10, 15, 20-Tetrakis(Benzo[b]thiophene)porphyrin (BTP) 38
2.1.2. Synthesis and structural characterization of 5, 10, 15, 20–Tetrakis(7-sulfonatobenzo[b]thiophene)porphyrin (SBTP) 41
2.1.3. Photophysical properties of BTP and SBTP 45
2.1.4. Cytotoxicity and photocytotoxicity of SBTP 49
2.1.5. Subcellular localization of SBTP 51
2.1.6. Cellular uptake property of SBTP 53
2.1.7. Intracellular ROS generation of SBTP under photodynamic action 55
2.1.8. High-content cell death dynamics 57
2.1.9. Studies on intrinsic and extrinsic apoptotic pathways 60
2.1.10. DNA fragmentation assay 62
2.2.0. Discussion 65
2.3.0. Conclusions 72
2.4.0. Materials and methods 73
2.4.1. General methods 73
2.4.2. Synthesis of 5, 10, 15, 20 – Tetrakis(benzo[b]thiophene) porphyrin (BTP) 75
2.4.3. Synthesis of 5, 10, 15, 20 – Tetrakis (3-sulfonatobenzo[b]thiophene) porphyrin (SBTP) 76
2.4.4. MTT assay 77
2.4.5. Intracellular uptake of SBTP by MCF-7 cells 78
2.4.6. Intracellular localization assay 78
2.4.7. Intracellular ROS generation 79
2.4.8. High-content screening assay 79
2.4.9. Intrinsic/extrinsic apoptotic pathway studies 80
2.5.0. DNA fragmentation assay 81
References 82
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dc.formatapplication/pdf-
dc.format.extent2577870 bytes-
dc.format.mediumapplication/pdf-
dc.language.isoen-
dc.publisher서울대학교 대학원-
dc.subject약학과 약품분석학전공-
dc.subject.ddc615-
dc.titleSynthesis of 5, 10, 15, 20-Tetrakis(7-sulfanatobenzo[b]thiophene) Porphyrin for Mitochondria and DNA Targeted Photodynamic Therapy-
dc.title.alternative미토콘드리아 및 DNA 타겟 광역동 치료를 위한 술폰산벤조티오핀 포피린 합성-
dc.typeThesis-
dc.description.degreeDoctor-
dc.citation.pages105-
dc.contributor.affiliation약학대학 약학과-
dc.date.awarded2016-02-
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