本論文主要研究銥和銠卟啉絡合物與鹵代苯 (ArX, X = Cl, Br, I)的碳-鹵鍵(Ar-X)的斷裂反應及其應用。本論文分為四個部分:(1)銠卟啉絡合物與鹵代苯(ArX, X = Cl, Br, I)之間的碳-鹵鍵(Ar-X)斷裂反應;(2)氟氯化苯的碳-氟鍵(Ar-F)與碳-氯鍵(Ar-Cl)斷裂的競爭反應;(3)氟取代基對金屬(銥和銠)-芳香碳(M-Ar)鍵強弱的影響;以及(4)銥卟啉氟硼荧絡合物的合成。 / 第一部分闡述了銠卟啉絡合物(Rh(ttp)Cl)與鹵代苯(ArX, X = Cl, Br, I) 之間的碳-鹵鍵 (Ar-X) 斷裂反應以及反應機理。在鹼性條件下,無論富電子還是缺電子的鹵代苯都能與Rh(ttp)Cl反應,生成Ar-X鍵斷裂的產物──銠卟啉芳基絡合物(Rh(ttp)Ar) 。機理研究顯示, Rh(ttp)Cl 首先與氫氧根離子反應生成Rh(ttp)OH,進而通過二聚反應生成[Rh(ttp)]₂。[Rh(ttp)]₂在加熱條件下與Rh(ttp)自由基可以互相轉化,產生的Rh(ttp)自由基與鹵代苯進行原位取代反應,生成銠卟啉芳基絡合物(Rh(ttp)Ar)和鹵素自由基。鹵素自由基可以和另一個Rh(ttp)自由基反應生成Rh(ttp)X,在氫氧根離子存在的條件下,Rh(ttp)X將再次轉化為Rh(ttp)OH繼續反應。 / 第二部分描述了氟氯化苯中碳-氟鍵(Ar-F)與碳-氯鍵(Ar-Cl)斷裂的競爭反應。機理研究顯示碳-氟鍵(Ar-F)斷裂的中間體是M(por)⁻,而碳-氯鍵(Ar-Cl)斷裂的中間體是MII(por)。因此,我們可以通過改變反應條件而控制生成物。例如,在較低溫度下和強鹼性的極性溶劑中,以M(por)⁻前體作為反應物,可以獲得較多的碳-氟鍵(Ar-F)斷裂的產物;而在較高溫度下和弱鹼性的非極性溶劑中,可以獲得較多的碳-氯鍵(Ar-Cl)斷裂的產物。 / 第三部分敘述了間位氟取代基對金屬-芳香碳(M-Ar)鍵的增強作用。有間位氟取代基的金屬(銥,銠)卟啉芳基絡合物(M(ttp)ArF)是最穩定的同分異構體。在250°C條件下,當反應30天後,Ir(ttp)C₆H₄F的三個異構體達到平衡狀態,其鄰位:間位:對位的比例大約為0:5:1。理論計算的結果也顯示Ir(ttp)(3-fluorophenyl)相對Ir(ttp)(2-fluorophenyl)和Ir(ttp)(4-fluorophenyl)有更低的能量。氟取代基在鄰位時,氟與卟啉之間空間位阻較大,減弱了金屬-芳香碳(M-Ar)鍵的鍵能。與氟取代基在對位相比,在間位時具有更好的吸電子效應,從而增加了金屬-芳香碳(M-Ar)鍵的極性,增強了金屬-芳香碳(M-Ar)鍵鍵能。 / 第四部分描述了利用碳-鹵鍵 (Ar-X) 的斷裂,合成銥卟啉氟硼荧絡合物的反應。銥卟啉氟硼荧絡合物的產率可以達到70%。銥卟啉氟硼荧絡合物在生物成像和放射療法都有潛在的應用。銥卟啉氟硼荧絡合物是用金屬自由基與氟硼荧反應合成的。 / This thesis focuses on the reaction scopes, mechanistic investigations and applications of base-promoted aryl carbon-halogen (Ar-X) bond cleavage with iridium and rhodium porphyrin complexes. This thesis is divided into four parts: (1) Ar-X (X = Cl, Br, I) bond cleavage with Rh(ttp)Cl; (2) competitive Ar-F and Ar-Cl bond cleavage with iridium and rhodium porphyrins; (3) fluorine substituent effect on the M-Ar (M = Ir, Rh) bond strength; and (4) synthesis of iridium porphyrin BODIPY complexes. / Part I describes the reaction scopes and mechanism of Ar-X (X = I, Br, Cl) bond cleavage with Rh(ttp)Cl (ttp = 5,10,15,20-tetratolylporphyrinato dianion). Under basic conditions, both electron-rich and electron-deficient ArX undergo Ar-X bond cleavage to give Rh(ttp)Ar in good yields. [with diagram] / The mechanistic investigations suggest that RhIII(ttp)Cl first undergoes ligand substitution by OH- to give RhIII(ttp)OH, which forms [RhII(ttp)]₂ through reductive dimerization. RhII(ttp) radical, which is in equilibrium with [RhII(ttp)]₂, cleaves the Ar-X (X = I, Br, Cl) bond through metalloradical ipso-substitution and gives RhIII(ttp)Ar and X radical. X radical recombines with another RhII(ttp) radical to generate RhIII(ttp)X, which gives back RhIII(ttp)OH through ligand substitution by OH-. [with diagram] / Part II describes the competitive Ar-F and Ar-X (X = Cl, Br) bond cleavage reactions of fluorochlorobenzenes with iridium and rhodium porphyrin complexes. Mechanistic studies suggest that M(por)⁻ is the intermediate for the Ar-F bond cleavage while MII(por) is the intermediate for the Ar-X bond cleavage. By taking advantage of the difference in mechanisms of the Ar-F and Ar-X bond cleavages, the selectivity of bond cleavage can be controlled by varying the reaction conditions. The Ar-F bond cleavage is favored in a polar solvent with a stronger base at lower temperatures with M(por)⁻ precursor, and the Ar-X bond cleavage is favored under non-polar conditions with a weaker base and at higher temperatures. [with diagram] / Part III describes the meta-fluorine substituent effect on strengthening the M-Ar (M = Ir, Rh) bond of M(ttp)ArF. M(ttp)ArF with meta-fluorine substituent are the most stable isomers among the isomeric Ar-H bond cleavage products. At 250 °C for 30 days, the three isomers of Ir(ttp)C₆H₄F reached an equilibrium with o : m : p = 0 : 5 : 1. The theoretical calculations also suggest that Ir(ttp)(3-fluorophenyl) is of lower energy than Ir(ttp)(2-fluorophenyl) and Ir(ttp)(4-fluorophenyl). The ortho-fluorine substituent exhibits steric effect which weakens the M-Ar bond. The meta-fluorine, which is more electron-withdrawing than para-fluorine, enhances the polarity of the M-C(ipso) bond and thus strengthens the M-Ar bond. [with diagram] / Part IV describes the application of Ar-I bond cleavage with Ir(ttp)(CO)Cl in synthesizing iridium porphyrin boron-dipyrromethene (BODIPY) complexes, which are potential photosensitizers for biological imaging and photodynamic therapy. The clinically interested iridium porphyrin BODIPY complexes have been prepared by a radical process of metalloradical with BODIPY. [with diagram] / Detailed summary in vernacular field only. / Detailed summary in vernacular field only. / Detailed summary in vernacular field only. / Detailed summary in vernacular field only. / Detailed summary in vernacular field only. / Qian, Yingying. / Thesis (Ph.D.) Chinese University of Hong Kong, 2014. / Includes bibliographical references. / Abstracts also in Chinese.
Identifer | oai:union.ndltd.org:cuhk.edu.hk/oai:cuhk-dr:cuhk_1077677 |
Date | January 2014 |
Contributors | Qian, Yingying (author.), Chan, Kin Shing , 1958- (thesis advisor.), Chinese University of Hong Kong Graduate School. Division of Chemistry, (degree granting institution.) |
Source Sets | The Chinese University of Hong Kong |
Language | English, Chinese |
Detected Language | English |
Type | Text, bibliography, text |
Format | electronic resource, electronic resource, remote, 1 online resource (xiv, 274 leaves) : illustrations (some color), computer, online resource |
Rights | Use of this resource is governed by the terms and conditions of the Creative Commons “Attribution-NonCommercial-NoDerivatives 4.0 International” License (http://creativecommons.org/licenses/by-nc-nd/4.0/) |
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