Crystal structural studies of destripeptide (B28-B30) insulin

Single crystals of destripeptide (B28-B30) insulin (DTRI) in three forms were obtained by hanging-drop vapor diffusion method. Form 1 belongs to P21 space group with cell parameters a-4.77 nm, b=6.19 nm, c=6.12 nm, β=110.3°. Form 2 belongs to P4122 or P4322 space group with cell parameters a= 6.45 nm, c=12.07 nm. Form 3 belongs to P212121 space group with cell parameters a=4.98 nm, b=5.16 nm, c=10.06 nm. The structure of form 1 crystal was determined by molecular replacement method and refined at 0.23 nm resolution. The R-factor of the final model is 18.8% with r.m.s. deviations of 0.001 5 nm and 3.3?for the bond lengths and the bond angles, respectively. Studies on the crystal structure show that the removal of B28 Pro has brought DTRI structural changes which made it dissociate more easily than native insulin although DTRI can still form a hexamer.     

Rhythmische Abscheidung von Stearinsäure aus alkoholischer und ätherischer Lösung

Kurze Zusammenfassung Stearins?ure scheidet sich aus hei?er alkoholischer L?sung (100 g in 70 ccm) und aus ges?ttigter ?therischer L?sung in Form von konzentrischen Ringen aus. Ein Versuch, diese Bildung zu erkl?ren, nimmt das Wechselspiel zwischen fortschreitender Abkühlung und freiwerdender Kristallisationsw?rme als ma?gebend an.     

Effects of 2-Hydroxypropyl-b-cyclodextrin on Polymorphic Transition of Chlorpropamide in Various Conditions: Temperature, Humidity and Moulding Pressure

The amorphous complex of 2-hydroxypropyl--cyclodextrin (HP--CyD) with an oral hypoglycemic agent, chlorpropamide (CPM), in a molar ratio of 1:1 was prepared by the spray-drying method. The effects of storage (temperature and humidity) and moulding pressure on the polymorphic transition of CPM in HP--CyD matrix were investigated, in comparison with those of the CPM polymorphs, Form A (stable form) and Form C (metastable form). The formation of an amorphous complex of CPM with HP--CyD was confirmed by powder X-ray diffractometry and differential scanning calorimetry. During storage at various temperature and humidity conditions, the metastable Form C of CPM converted to the stable Form A, where the conversion proceeded according to the Jander equation with an activation energy of 51 kJ/mol (25–60–°C) and a reaction-order of 1.55 with respect to water content (relative humidity (RH) 20–75%). No polymorphic transition of Form A crystals was observed under the experimental conditions. In the case of the amorphous HP--CyD complex, Form C crystals were slowly produced, but the further conversion of the resulting Form C to Form A was markedly suppressed in HP--CyD matrix. Upon compression (2000kg/cm²), Forms A and C were converted to amorphous CPM in a major portion and Forms C and A, respectively, in a minor portion. The polymorphic transition behavior was clearly reflected in the dissolution rate of CPM, i.e., (1) the dissolution rate was in the order of HP--CyD complex (Form C) Form A, and (2) the dissolution rate of Forms A and C after the compression increased because of the conversion to amorphous state, while the complex maintained the fast dissolving property even after the compression. The results indicated that HP--CyD is useful not only for converting crystalline CPM to an amorphous substance, but also for maintaining the metastable form with fast dissolution rate, Form C, over a long period.     

Crystal forms of a capsaicin derivative analgesic DA-5018

DA-5018 is a new capsaicin derivative and has analgesic effect. The objective of this work was to investigate the existence of polymorphs and pseudopolymorphs of DA-5018 and the transformation of crystal forms. Eight crystal forms of DA-5018 have been isolated by recrystallization and characterized by powder X-ray diffractometry (PXRD), differential scanning calorimetry (DSC), and thermogravimetric analysis (TG). The PXRD and DSC patterns of the eight crystal forms were different respectively. In the dissolution studies in simulated intestinal fluid at 37±0.5°C, the solubility of Form 2 was the highest. And the solubility in water decreased in rank order: Form 2>Form 3>Form 1>Form 5>Form 7>Form 4>Form 6>Form 8. Eight crystal forms were shown to have a good physical stability at room temperature for 60 days.     

Use of isothermal microcalorimetry in pharmaceutical preformulation studies,Part I. Monitoring crystalline phase transitions

Solid-state transformation kinetics of two crystal forms of a synthetic tetrapeptide was monitored by isothermal microcalorimetry and complementary solid-state analytical techniques. Form B, the crystal form obtained from the synthetic process transformed to Form D upon exposure to higher relative humidity conditions (>60% RH). The transformation occurred rapidly at higher temperature, and relative humidities. An intermediate phase of very low crystallinity (amorphous-like phase) was observed when transformation was slow. Form D was observed to be physically stable at higher relative humidities and thus the preferred crystal form for development. Exposure of Form B to high relative humidity was the only process through which Form D was obtained. Optimal conditions for transformation of Form B to Form D were determined by microcalorimetric experiments and were used for larger scale processing of Form B to Form D.     

Über die katalytische Hydrierung von o-Chinondiacetaten

Zusammenfassung Durch Hydrierung von methylsubstituierten o-Chinondiacetaten gelingt es, reine Brenzcatechinmonoacetate zu erhalten. In mehreren Fällen tritt im Laufe der Hydrierung Umesterung ein; d. h. es liegt der ursprüngliche Oxosauerstoff in Form einer Acetatgruppierung vor. Es wird aber auch ein Fall beschrieben, bei dem diese Umesterung nicht eintritt.Herrn Prof. Dr. tech.A. Brukl zum 70. Geburtstag gewidmet (F. W.).     

Polymorphic forms of bisoprolol fumarate

Bisoprolol fumarate is a beta blocker-type drug substance which has been well known for several decades. However, no relevant data can be found in the literature about its crystal polymorphism. The purpose of this paper was to present two anhydrous forms (Form I and Form II) and a hydrate of bisoprolol fumarate substance. Crystalline forms were studied by various solid-state analytical methods: Fourier transform infrared (FT-IR) spectroscopy, X-ray powder diffraction (XRPD), dynamic vapor sorption (DVS) and thermoanalytical methods (thermogravimetry and differential scanning calorimetry). Thermodynamic stability and solubility of the presented polymorphs were also investigated. Both FT-IR and XRPD methods were found to be suitable for the characterization of the different crystal structures. Thermoanalytical measurements showed that (1) Form I and Form II own clearly different melting points and (2) both Form II and hydrate forms can transform into Form I at higher temperature values. Results of the DVS measurements prove that both Form I and Form II became metastable under extremely humid conditions (>?80% RH) and converted into the hydrate. Thermodynamic stability studies showed that Form I and Form II polymorphs are in enantiotropic relationship with an enantiotropic point at about 40–45 °C. Solubility studies indicated that all of the prepared forms are highly soluble, and no difference was found between them. Considering the recommendations of the corresponding International Conference of Harmonization guideline, it can be stated that no specification is required for crystal polymorphism in case of this substance.

     

Thermodynamic Analysis of DSC Data for Acetaminophen Polymorphs

This article provides a thermodynamic analysis of DSC data for acetaminophen polymorphic forms I and II by measurement of heat capacity. Form I is found to have lower heat capacity and free energy and hence better stability than Form II down to at least –30°C. The transition temperature below which Form II becomes more stable was determined to be less than –120°C. Form I is more stable than Form II as a consequence of its higher entropy, since its crystallographic packing arrangement is of larger energy. This revised version was published online in August 2006 with corrections to the Cover Date.     

Thermal behavior of orthorhombic polymorphs I and II of spironolactone

Investigation into the thermal behavior of orthorhombic Forms I and II of spironolactone, by means of differential scanning calorimetry and high-resolution X-ray powder diffraction, showed that Form I melts then recrystallizes into Form II at 373–393 K, i.e. in the temperature range within which high resolution X-ray powder diffration showed that Form I transforms into Form II. Refinements of the lattice parameters of the two forms indicated that Form I is denser than Form II in the range from 298 K up to the temperature at which it melts.     

Massenspektrometrische Nitrat-Spurenbestimmung in Gew?ssern

Ohne Zusammenfassung

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Mass-spectrometric determination of traces of nitrate in waters

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Herrn Prof. Dr. W. Fresenius zum 70. Geburtstag gewidmet; in ausführlicher Form bereits im Geburtstagsheft Fresenius Z Anal Chem (1983) 315:454 veröffentlicht

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Der Deutschen Forschungsgemeinschaft sowie dem Bundesministerium für Forschung und Technologie danken wir für die finanzielle Unterstützung.     

Thermal Properties of Binary Mixtures of β-Cyclodextrin with Carbamazepine Polymorphs

The thermal behaviour of binary mixtures between β-cyclodextrin (β-CD) and either carbamazepine polymorphic Form I (CBZ I), Form III (CBZ III) or dihydrate was investigated in order to assess possible interactions of CBZ solid phases with β-CD. Physical mixtures and kneaded binaries of β-CD and different CBZ crystal forms were studied by differential scanning calorimetry, thermogravimetric analysis and hot stage microscopy. The pattern of transition of CBZ Form III into Form I is strongly influenced by β-CD. The liquid-solid transition is practically absent when anhydrous CBZ/β-CD mixes are tested, as a consequence of an interaction between β-CD and liquid CBZ that hinders CBZ recrystallisation as Form I occurring after CBZ Form III melting. Water loss on heating of CBZ dihydrate in the presence of β-CD leads in all cases to the formation of CBZ Form I. This revised version was published online in August 2006 with corrections to the Cover Date.     

Solid state of a new flavonoid derivative DA-6034

DA-6034 is a new synthetic flavonoid known to possess anti-inflammatory activity. The objective of this work was to investigate the existence of polymorphs and pseudopolymorphs of DA-6034. Six crystal forms, one hydrate form and five solvates, of DA-6034 have been isolated by recrystallization and characterized by differential scanning calorimetry (DSC), thermogravimetric analysis (TG), and powder X-ray diffractometry (PXRD). From the DSC and TG data it was confirmed that Form 1 is monohydrate; Form 2 is DMSO solvate; Form 3 is 1/2 DMSO solvate; Form 4 is 1/2 methyl ethyl ketone solvate; Form 5 is 1.5 H₂O, 1/2 acetic acid solvate; Form 6 is 1/2 H₂O, 1/4 butanol solvate. The PXRD patterns of the six crystal forms were different respectively. In the dissolution studies in pH 6.8 ± 0.05 buffer at 37 ± 0.5 °C, the solubility of solvates was higher than that of Form 1.     

A new polymorph of 2,6‐diaminopyridine

2,6‐Diaminopyridine (26‐DAP, C₅H₇N₃) is a common intermediate in the synthesis of aromatic azo chromophores, which are widespread in the dyes and pigments industry. Sublimation of commercial 26‐DAP powder yielded a new polymorph, denoted Form II, which grew as colorless orthorhombic needles. Recrystallization from acetone or toluene also yielded Form II as the major phase. Thermal analysis shows that Form II is a less stable polymorph and it converts upon heating at 335 K to the previously reported Form I.     

Conformal transition of form II to form I in poly(L-proline) and the aggregation of form I. I. Acetic acid–propanol solvent system

The conformational transition of Form II → Form I of Poly-L-proline and the intermolecular aggregation of the product Form I during and after the transition in the HOAc-propanol mixture solvent were studied, the ratio of HOAc:propanol being changed as 1:9, 1:6, and 1:4 v/v. For the study, the viscosity, light scattering, and dynamic light scattering of the system were measured. The experimental results exhibit that the concentration of Form II promotes the end-to-end type aggregation during and after the transition Form II → I. The extent of the aggregation is reduced in the order of the ratios of HOAc/propanol 1:9, 1:6, and 1:4 v/v. The end-to-end type aggregation is also reduced at higher temperatures. It was also observed that the end-to-end type aggregation occurs abruptly and strongly after the transition of Form II → I occurred to some extent. The point of the abrupt occurrence depends on the solvents and temperature. The light scattering and translational diffusion-coefficient measurements showed also similar phenomena. It was also observed that the side-by-side type aggregation occurs when the initial concentration of Form II of poly-L-proline is relatively small, and the transition temperature is relatively high (35 and 45°C). All the above mentioned experimental results are explained by a simple principle described in the text.     

X-ray structural studies on two forms of β-cyclodextrin barbital complexes

The crystal structures of two forms of -cyclodextrin barbital complexes (Form I and Form II) were investigated by X-ray analysis. In Form I crystal, two -cyclodextrin(-CyD) molecules including two barbital molecules form a dimeric structure by the hydrogen bonds among their secondary hydroxyl groups. The unit cell volume of Form II is about twice as large as that of Form I and there exist two -CyD dimers in Form II. Although the (Host)/(Guest) ratio is 1/1, only one barbital molecule can be found in Form II at the present stage. The sinilarities and differences between the two crystal structures are mainly discussed here.     

Thermal behaviour of melt crystallized phenylbutazone

In the DSC curves, the melting point of phenylbutazone Form A was affected by the heating rate (first heat cycle). The DSC curves of the melt crystallized phenylbutazone (second heat cycle) showed the endothermic peaks of both Form C and Form A. The change in the first heat cycle of either the heating rate, the upper temperature limit, or the isothermal hold period at the upper temperature limit affected the value of the area ratio between the endothermic peaks of the two polymorphs in the DSC curves of the melt crystallized phenylbutazone. It was therefore suggested that the value of the area ratio is related to the energy supplied to the melt phenylbutazone in the first heat cycle. According to this hypothesis, the energy level that the melt should reach to crystallize as the metastable Form C should be higher than the essential one to crystallize as the stable Form A.

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Zusammenfassung Bei der Aufname der DSC-Kurven wird der Schmelzpunkt von Phenylbutazon Form A durch die Aufheizgeschwindigkeit beeinflusst (erster Aufheizzyklus). Die DSC-Kurven des aus der Schmelze kristallisierten Phenylbutazon (zweiter Aufheizzyklus) zeigt beide endothermen Peaks der Form C und Form A.Eine Veränderung der Aufheizgeschwindigkeit, der oberen Temperaturgrenze oder der isothermen Wartezeit auf der oberen Temperaturgrenze des ersten Aufheizzyklus beeinflussen das Verhältnis der Flächen der endothermen Peaks der beiden polymorhen Formen in der DSC Kurve des aus der Schmelze kristallisierten Phenylbutazons. Es wird angenommen, daß der Wert für das Verhältnis der Flächen eine Funktion der im ersten Aufheizzyklus für das geschmolzene Phenylbutazon aufgewendeten Energie ist. In Übereinstimmung mit dieser Hypothese müßte das Energieniveau, welches die Schmelze erreichen muß, um als metastabile Form C zu kristallisieren, höher liegen als jenes, bei der sie als stabile Form A kristallisiert.

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This work was possible by a grant of the Ministero della Pubblica Istruzione, Rome, Italy.     

Organic Crystals with Response to Multiple Stimuli: Mechanical Bending,Acid-Induced Bending and Heating-Induced Jumping

Multiple stimuli-responsive molecular crystals are attracting extensive attentions due to their potential as smart materials, such as molecular machines, actuators, and sensors. However, the task of giving a single crystal multiple stimuli-responsive properties remains extremely challenging. Herein, we found two polymorphs (Form O and Form R) of a Schiff base compound, which could respond to multiple stimuli (external force, acid, heat). Form O and Form R have different elastic deformability, which can be attributed to the differences in the molecular conformation, structural packing and intermolecular interactions. Moreover, both polymorphs exhibit reversible bending driven by volatile acid vapor, which we hypothesize is caused by reversible protonation reaction of imines with formic acid. In addition, jumping can be triggered by heating due to the significant anisotropic expansion. The integration of reversible bending and jumping into one single crystal expands the application scope of stimuli-responsive crystalline materials.     

Polymorphs of the antiviral drug ganciclovir

Ganciclovir (GCV; systematic name: 2‐amino‐9‐{[(1,3‐dihydroxypropan‐2‐yl)oxy]methyl}‐6,9‐dihydro‐1H‐purin‐6‐one), C₉H₁₃N₅O₄, an antiviral drug for treating cytomegalovirus infections, has two known polymorphs (Forms I and II), but only the structure of the metastable Form II has been reported [Kawamura & Hirayama (2009). X‐ray Struct. Anal. Online , 25 , 51–52]. We describe a successful preparation of GCV Form I and its crystal structure. GCV is an achiral molecule in the sense that its individual conformers, which are generally chiral objects, undergo fast interconversion in the liquid state and cannot be isolated. In the crystalline state, GCV exists as two inversion‐related conformers in Form I and as a single chiral conformer in Form II. This situation is similar to that observed for glycine, also an achiral molecule, whose α‐polymorph contains two inversion‐related conformers, while the γ‐polymorph contains a single conformer that is chiral. The hydrogen bonds are exclusively intermolecular in Form I, but both inter‐ and intramolecular in Form II, which accounts for the different molecular conformations in the two polymorphs.     

The use of high-speed differential scanning calorimetry (Hyper-DSC™) to study the thermal properties of carbamazepine polymorphs

The thermal properties of two polymorphs of the drug carbamazepine, Forms I and III, were studied using high-speed differential scanning calorimetry (DSC). Previously, accurate determination of the heat enthalpy of fusion of Form III has not been possible using DSC at typical heating rates, due to concurrent exothermic recrystallisation to the higher-melting Form I. Here, it is demonstrated that heating rates of 250° C/min altered the kinetics of the melting transition of Form III such that this concurrent exothermic recrystallisation was inhibited. This allowed direct measurement of the enthalpy of the melting endotherm for Form III from a single transition. The enthalpy of this transition was found to be 109.5 J/g. Further investigations were then performed to test the utility of this technique in quantifying relative amounts of Forms I and III in mixtures of the two polymorphs. It was demonstrated that a limit of detection of 1% (w/w) was possible in this system. However, accurate quantification was not possible due to seeding effects initiating recrystallisation to Form I in these mixtures, even at these elevated heating rates. The utility of this novel technique as a fast analytical tool for studying the polymorphic behaviour of metastable polymorphs has been successfully demonstrated.     

Reassessment of paracetamol orthorhombic Form III and determination of a novel low‐temperature monoclinic Form III‐m from powder diffraction data

Paracetamol [N‐(4‐hydroxyphenyl)acetamide, C₈H₉NO₂] has several polymorphs, just like many other drugs. The most stable polymorphs, denoted Forms I and II, can be obtained easily and their crystal structures are known. Crystals of the orthorhombic, less stable, room‐temperature Form III are difficult to grow; they need a special recipe to crystallize and suffer from severe preferred orientation. A crystal structure model of Form III has been proposed and solved from a combination of structure prediction and powder X‐ray diffraction (PXRD) [Perrin et al. (2009). Chem. Commun. 22 , 3181–3183]. The final R_wp value of 0.138 and the corresponding considerable residual trace were reasons to check its validity. A new structure determination of Form III using new high‐resolution PXRD data led to a final R_wp value of 0.042 and an improvement of the earlier proposed model. In addition, a reversible phase transition was found at 170–220 K between the orthorhombic Form III and a novel monoclinic Form III‐m. The crystal structure of Form III‐m has been determined and refined from PXRD data to a final R_wp value of 0.059.