Different forms of antiparallel stacking of hydrogen-bonded antidromic rings in the solid state: polymorphism with virtually the same unit cell and two-dimensional isostructurality with alternating layers

As a continuation of a systematic structural analysis of 2‐hydroxycycloalkanecarboxylic acids and their carboxamide analogs, the effects of antidromic rings [Jeffrey & Saenger (1991). Hydrogen Bonding in Biological Structures. Berlin, Heidelberg: Springer Verlag] upon the layer stacking of cyclo...

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Veröffentlicht in:	Acta crystallographica. Section B, Structural science Structural science, 2004-12, Vol.60 (6), p.755-762
Hauptverfasser:	Kálmán, Alajos, Fábián, László, Argay, Gyula, Bernáth, Gábor, Cs. Gyarmati, Zsuzsanna
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Sprache:	eng
Schlagworte:	Aliphatic, non-condensed and condensed benzenic, and alicyclic compounds Condensed matter: structure, mechanical and thermal properties Crystalline state (including molecular motions in solids) Crystallographic aspects of phase transformations pressure effects Exact sciences and technology isostructurality Organic compounds Physics Polymorphism solvent effects Structure of solids and liquids crystallography Structure of specific crystalline solids
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container_title	Acta crystallographica. Section B, Structural science
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creator	Kálmán, Alajos Fábián, László Argay, Gyula Bernáth, Gábor Cs. Gyarmati, Zsuzsanna
description	As a continuation of a systematic structural analysis of 2‐hydroxycycloalkanecarboxylic acids and their carboxamide analogs, the effects of antidromic rings [Jeffrey & Saenger (1991). Hydrogen Bonding in Biological Structures. Berlin, Heidelberg: Springer Verlag] upon the layer stacking of cyclopentane and cycloheptane derivatives are compared. Determination of the structure of trans‐2‐hydroxycycloheptanecarboxylic acid (2) led to the discovery of two polymorphs with virtually the same unit cell [Kálmán et al. (2003). J. Am. Chem. Soc.125, 34–35]. (i) The layer stacking of the antidromic rings for the whole single crystal is antiparallel (2b). (ii) The antidromic rings and the 21 axis are parallel (2a), consequently the domains of the single crystal must be antiparallel. While their polymorphism is solvent‐controlled, they illustrate a novel form of two‐dimensional isostructurality. Antiparallel layer stacking is again demonstrated by trans‐2‐hydroxycycloheptanecarboxamide (3) (space group Pbca). It is built up from layers isostructural with those in the homologous trans‐2‐hydroxycyclopentanecarboxamide (4) [Kálmán et al. (2001). Acta Cryst. B57, 539–550], but in this structure (space group Pca21) the layers are stacked in parallel mode. Similar to (2a) and (2b), the antiparallel layer stacking in (3) versus their parallel array in (4) illustrates the two‐dimensional isostructurality with alternating layer orientations. Although (3) and (4) display isostructurality, they are not isomorphous.
doi_str_mv	10.1107/S0108768104024553
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While their polymorphism is solvent‐controlled, they illustrate a novel form of two‐dimensional isostructurality. Antiparallel layer stacking is again demonstrated by trans‐2‐hydroxycycloheptanecarboxamide (3) (space group Pbca). It is built up from layers isostructural with those in the homologous trans‐2‐hydroxycyclopentanecarboxamide (4) [Kálmán et al. (2001). Acta Cryst. B57, 539–550], but in this structure (space group Pca21) the layers are stacked in parallel mode. Similar to (2a) and (2b), the antiparallel layer stacking in (3) versus their parallel array in (4) illustrates the two‐dimensional isostructurality with alternating layer orientations. 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Gyarmati, Zsuzsanna</creatorcontrib><title>Different forms of antiparallel stacking of hydrogen-bonded antidromic rings in the solid state: polymorphism with virtually the same unit cell and two-dimensional isostructurality with alternating layers</title><title>Acta crystallographica. Section B, Structural science</title><addtitle>Acta Cryst. B</addtitle><description>As a continuation of a systematic structural analysis of 2‐hydroxycycloalkanecarboxylic acids and their carboxamide analogs, the effects of antidromic rings [Jeffrey & Saenger (1991). Hydrogen Bonding in Biological Structures. Berlin, Heidelberg: Springer Verlag] upon the layer stacking of cyclopentane and cycloheptane derivatives are compared. Determination of the structure of trans‐2‐hydroxycycloheptanecarboxylic acid (2) led to the discovery of two polymorphs with virtually the same unit cell [Kálmán et al. (2003). J. Am. Chem. Soc.125, 34–35]. (i) The layer stacking of the antidromic rings for the whole single crystal is antiparallel (2b). (ii) The antidromic rings and the 21 axis are parallel (2a), consequently the domains of the single crystal must be antiparallel. While their polymorphism is solvent‐controlled, they illustrate a novel form of two‐dimensional isostructurality. Antiparallel layer stacking is again demonstrated by trans‐2‐hydroxycycloheptanecarboxamide (3) (space group Pbca). It is built up from layers isostructural with those in the homologous trans‐2‐hydroxycyclopentanecarboxamide (4) [Kálmán et al. (2001). Acta Cryst. B57, 539–550], but in this structure (space group Pca21) the layers are stacked in parallel mode. Similar to (2a) and (2b), the antiparallel layer stacking in (3) versus their parallel array in (4) illustrates the two‐dimensional isostructurality with alternating layer orientations. Although (3) and (4) display isostructurality, they are not isomorphous.</description><subject>Aliphatic, non-condensed and condensed benzenic, and alicyclic compounds</subject><subject>Condensed matter: structure, mechanical and thermal properties</subject><subject>Crystalline state (including molecular motions in solids)</subject><subject>Crystallographic aspects of phase transformations; pressure effects</subject><subject>Exact sciences and technology</subject><subject>isostructurality</subject><subject>Organic compounds</subject><subject>Physics</subject><subject>Polymorphism</subject><subject>solvent effects</subject><subject>Structure of solids and liquids; crystallography</subject><subject>Structure of specific crystalline solids</subject><issn>0108-7681</issn><issn>1600-5740</issn><fulltext>true</fulltext><rsrctype>article</rsrctype><creationdate>2004</creationdate><recordtype>article</recordtype><recordid>eNqFkc1u1DAUhSMEokPhAdggb2AXuJ78uezKTGmRKlgARXQT-eemY-rYwXYY8o48FA4Z0QULVpZ8vnN8rJNlTym8pBSaVx-BAmtqRqGEdVlVxb1sRWuAvGpKuJ-tZjmf9aPsUQjfAKCkDB5mRzSxZcGaVfZrq7sOPdpIOuf7QFxHuI164J4bg4aEyOWttjezsJuUdzdoc-GsQvUHTDe9lsQnJBBtSdwhCc5oNTsjviaDM1Pv_LDToSd7HXfkh_ZxTOnTAvMeyWh1JBKNSZmKxL3Lle7RBu0sN0QHF6IfZRxTKR2nJYabiN7yOJczfEIfHmcPOm4CPjmcx9nnt2efNhf55Yfzd5vTy1yWtKZ5yYUQTNRNvWa1pLwrOUcQqBivBJx0WFUyKUo0UAuBlK4LiYIpUYMCkGVxnL1Ycgfvvo8YYtvrMLfnFt0Y2rqB6qRgVQLpAkrvQvDYtYPXPfdTS6GdJ2z_mTB5nh3CR9GjunMcNkvA8wPAg-Sm89xKHe64ukhZDSSOLdxeG5z-_3J7-vXN9qwCSpM1X6w6RPz518r9bfpb0VTtl_fn7eb66mJ7VRbtdfEbPfDKVw</recordid><startdate>200412</startdate><enddate>200412</enddate><creator>Kálmán, Alajos</creator><creator>Fábián, László</creator><creator>Argay, Gyula</creator><creator>Bernáth, Gábor</creator><creator>Cs. 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B</addtitle><date>2004-12</date><risdate>2004</risdate><volume>60</volume><issue>6</issue><spage>755</spage><epage>762</epage><pages>755-762</pages><issn>0108-7681</issn><eissn>1600-5740</eissn><coden>ASBSDK</coden><abstract>As a continuation of a systematic structural analysis of 2‐hydroxycycloalkanecarboxylic acids and their carboxamide analogs, the effects of antidromic rings [Jeffrey & Saenger (1991). Hydrogen Bonding in Biological Structures. Berlin, Heidelberg: Springer Verlag] upon the layer stacking of cyclopentane and cycloheptane derivatives are compared. Determination of the structure of trans‐2‐hydroxycycloheptanecarboxylic acid (2) led to the discovery of two polymorphs with virtually the same unit cell [Kálmán et al. (2003). J. Am. Chem. Soc.125, 34–35]. (i) The layer stacking of the antidromic rings for the whole single crystal is antiparallel (2b). (ii) The antidromic rings and the 21 axis are parallel (2a), consequently the domains of the single crystal must be antiparallel. While their polymorphism is solvent‐controlled, they illustrate a novel form of two‐dimensional isostructurality. Antiparallel layer stacking is again demonstrated by trans‐2‐hydroxycycloheptanecarboxamide (3) (space group Pbca). It is built up from layers isostructural with those in the homologous trans‐2‐hydroxycyclopentanecarboxamide (4) [Kálmán et al. (2001). Acta Cryst. B57, 539–550], but in this structure (space group Pca21) the layers are stacked in parallel mode. Similar to (2a) and (2b), the antiparallel layer stacking in (3) versus their parallel array in (4) illustrates the two‐dimensional isostructurality with alternating layer orientations. 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subjects	Aliphatic, non-condensed and condensed benzenic, and alicyclic compounds Condensed matter: structure, mechanical and thermal properties Crystalline state (including molecular motions in solids) Crystallographic aspects of phase transformations pressure effects Exact sciences and technology isostructurality Organic compounds Physics Polymorphism solvent effects Structure of solids and liquids crystallography Structure of specific crystalline solids
title	Different forms of antiparallel stacking of hydrogen-bonded antidromic rings in the solid state: polymorphism with virtually the same unit cell and two-dimensional isostructurality with alternating layers
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