細菌肽聚醣衍生物之合成與功能性探討

游庭昀; Ting-Yun You

Please use this identifier to cite or link to this item: http://tdr.lib.ntu.edu.tw/jspui/handle/123456789/91494

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???org.dspace.app.webui.jsptag.ItemTag.dcfield???	Value	Language
dc.contributor.advisor	羅禮強	zh_TW
dc.contributor.advisor	Lee-Chiang Lo	en
dc.contributor.author	游庭昀	zh_TW
dc.contributor.author	Ting-Yun You	en
dc.date.accessioned	2024-01-28T16:15:16Z	-
dc.date.available	2024-01-29	-
dc.date.copyright	2024-01-27	-
dc.date.issued	2023	-
dc.date.submitted	2023-08-04	-
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dc.identifier.uri	http://tdr.lib.ntu.edu.tw/jspui/handle/123456789/91494	-
dc.description.abstract	有別於直接作用於細菌的抗生素，細菌細胞壁之降解分子片段被證實可以誘發宿主免疫機制並清除細菌，具有抵禦病原體感染、甚至是具抗藥性的細菌的潛力，是一個亟需發展的領域。細菌細胞壁組成多元且特性複雜，而其共通主要成分為肽聚醣。為了研究這些與肽聚醣相關的議題，在本文中，透過多步驟化學合成的設計，製備了系統性結構改質之肽聚醣分子群及其前驅物。本論文研究分為兩個部分：第一部分、針對胞壁肽系統性化學結構改質之自噬活化劑篩選以應用於殺菌能力之探討　　為了對抗細菌感染，透過小分子引發宿主先天性免疫機制作為新的治療策略開始受到關注。透過天然肽聚醣特定片段──胞壁二肽(MDP)引發自噬進而清除細菌的研究，證明了分子誘導之細胞自噬現象與殺菌能力有高度相關。為了解具有殺菌能力之分子結構，這裡我們延續實驗室所開發的化學合成及天然物純化策略，由細菌純化出天然成分如肽聚醣及磷壁酸，以及由(i)單醣中間體、(ii)正交保護雙醣中間體，(iii)二胺基庚二酸(meso-DAP)改質骨架之三肽作衍生化的化學方法，系統性製備一系列胞壁肽衍生物之分子庫。透過細胞實驗建立自噬表現分析之細胞平台，以檢測細胞壁相關衍生物分子庫潛在的自噬活化劑。接著進一步經由沙門氏桿菌清除實驗篩選出相較天然物MDP具有更佳殺菌能力之化合物6、 9及 15，並以微量熱泳動技術探討配體-受器作用力鑑定其模式識別受體及機制，我們初步選擇以與肽聚醣相關性高的人體核苷酸結合寡聚化區域受器(NOD-like receptors)進行實驗，發現化合物15是經由NOD1引發自噬及細菌清除，而化合物6及9則透過其他機制達到細菌清除的效果，透過NOD1及NOD2專一性NF-κB活性測試驗證，提出分子結構、NF-κB及自噬三者之可能關聯性。第二部分、發展以胞壁肽為基礎之二聚體衍生物應用於人類受體NOD2活性探討　　MDP及其衍生物經研究證實具備生物活性，並應用於對抗細菌感染或腫瘤。受到人類受體NOD2引發寡聚化機制的模型啟發，我們以胞壁肽為骨架設計了一系列具有不同位向和長度的新型同源二聚體MDP複合物，並評估其對NOD2活性的影響。經由改善現有的合成方法在MDP醣六號位及胜肽引進胺基，並進行不同長度衍生化得到同源二聚MDP複合物，同時透過細胞實驗分析其長度對NOD2的活性影響，發現分子量1000的間隔為最佳長度，並在後續以微量熱泳動進行配體－受體作用力測試，我們觀察到二聚體複合物36c (1000)與NOD2的解離常數約在12 μM，略優於MDP。此外，我們初步示範將此分子設計方法應用於嫁接複合物及螢光基團並證實其對NOD2的作用力及功能，以期未來應用於其他藥物的嫁接。	zh_TW
dc.description.abstract	Unlike antibiotics that directly act on bacteria, the bio-degraded fragments of bacterial cell wall induce host immune responses to generate pathogen clearance. This is another emerging field for developing a new treatment against bacterial infection even including drug-resistant bacteria. The bacterial cell wall has diverse composition and complex characteristics, of which primary common component is peptidoglycan (PGN). To further study these PGN-related issues, in this thesis, the key lies in the design and synthesis of PGN-associated molecules and their precursors through multi-step synthesis to get systematically modified muropeptides with well-defined structures to investigate the structural requirements for their bioactivity. This research is divided into two parts: Part I. Discovery of muropeptide-derived molecules as autophagy inducers by cellular phenotypic approach to study bacterial clearance (Chapter 2) To develop new therapeutic strategies against bacterial infection, the small molecule-based immunobiotics that can induce host immune responses have gained attention. Through the mechanism studies of muramyl dipeptide (MDP), the strong correlation between autophagy and antibacterial ability was demonstrated in autophagy-mediated bacterial clearance. To elucidate the structural requirements for antibacterial ability, a series of bacterial cell wall-related and muropeptide-derived molecules was prepared by isolation methods or chemical approaches. These PGN derivatives were evaluated toward autophagic responses via a cellular phenotypic approach, and 7 potential autophagy inducers were found through derived from the modification of 3 primary hits, including 2 muropeptides and 1 tripeptide-based molecule. Further in vitro studies demonstrated that compounds 6, 9, and 15, showed a more efficient clearance of intracellular S. typhimurium than the current inducer MDP. In mechanism studies by microscale thermophoresis and receptor-specific NF-κB assay, compound 15 induced autophagy and subsequent bacterial clearance via NOD1 signaling pathway. However, compounds 6 and 9 might activate additional pathways leading to subsequent autophagy-mediated bacterial clearance. These results provide initial insights into the interplay among molecular structures, NF-κB, and autophagy. Part II. Preparation of dimeric MDP analogs with a variant spacer and their functional study toward NOD2 (Chapter 3) MDP and its analogs has received particular attention due to their antibacterial or anti-tumor activities. Inspired by NOD2-mediated oligomerization, we designed novel homo-dimeric MDP conjugates with different orientations and spacer lengths using a reverse genetic approach. It is revealed that 36c with proper orientation and optimized spacer of 1000 Da in a molecular weight exhibited the best activity toward NOD2-specific NF-κB activity. In the subsequent experiments, we conducted ligand-receptor interaction studies using microscale thermophoresis (MST). Through this technique, we observed that the binding affinity between dimeric 36c and NOD2 is approximately 12 μM, slightly better than that of MDP. This molecular design approach shows potential for future applications in conjugation of other drugs, such as antibody drug conjugates.	en
dc.description.provenance	Submitted by admin ntu (admin@lib.ntu.edu.tw) on 2024-01-28T16:15:16Z No. of bitstreams: 0	en
dc.description.provenance	Made available in DSpace on 2024-01-28T16:15:16Z (GMT). No. of bitstreams: 0	en
dc.description.tableofcontents	口試委員會審定書 i 誌謝 ii 摘要 iii ABSTRACT v CONTENTS vii LIST OF FIGURES x LIST OF TABLES xiii LIST OF SCHEMES xiv ABBREVIATION xv Chapter 1 Introduction 1 1.1 Bacterial cell wall composition and peptidoglycan 1 1.2 Host-microbe interaction 3 1.2.1 Pattern recognition receptors (PRRs) 3 1.2.2 Host innate immune defense 3 1.3 Small molecule-based immunobiotics 4 1.3.1 Current methods to assess antibacterial ability 5 Chapter 2 Discovery of muropeptide-derived molecules as autophagy inducers by cellular phenotypic approach to study bacterial clearance 6 2.1 Background 6 2.1.1 Mechanism of bacterial clearance 6 2.1.2 Autophagy screening platform 7 2.1.3 Current cell wall-related autophagy inducers 8 2.1.4 Current Limitations 8 2.1.5 Motivation 9 2.2 Results and Discussion 9 2.2.1 The strategy for identification of novel synthetic immunobiotics 9 2.2.2 Initial bio-evaluation by autophagy 10 2.2.3 Preparation of muropeptides 14 2.2.4 Bio-evaluation of diversity-oriented molecules by autophagy 16 2.2.5 Further assessments on bacterial clearance against S. typhimurium 19 2.2.6 Analysis of ligand-receptor interaction and NF-κB activity study 20 2.3 Sub-summary and perspectives 22 Chapter 3 Synthesis and functional evaluation of dimeric muropeptide analogues with varied spacers 23 3.1 Background 23 3.1.1 The interaction of NOD2 and its ligands 23 3.1.2 Tripartite structure of NOD2 and its activation mechanism 23 3.1.3 Previous reported modified MDPs 24 3.1.4 Previous reported modified MDP conjugates for immuno-therapeutics 27 3.1.5 Current controversy: the conflicting studies on 6-modified MDPs 28 3.1.6 Motivation and design 29 3.2 Results and Discussion 31 3.2.1 The strategy for developing novel MDP conjugates 31 3.2.2 Preparation of core A 32 3.2.3 Alternative route: preparation of core A 34 3.2.4 Bio-evaluation of different cores toward NOD2 via NF-κB assay 36 3.2.5 Preparation of dimeric MDP conjugates 37 3.2.6 Bio-evaluation of dimers and monomers with different spacers via NF-κB assay 40 3.2.7 Bio-evaluation of MDP conjugates 42 3.2.8 The binding influence between NOD2 and dimeric muropeptides 44 3.3 Sub-summary and perspectives 45 Chapter 4 Conclusions 47 Chapter 5 Experimental section 48 5.1 General information 48 5.1.1 MALDI-TOF mass analysis 48 5.2 Preparation and Characterization of Compounds 49 5.2.1 General procedure for Boc deprotection 49 5.2.2 General procedure for basic hydrolysis of ester 49 5.2.3 General procedure for the preparation of dimers 36b-e and monomers 37b-e 68 5.3 Materials and Biological Methods 77 5.3.1 Immunofluorescence 77 5.3.2 Macrophage killing assay 77 5.3.3 Plasmids 78 5.3.4 Protein expression 78 5.3.5 Microscale thermophoresis analysis 78 5.3.6 Measurement of NF-κB transcriptional activity 79 5.3.7 Statistical Analysis 79 REFERENCES 80 APPENDIX A 86 APPENDIX B 116	-
dc.language.iso	en	-
dc.subject	肽聚醣	zh_TW
dc.subject	同源二聚體	zh_TW
dc.subject	微量熱泳動	zh_TW
dc.subject	鍵結常數	zh_TW
dc.subject	沙門氏桿菌	zh_TW
dc.subject	細菌清除	zh_TW
dc.subject	細胞表現分析	zh_TW
dc.subject	核轉錄因子	zh_TW
dc.subject	二胺基庚二酸	zh_TW
dc.subject	先天性免疫	zh_TW
dc.subject	核苷酸結合寡聚化區域受器 (NOD)	zh_TW
dc.subject	自噬現象	zh_TW
dc.subject	胞壁肽	zh_TW
dc.subject	細菌細胞壁	zh_TW
dc.subject	binding affinity	en
dc.subject	bacterial cell wall	en
dc.subject	peptidoglycan (PGN)	en
dc.subject	muropeptides	en
dc.subject	immunobiotics	en
dc.subject	MDP	en
dc.subject	autophagy	en
dc.subject	NOD	en
dc.subject	bacterial clearance	en
dc.subject	cellular phenotypic approach	en
dc.subject	NF-kB	en
dc.subject	homodimer	en
dc.title	細菌肽聚醣衍生物之合成與功能性探討	zh_TW
dc.title	Synthesis and Functional Study of Bacterial Peptidoglycan Derivatives	en
dc.type	Thesis	-
dc.date.schoolyear	111-2	-
dc.description.degree	碩士	-
dc.contributor.coadvisor	鄭偉杰	zh_TW
dc.contributor.coadvisor	Wei-Chieh Cheng	en
dc.contributor.oralexamcommittee	陳斯婷;鄭婷仁	zh_TW
dc.contributor.oralexamcommittee	Szu-Ting Chen;Ting-Jen Cheng	en
dc.subject.keyword	細菌細胞壁,肽聚醣,胞壁肽,自噬現象,核苷酸結合寡聚化區域受器 (NOD),先天性免疫,二胺基庚二酸,核轉錄因子,細胞表現分析,細菌清除,沙門氏桿菌,鍵結常數,微量熱泳動,同源二聚體,	zh_TW
dc.subject.keyword	bacterial cell wall,peptidoglycan (PGN),muropeptides,immunobiotics,MDP,autophagy,NOD,bacterial clearance,cellular phenotypic approach,NF-kB,homodimer,binding affinity,	en
dc.relation.page	120	-
dc.identifier.doi	10.6342/NTU202303011	-
dc.rights.note	同意授權(限校園內公開)	-
dc.date.accepted	2023-08-08	-
dc.contributor.author-college	理學院	-
dc.contributor.author-dept	化學系	-
dc.date.embargo-lift	2028-08-04	-
Appears in Collections:	化學系

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