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Conjugation of CD40-binding peptide to glycol chitosan nanoparticle for localized delivery of tumor microenvironment modulator : 종양미세환경 조절인자의 국소적 전달을 위한 펩타이드 글라이콜 키토산 나노입자 결합체 연구

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dc.contributor.advisor김병수-
dc.contributor.author김소정-
dc.date.accessioned2017-07-14T02:24:23Z-
dc.date.available2017-07-14T02:24:23Z-
dc.date.issued2017-02-
dc.identifier.other000000142234-
dc.identifier.urihttps://hdl.handle.net/10371/122471-
dc.description학위논문 (석사)-- 서울대학교 대학원 : 바이오엔지니어링전공, 2017. 2. 김병수.-
dc.description.abstractCancer immunotherapy focuses on helping the immune system fight and control cancer and has rapidly progressed in the recent years. Agonistic CD40 monoclonal antibodies have been proposed as a new therapeutic method that enhances anticancer immunity by various mechanisms that alter the immune-suppressive tumor microenvironment. Previous researches have shown that CD40 binding not only causes tumor cell death but also activates macrophages to rapidly penetrate tumors, become tumoricidal and promote the reduction of tumor stroma. In this study, in order to avoid unwanted systemic side effects while maintaining the anti-tumor effects of CD40 antibody, localized delivery of agonistic CD40-binding peptide (CD40p) that mimics a portion of human CD40 ligand was achieved by conjugating CD40p to hydrophobically modified glycol chitosan nanoparticles (CD40p-CNP). The immunomodulatory nanoparticles showed cytotoxicity against human cancer cells and enhanced phagocytic activity of macrophages in vitro. Systemic injection of CD40p-CNP into tumor-bearing mice resulted in tumor-targeted delivery and significant inhibition of tumor growth that was similar to the effect of local injection of CD40p. Also, the potential of localized cancer immunotherapy via CD40-dependent mechanism that targets tumor stroma in the treatment of cancer was demonstrated. The primary findings of this study provide a new platform to treat cancer through localized delivery of immunotherapeutic agents via systemic injection of nanoparticle which can also be combined with other treatment modalities to facilitate its effect.-
dc.description.tableofcontents1. Introduction 1
2. Materials and methods 5
2.1 Materials 5
2.2 Synthesis of glycol chitosan nanoparticle 7
2.3 Conjugation of CD40-binding peptide to CNP 8
2.4 Labeling of peptide and nanoparticles with Cy5.5 9
2.5 Characterization of nanoparticles 11
2.6 Cell culture 12
2.7 In vitro uptake of nanoparticles by differentiated macrophages 13
2.8 In vitro toxicity 14
2.9 In vitro phagocytosis assay 15
2.10 In vivo and ex vivo imaging in tumor-bearing mice 16
2.11 Evaluation of in vivo tumor inhibition 17
2.12 Western blot analysis 18
2.13 Histological evaluation 20
3. Results and discussion 12
3.1 Formulation and characterization of CD40p-CNP 12
3.2 Cellular uptake of CD40p-CNP by differentiated macrophages 29
3.3 In vitro cytotoxicity analysis of CD40p-CNP 31
3.4 Activation of macrophages by CD40p-CNP 33
3.5 Phagocytosis of cancer cells by macrophages upon activation by CD40p- CNP 36
3.6 In vivo accumulation of CD40p-CNP in tumors 39
3.7 Inhibitory effect of CD40p-CNP on in vivo tumor growth 41
3.8 Histological analysis 43
4. Conclusion 45
5. References 46
요약 (국문초록) 51
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dc.formatapplication/pdf-
dc.format.extent1858698 bytes-
dc.format.mediumapplication/pdf-
dc.language.isoen-
dc.publisher서울대학교 대학원-
dc.subjectcancer immunotherapy-
dc.subjectCD40 binding peptide-
dc.subjectCD40 antibody-
dc.subjectglycol chitosan nanoparticle-
dc.subjecttumor microenvironment-
dc.subjecttumor-infiltrated lymphocytes-
dc.subjecttumor growth inhibition-
dc.subject.ddc660-
dc.titleConjugation of CD40-binding peptide to glycol chitosan nanoparticle for localized delivery of tumor microenvironment modulator-
dc.title.alternative종양미세환경 조절인자의 국소적 전달을 위한 펩타이드 글라이콜 키토산 나노입자 결합체 연구-
dc.typeThesis-
dc.description.degreeMaster-
dc.citation.pages60-
dc.contributor.affiliation공과대학 협동과정 바이오엔지니어링전공-
dc.date.awarded2017-02-
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