Amide-Functionalized Naphthyridines on a RhII-RhII Platform: Effect of Steric Crowding, Hemilability, and Hydrogen-Bonding Interactions on the Structural Diversity and Catalytic Activity of Dirhodium(II) Complexes

Amide-Functionalized Naphthyridines on a RhII-RhII Platform: Effect of Steric Crowding, Hemilability, and Hydrogen-Bonding Interactions on the Structural Diversity and Catalytic Activity of Dirhodium(II) Complexes

Ferrocene‐amide‐functionalized 1,8‐naphthyridine (NP) based ligands {[(5,7‐dimethyl‐1,8‐naphthyridin‐2‐yl)amino]carbonyl}ferrocene (L1H) and {[(3‐phenyl‐1,8‐naphthyridin‐2‐yl)amino]carbonyl}ferrocene (L2H) have been synthesized. Room‐temperature treatment of both the ligands with Rh2(CH3COO)4 produc...

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Veröffentlicht in:Chemistry : a European journal 2014-12, Vol.20 (50), p.16537-16549
Hauptverfasser: Sarkar, Mithun, Daw, Prosenjit, Ghatak, Tapas, Bera, Jitendra K.
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CH activation
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rhodium
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description Ferrocene‐amide‐functionalized 1,8‐naphthyridine (NP) based ligands {[(5,7‐dimethyl‐1,8‐naphthyridin‐2‐yl)amino]carbonyl}ferrocene (L1H) and {[(3‐phenyl‐1,8‐naphthyridin‐2‐yl)amino]carbonyl}ferrocene (L2H) have been synthesized. Room‐temperature treatment of both the ligands with Rh2(CH3COO)4 produced [Rh2(CH3COO)3(L1)] (1) and [Rh2(CH3COO)3(L2)] (2) as neutral complexes in which the ligands were deprotonated and bound in a tridentate fashion. The steric effect of the ortho‐methyl group in L1H and the inertness of the bridging carboxylate groups prevented the incorporation of the second ligand on the {RhII–RhII} unit. The use of the more labile Rh2(CF3COO)4 salt with L1H produced a cis bis‐adduct [Rh2(CF3COO)4(L1H)2] (3), whereas L2H resulted in a trans bis‐adduct [Rh2(CF3COO)3(L2)(L2H)] (4). Ligand L1H exhibits chelate binding in 3 and L2H forms a bridge‐chelate mode in 4. Hydrogen‐bonding interactions between the amide hydrogen and carboxylate oxygen atoms play an important role in the formation of these complexes. In the absence of this hydrogen‐bonding interaction, both ligands bind axially as evident from the X‐ray structure of [Rh2(CH3COO)2(CH3CN)4(L2H)2](BF4)2 (6). However, the axial ligands reorganize at reflux into a bridge‐chelate coordination mode and produce [Rh2(CH3COO)2(CH3CN)2(L1H)](BF4)2 (5) and [Rh2(CH3COO)2(L2H)2](BF4)2 (7). Judicious selection of the dirhodium(II) precursors, choice of ligand, and adaptation of the correct reaction conditions affords 7, which features hemilabile amide side arms that occupy sites trans to the Rh–Rh bond. Consequently, this compound exhibits higher catalytic activity for carbene insertion to the CH bond of substituted indoles by using appropriate diazo compounds, whereas other compounds are far less reactive. Thus, this work demonstrates the utility of steric crowding, hemilability, and hydrogen‐bonding functionalities to govern the structure and catalytic efficacyof dirhodium(II,II) compounds. The introduction of structural diversity into RhII–RhII complexes is achieved with amide‐functionalized 1,8‐naphthyridine ligands modulated by steric crowding, bridging carboxylate groups that are labile, and hydrogen‐bonding interactions between the amide hydrogen and carboxylate oxygen atoms. The amide functionality shows hemilabile behavior at the axial sites, thus making the dirhodium complex effective for the catalytic CH functionalization of indoles with appropriate diazo compounds (see scheme).
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Room‐temperature treatment of both the ligands with Rh2(CH3COO)4 produced [Rh2(CH3COO)3(L1)] (1) and [Rh2(CH3COO)3(L2)] (2) as neutral complexes in which the ligands were deprotonated and bound in a tridentate fashion. The steric effect of the ortho‐methyl group in L1H and the inertness of the bridging carboxylate groups prevented the incorporation of the second ligand on the {RhII–RhII} unit. The use of the more labile Rh2(CF3COO)4 salt with L1H produced a cis bis‐adduct [Rh2(CF3COO)4(L1H)2] (3), whereas L2H resulted in a trans bis‐adduct [Rh2(CF3COO)3(L2)(L2H)] (4). Ligand L1H exhibits chelate binding in 3 and L2H forms a bridge‐chelate mode in 4. Hydrogen‐bonding interactions between the amide hydrogen and carboxylate oxygen atoms play an important role in the formation of these complexes. In the absence of this hydrogen‐bonding interaction, both ligands bind axially as evident from the X‐ray structure of [Rh2(CH3COO)2(CH3CN)4(L2H)2](BF4)2 (6). However, the axial ligands reorganize at reflux into a bridge‐chelate coordination mode and produce [Rh2(CH3COO)2(CH3CN)2(L1H)](BF4)2 (5) and [Rh2(CH3COO)2(L2H)2](BF4)2 (7). Judicious selection of the dirhodium(II) precursors, choice of ligand, and adaptation of the correct reaction conditions affords 7, which features hemilabile amide side arms that occupy sites trans to the Rh–Rh bond. Consequently, this compound exhibits higher catalytic activity for carbene insertion to the CH bond of substituted indoles by using appropriate diazo compounds, whereas other compounds are far less reactive. Thus, this work demonstrates the utility of steric crowding, hemilability, and hydrogen‐bonding functionalities to govern the structure and catalytic efficacyof dirhodium(II,II) compounds. The introduction of structural diversity into RhII–RhII complexes is achieved with amide‐functionalized 1,8‐naphthyridine ligands modulated by steric crowding, bridging carboxylate groups that are labile, and hydrogen‐bonding interactions between the amide hydrogen and carboxylate oxygen atoms. The amide functionality shows hemilabile behavior at the axial sites, thus making the dirhodium complex effective for the catalytic CH functionalization of indoles with appropriate diazo compounds (see scheme).</description><identifier>ISSN: 0947-6539</identifier><identifier>EISSN: 1521-3765</identifier><identifier>DOI: 10.1002/chem.201402936</identifier><identifier>CODEN: CEUJED</identifier><language>eng</language><publisher>Weinheim: WILEY-VCH Verlag</publisher><subject>catalysis ; Chemistry ; CH activation ; hemilability ; hydrogen bonds ; Ligands ; naphthyridine ; rhodium</subject><ispartof>Chemistry : a European journal, 2014-12, Vol.20 (50), p.16537-16549</ispartof><rights>2014 WILEY‐VCH Verlag GmbH &amp; Co. KGaA, Weinheim</rights><rights>2014 WILEY-VCH Verlag GmbH &amp; Co. 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Eur. J</addtitle><description>Ferrocene‐amide‐functionalized 1,8‐naphthyridine (NP) based ligands {[(5,7‐dimethyl‐1,8‐naphthyridin‐2‐yl)amino]carbonyl}ferrocene (L1H) and {[(3‐phenyl‐1,8‐naphthyridin‐2‐yl)amino]carbonyl}ferrocene (L2H) have been synthesized. Room‐temperature treatment of both the ligands with Rh2(CH3COO)4 produced [Rh2(CH3COO)3(L1)] (1) and [Rh2(CH3COO)3(L2)] (2) as neutral complexes in which the ligands were deprotonated and bound in a tridentate fashion. The steric effect of the ortho‐methyl group in L1H and the inertness of the bridging carboxylate groups prevented the incorporation of the second ligand on the {RhII–RhII} unit. The use of the more labile Rh2(CF3COO)4 salt with L1H produced a cis bis‐adduct [Rh2(CF3COO)4(L1H)2] (3), whereas L2H resulted in a trans bis‐adduct [Rh2(CF3COO)3(L2)(L2H)] (4). Ligand L1H exhibits chelate binding in 3 and L2H forms a bridge‐chelate mode in 4. Hydrogen‐bonding interactions between the amide hydrogen and carboxylate oxygen atoms play an important role in the formation of these complexes. In the absence of this hydrogen‐bonding interaction, both ligands bind axially as evident from the X‐ray structure of [Rh2(CH3COO)2(CH3CN)4(L2H)2](BF4)2 (6). However, the axial ligands reorganize at reflux into a bridge‐chelate coordination mode and produce [Rh2(CH3COO)2(CH3CN)2(L1H)](BF4)2 (5) and [Rh2(CH3COO)2(L2H)2](BF4)2 (7). Judicious selection of the dirhodium(II) precursors, choice of ligand, and adaptation of the correct reaction conditions affords 7, which features hemilabile amide side arms that occupy sites trans to the Rh–Rh bond. Consequently, this compound exhibits higher catalytic activity for carbene insertion to the CH bond of substituted indoles by using appropriate diazo compounds, whereas other compounds are far less reactive. Thus, this work demonstrates the utility of steric crowding, hemilability, and hydrogen‐bonding functionalities to govern the structure and catalytic efficacyof dirhodium(II,II) compounds. The introduction of structural diversity into RhII–RhII complexes is achieved with amide‐functionalized 1,8‐naphthyridine ligands modulated by steric crowding, bridging carboxylate groups that are labile, and hydrogen‐bonding interactions between the amide hydrogen and carboxylate oxygen atoms. The amide functionality shows hemilabile behavior at the axial sites, thus making the dirhodium complex effective for the catalytic CH functionalization of indoles with appropriate diazo compounds (see scheme).</description><subject>catalysis</subject><subject>Chemistry</subject><subject>CH activation</subject><subject>hemilability</subject><subject>hydrogen bonds</subject><subject>Ligands</subject><subject>naphthyridine</subject><subject>rhodium</subject><issn>0947-6539</issn><issn>1521-3765</issn><fulltext>true</fulltext><rsrctype>article</rsrctype><creationdate>2014</creationdate><recordtype>article</recordtype><recordid>eNo9kVtv1DAQhSNEJZaWV54t8QJSU3yJnYS3Jd1LpHZBXFTEi-V1JhuXJF4cp234n_wfkl20LzOa0fnmSHOC4DXBVwRj-l5X0FxRTCJMUyaeBTPCKQlZLPjzYIbTKA4FZ-mL4GXX3WOMU8HYLPg7b0wB4bJvtTe2VbX5AwXaqH3lq8GZwrTQIdsihb5UeR5OBX2ulS-taz6gRVmC9siW6KsHZzTKnH0cmd0lWkNjarU1tfHDJVJtgdZD4ewO2vCjbScNytsRUgffg4evYLzjeu17p2p0bR7AdSN-oDPlVT340WM-Eg_TerS9Nq6yhembt3n-DmW22dfwBN1FcFaquoNX__t58H25-Jatw5tPqzyb34Q7SlIRggaxTZJSUMw4jxPOIYl1RGOgvEhLzLepTiIMJaTTrAmjQjMQkYqTlGJg58Gb4929s7976Ly8t70bv9hJImjCieARH1XpUfVoahjk3plGuUESLKfc5JSbPOUms_Xi9jSNbHhkTefh6cQq90uKmMVc3m1WcvVzc_eDLNfylv0D97WhRw</recordid><startdate>20141208</startdate><enddate>20141208</enddate><creator>Sarkar, Mithun</creator><creator>Daw, Prosenjit</creator><creator>Ghatak, Tapas</creator><creator>Bera, Jitendra K.</creator><general>WILEY-VCH Verlag</general><general>WILEY‐VCH Verlag</general><general>Wiley Subscription Services, Inc</general><scope>BSCLL</scope><scope>7SR</scope><scope>8BQ</scope><scope>8FD</scope><scope>JG9</scope><scope>K9.</scope></search><sort><creationdate>20141208</creationdate><title>Amide-Functionalized Naphthyridines on a RhII-RhII Platform: Effect of Steric Crowding, Hemilability, and Hydrogen-Bonding Interactions on the Structural Diversity and Catalytic Activity of Dirhodium(II) Complexes</title><author>Sarkar, Mithun ; Daw, Prosenjit ; Ghatak, Tapas ; Bera, Jitendra K.</author></sort><facets><frbrtype>5</frbrtype><frbrgroupid>cdi_FETCH-LOGICAL-g2196-ece6b88f6203557855e87c427e25d9f05b9c840efe95d9fc1326c3e64a78920e3</frbrgroupid><rsrctype>articles</rsrctype><prefilter>articles</prefilter><language>eng</language><creationdate>2014</creationdate><topic>catalysis</topic><topic>Chemistry</topic><topic>CH activation</topic><topic>hemilability</topic><topic>hydrogen bonds</topic><topic>Ligands</topic><topic>naphthyridine</topic><topic>rhodium</topic><toplevel>peer_reviewed</toplevel><toplevel>online_resources</toplevel><creatorcontrib>Sarkar, Mithun</creatorcontrib><creatorcontrib>Daw, Prosenjit</creatorcontrib><creatorcontrib>Ghatak, Tapas</creatorcontrib><creatorcontrib>Bera, Jitendra K.</creatorcontrib><collection>Istex</collection><collection>Engineered Materials Abstracts</collection><collection>METADEX</collection><collection>Technology Research Database</collection><collection>Materials Research Database</collection><collection>ProQuest Health &amp; Medical Complete (Alumni)</collection><jtitle>Chemistry : a European journal</jtitle></facets><delivery><delcategory>Remote Search Resource</delcategory><fulltext>fulltext</fulltext></delivery><addata><au>Sarkar, Mithun</au><au>Daw, Prosenjit</au><au>Ghatak, Tapas</au><au>Bera, Jitendra K.</au><format>journal</format><genre>article</genre><ristype>JOUR</ristype><atitle>Amide-Functionalized Naphthyridines on a RhII-RhII Platform: Effect of Steric Crowding, Hemilability, and Hydrogen-Bonding Interactions on the Structural Diversity and Catalytic Activity of Dirhodium(II) Complexes</atitle><jtitle>Chemistry : a European journal</jtitle><addtitle>Chem. Eur. J</addtitle><date>2014-12-08</date><risdate>2014</risdate><volume>20</volume><issue>50</issue><spage>16537</spage><epage>16549</epage><pages>16537-16549</pages><issn>0947-6539</issn><eissn>1521-3765</eissn><coden>CEUJED</coden><abstract>Ferrocene‐amide‐functionalized 1,8‐naphthyridine (NP) based ligands {[(5,7‐dimethyl‐1,8‐naphthyridin‐2‐yl)amino]carbonyl}ferrocene (L1H) and {[(3‐phenyl‐1,8‐naphthyridin‐2‐yl)amino]carbonyl}ferrocene (L2H) have been synthesized. Room‐temperature treatment of both the ligands with Rh2(CH3COO)4 produced [Rh2(CH3COO)3(L1)] (1) and [Rh2(CH3COO)3(L2)] (2) as neutral complexes in which the ligands were deprotonated and bound in a tridentate fashion. The steric effect of the ortho‐methyl group in L1H and the inertness of the bridging carboxylate groups prevented the incorporation of the second ligand on the {RhII–RhII} unit. The use of the more labile Rh2(CF3COO)4 salt with L1H produced a cis bis‐adduct [Rh2(CF3COO)4(L1H)2] (3), whereas L2H resulted in a trans bis‐adduct [Rh2(CF3COO)3(L2)(L2H)] (4). Ligand L1H exhibits chelate binding in 3 and L2H forms a bridge‐chelate mode in 4. Hydrogen‐bonding interactions between the amide hydrogen and carboxylate oxygen atoms play an important role in the formation of these complexes. In the absence of this hydrogen‐bonding interaction, both ligands bind axially as evident from the X‐ray structure of [Rh2(CH3COO)2(CH3CN)4(L2H)2](BF4)2 (6). However, the axial ligands reorganize at reflux into a bridge‐chelate coordination mode and produce [Rh2(CH3COO)2(CH3CN)2(L1H)](BF4)2 (5) and [Rh2(CH3COO)2(L2H)2](BF4)2 (7). Judicious selection of the dirhodium(II) precursors, choice of ligand, and adaptation of the correct reaction conditions affords 7, which features hemilabile amide side arms that occupy sites trans to the Rh–Rh bond. Consequently, this compound exhibits higher catalytic activity for carbene insertion to the CH bond of substituted indoles by using appropriate diazo compounds, whereas other compounds are far less reactive. Thus, this work demonstrates the utility of steric crowding, hemilability, and hydrogen‐bonding functionalities to govern the structure and catalytic efficacyof dirhodium(II,II) compounds. The introduction of structural diversity into RhII–RhII complexes is achieved with amide‐functionalized 1,8‐naphthyridine ligands modulated by steric crowding, bridging carboxylate groups that are labile, and hydrogen‐bonding interactions between the amide hydrogen and carboxylate oxygen atoms. The amide functionality shows hemilabile behavior at the axial sites, thus making the dirhodium complex effective for the catalytic CH functionalization of indoles with appropriate diazo compounds (see scheme).</abstract><cop>Weinheim</cop><pub>WILEY-VCH Verlag</pub><doi>10.1002/chem.201402936</doi><tpages>13</tpages></addata></record>
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subjects catalysis
Chemistry
CH activation
hemilability
hydrogen bonds
Ligands
naphthyridine
rhodium
title Amide-Functionalized Naphthyridines on a RhII-RhII Platform: Effect of Steric Crowding, Hemilability, and Hydrogen-Bonding Interactions on the Structural Diversity and Catalytic Activity of Dirhodium(II) Complexes
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