Multi-component reactions for the synthesis of current spiro-quinoxaline pyrrolizidine carboxylates via [3+2] cycloaddition reactions

被引:0
作者
Shinde, Sundar S. [1 ]
Deokar, Dipak B. [1 ]
Laha, Soumi [2 ]
Bhaskar, S. Uday [2 ]
Sridhar, B. [3 ]
Likhar, Pravin R. [1 ]
机构
[1] CSIR Indian Inst Chem Technol, Catalysis & Fine Chem Dept, Uppal Rd, Hyderabad 500007, India
[2] Malla Reddy Engn Coll Autonomous, Hyderabad 500010, Telengana, India
[3] CSIR Indian Inst Chem Technol, XRay Crystallog Ctr, Hyderabad 500007, India
来源
ARKIVOC | 2024年
关键词
Ninhydrin; o-phenylenediamine; L-proline; alkynes; DERIVATIVES; REGIO;
D O I
10.24820/ark.5550190.p012.282
中图分类号
O62 [有机化学];
学科分类号
070303 ; 081704 ;
摘要
A novel series of multi-component reactions (MCRs) has been devised for the synthesis of spiro-quinoxaline pyrrolizine compounds using ninhydrin, o-phenylenediamine, proline, and propiolate esters via a [3+2] cycloaddition process. This efficient one-pot sequential four-component synthesis demonstrates high performance in acetonitrile, yielding spiro-quinoxaline pyrrolizine derivatives with remarkable efficiency. Spiro-quinoxaline pyrrolizine structures represent versatile molecular frameworks with potential applications in drug discovery, showcasing intriguing features for scaffold diversification.
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页数:13
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共 28 条
[1]   An expedient microwave assisted regio-and stereoselective synthesis of spiroquinoxaline pyrrolizine derivatives and their AChE inhibitory activity [J].
Akondi, Adinarayana Murthy ;
Mekala, Sowmya ;
Kantam, Mannepalli Lakshmi ;
Trivedi, Rajiv ;
Chowhan, L. Raju ;
Das, Amitava .
NEW JOURNAL OF CHEMISTRY, 2017, 41 (02) :873-878
[2]   Pyrrolizines: Promising scaffolds for anticancer drugs [J].
Belal, Amany ;
El-Gendy, Bahaa El-Dien M. .
BIOORGANIC & MEDICINAL CHEMISTRY, 2014, 22 (01) :46-53
[3]   Mitomycin C: a clinical update [J].
Bradner, WT .
CANCER TREATMENT REVIEWS, 2001, 27 (01) :35-50
[4]   Facile synthesis of active antitubercular, cytotoxic and antibacterial agents: a Michael addition approach [J].
Chande, MS ;
Verma, RS ;
Barve, PA ;
Khanwelkar, RR ;
Vaidya, RB ;
Ajaikumar, KB .
EUROPEAN JOURNAL OF MEDICINAL CHEMISTRY, 2005, 40 (11) :1143-1148
[5]   Potential anticancer activity of naturally occurring and semisynthetic derivatives of aculeatins A and B from Amomum aculeatum [J].
Chin, Young-Won ;
Salim, Angela A. ;
Su, Bao-Ning ;
Mi, Qiuwen ;
Chai, Hee-Byung ;
Riswan, Soedarsono ;
Kardono, Leonardus B. S. ;
Ruskandi, Agus ;
Farnsworth, Norman R. ;
Swansonj, Steven M. ;
Yinghorn, A. Douglas .
JOURNAL OF NATURAL PRODUCTS, 2008, 71 (03) :390-395
[6]  
Frank R., 2008, US. Pat., Patent No. 20080269271
[7]   Decaspirones F-I, bioactive secondary metabolites from the saprophytic fungus Helicoma viridis [J].
Hu, Hejiao ;
Guo, Huijuan ;
Li, Erwei ;
Liu, Xingzhong ;
Zhou, Yuguang ;
Che, Yongsheng .
JOURNAL OF NATURAL PRODUCTS, 2006, 69 (12) :1672-1675
[8]   Cremastrine, a pyrrolizidine alkaloid from Cremastra appendiculata [J].
Ikeda, Y ;
Nonaka, H ;
Furumai, T ;
Igarashi, Y .
JOURNAL OF NATURAL PRODUCTS, 2005, 68 (04) :572-573
[9]   Synthesis, physicochemical and anticonvulsant properties of new N-phenylamino derivatives of 2-azaspiro[4.4]nonane- and [4.5]decane-1,3-diones:: Part V [J].
Kaminski, Krzysztof ;
Obniska, Jolanta ;
Dybala, Malgorzata .
EUROPEAN JOURNAL OF MEDICINAL CHEMISTRY, 2008, 43 (01) :53-61
[10]   A new synthetic approach to pyrrolo[3,2-b]indoles via regioselective formation of pyrrole and intramolecular C-N coupling [J].
Karkhelikar, Manjusha V. ;
Rao, Vijay V. ;
Shinde, Sundar S. ;
Likhar, Pravin R. .
TETRAHEDRON LETTERS, 2016, 57 (43) :4803-4806
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