One Pot Synthesis of Bisphosphonate Esters: A Way to Synthesize Tetraphosphonate Esters

Abstract

Several methods for the preparation of symmetrical bisphosphonates of general type (RO)₂P(O)(R′OH)P(O)(OR)₂, have been developed, and investigated for their pharmacological. Pharmacological screening of these bisphosphonates have shown that these compounds have potent cardiovascular activity and are. potentialy useful in the treatment of hypertension. In this work we described of new method “one pot” for the synthesis of hydroxy bis and tetra phosphonates (I, II, III and IV).     

Hypepontine,a new quaternary alkaloid with antimicrobial properties

Abstract

New isoquinoline alkaloid hypepontine (1) together with a five known compounds, were identified in Hypecoum ponticum Velen, the partial synonym of Hypecoum procumbens L. The structure of the new substance was elucidated based on spectroscopic evidence. The tertiary and quaternary alkaloid mixtures as well as the isolated alkaloids were evaluated for their antibacterial and antifungal activity. The result revealed that the crude alkaloid mixture containing quaternary isoquinoline alkaloids showed potent antifungal and antibacterial activity.     

Synthesis of Novel Bisphosphonate Inhibitors of Phosphoglycerate Kinase (3-PGK) (E.C.2.7.2.3)

Abstract

Novel, aromatic bisphosphonates have been synthesised as non-systematic analogues of 1,3-bisphosphoglyceric acid (1,3-BPG). These incorporate non-scissile α-halo and α-methylene phosphonates and have submicromolar K _i values for 3 -PGK.     

Understanding the Charge Issues in Mono and di-Quaternary Ammonium Compounds for Their Determination by LC/ESI-MS/MS

Chromatographers often develop problems while optimizing a method for the quantification of quaternary ammonium compounds in ESI-MS/MS. Intransigency observed in quaternary ammonium compounds to undergo the classical molecular adduct formation [M+H]⁺ in ESI-MS/MS reduces confidence among chromatographers while working with unit mass resolution. In this study, we provide the evidence for an exceptional rule followed by mono- and di-quaternary ammonium compounds in ESI-MS/MS in the precursor ion formation. Under ESI conditions mono- and di-quaternary ammonium compounds form molecular ions with the formula of m ^q / z ^q rather than ( m + z )/ z . Formation of m ^q / 2 is observed for di-quaternary ammonium compounds in precursor ion scan and m ^q / 1 in product ion scan, if loss of one of the quaternary charge occurs during CID. In di-quaternary ammonium compounds, this process can also result in the formation of fragment ions with higher mass as compared to precursor ion. Hydrophilic interaction liquid chromatographic separation has been used to demonstrate the elution of quaternary ammonium compounds in a single run in the ESI-MS/MS. This work concludes that the analyst must realize and consider these charge issues while dealing with positively charged compounds in LC/ESI-MS/MS.     

通过三乙基铝促进的a-羟基环氧化合物的重排还原反应合成Madindoline母核片断——全取代环戊烯二酮单元

The fully substituted cyclopentenedione core of madindoline A （1） and B （2） as potent and selective inhibitor of IL-6 has been synthesized efficiently. The quaternary carbon center C-2＇ was constructed on the basis of a newly developed AIEt3-promoted tandem reductive rearrangement of α-hydroxy epoxides.     

Facile synthesis of highly functionalized novel pyrazolopyridones using oxoketene dithioacetal and their anti-HIV activity

A series of novel 3-amino-4,5-dihydro-6-methyl-4-oxo-N-aryl-1H-pyrazolo[4,3-c]pyridine-7-carboxamide have been synthesized starting from various oxoketene dithioacetals. The cyclocondensation reaction of 2-(bis(methylthio)methylene)-3-oxo-N-arylbutanamide 2a–w with cyanoacetamide using NaOiPr as base under reflux condition afforded novel highly functionalized pyridone 3a–w derivatives. Further, [3?+?2] cyclocondensation reaction of pyridones with hydrazine in the presence of alcohol was yielded pyrazolopyridones (23 nos) 4a–w with excellent yields. All newly synthesized compounds were evaluated for in vitro anti-HIV activity using MTT method. Most of these compounds have showed moderate to potent activity against HIV-1 (III_B) and HIV-2 (ROD) strains with an IC₅₀ ranging from >18 IC₅₀[µg/ml] to <100 IC₅₀[µg/ml]. Among them, compounds 4j and 4v were identified as the most promising compound for both types of HIV strains. (IC₅₀?=?18?µg/ml). Three compounds 4l, 4m, and 4p have been found potent anti-HIV 1 and 2 activity against MT-4 cells.     

Studies of Hydrous Zirconium Oxide. I. Thin-Layer Chromatography of Some Metal Ions on Hydrous Zirconium Oxide: Quantitative Separation of Bi(III) from Several other Metal Ions

Abstract

The analytical potentiality of hydrous zirconium oxide as an ionexchanger has been investigated by thin-layer chromatographic (TLC technique. Binder-free thin-layers of hydrous zirconium oxide are useful for 25 ternary and 12 quaternary separations. Quantitative separation of Bi (III) from some ternary and quaternary mixtures of metal ions has been achieved.     

Synthesis and NMR Spectroscopic Properties of C-Fluorinated Bisphosphonic Acids

Abstract

Fluorinated and halogenated bisphosphonates have gained widespread interests in chemistry, pharmacy and medicine. The concept of biochemical activity with metal-chelating agents has encouraged our research team to study synthesis, NMR and analytic chemistry of fluorinated aromatic and olefinic geminal bisphosphonates.     

The Synthesis of Diphenyl Phosphonate Analogues of α-Amino Acids as Enzyme Inhibitors

Abstract

α-Aminoalkylphosphonic acids are analogues of natural aminoacids and as such have been the subject of much research effort over past years¹. The diphenyl esters of α- aminoalkylphosphonic acids are particularly potent and show high selectivity as irreversible inhibitors of serine proteinases. Thus far, α-aminoalkylphosphonic acid ester analogues of a number of aliphatic- and aromatic aminoacids have been prepared including valine, phenylalanine, tryptophan, and tyrosine², and the basic aminoacids ornithine, lysine. etc.³. We have now also prepared the a-diphenyl phosphonate analogues of the acidic aminoacids, aspartic and glutamic⁴. These have been examined as potential inactivators of serine proteinases exhibiting a P₁ specificity for aspartate and glutamate, e.g. S. aureus V8 protease and granzyme B.     

New Bisphosphonates,Synthesis and Reactions

Abstract

The synthesis and reactions of new bisphosphonates with different substituents in α-position as well as a new type of trisphosphonate are described.     

Antioxidant phenolic compounds from the rhizomes of Astilbe rivularis

The rhizomes of Astilbe rivularis, commonly known as ‘Thulo Okhati’ are widely used in Nepal as tonic for uterine and menstrual disorders. In our preliminary study, the 70% MeOH extract of the rhizomes showed potent antioxidant activity. Hence, present study was aimed for the isolation of potent antioxidant constituents. Bergenin (1), 11-O-galloylbergenin (2), (+)-catechin (3), (?)-catechin (4), (?)-afzelechin (5), (?)-epiafzelechin (6) and 2-(β-D-glucopyranosyloxy)-4-hydroxylbenzenacetonitrile (7) were isolated from the rhizomes. Structures of these compounds were elucidated on the basis of spectroscopic methods. All these isolated compounds were evaluated for their in vitro antioxidant activity by 1,1-diphenyl-2-picrylhydrazyl (DPPH) radical scavenging assay. 11-O-Galloylbergenin (2), (+)-catechin (3), (?)-catechin (4), (?)-afzelechin (5) and (?)-epiafzelechin (6) showed potent antioxidant activity.     

A NEW PHASE TRANSFER CATALYST AND ITS APPLICATIONS IN ORGANIC TRANSFORMATIONS1*

ABSTRACT

A new quaternary ammonium bromide salt has been used for the first time in phase transfer catalysis (PTC) reactions such as oxidation of alcohols to carbonyl compounds, alkylation and esterification reactions. Improved yields and reduced reaction times have been achieved by this procedure.

     

The Design and Synthesis of Bone-Active Phosphinic Acid Analogues: 1. The Pyridylaminomethane Phosphonoalkylphosphinates

Abstract

The bisphosphonic acids and their salts, the bisphosphonates, have been the subject of study by a number of research groups for their marked ability to modulate bone metabolism. From a recent study of phosphinic acid isosteres, we have designed a novel related class of bone active agents, the pyridylaminomethane phosphonoaikylphosphinates I.     

HgII-containing MOFs constructed from bis-benzimidazole-based ligand with highly selective anion-exchange capacity

Two Hg(II)-containing metal–organic frameworks (MOFs) based on 1,1′-(1,5-pentanediyl)bis-1H-benzimidazole (pbbm), {[HgBr₂(pbbm)]?·?DMF} _n (1) and [HgI₂(pbbm)]₂ (2), have been constructed to explore new and potent ion-exchange materials. Single-crystal X-ray diffraction shows that 1 features a 1-D zigzag chain framework, while 2 presents a dimeric structure in which two Hg(II) cations are bridged by two pbbm ligands. The significant differences of these MOFs indicate that the counteranions have impact on assembling and structures of the resultant MOFs. Remarkably, coordinated Br^? in 1 can be replaced completely when the solid polymer is treated with an aqueous solution containing I^?. Confirmation of retention of structure is provided by FT-IR spectra and the XRPD pattern. The thermal stabilities of 1 and 2 have also been investigated.     

六～八元瓜环与三种N-苄基取代笼状客体的相互作用

合成了3种具有对不同瓜环选择性各异的双探针N-苄基取代笼状客体, 它们分别是N-苄基六次甲基四胺盐酸盐(1), N-苄基喹啉环啶盐酸盐(2), N-苄基-1,4-二氮杂双环[2.2.1]辛烷盐酸盐(3), 利用¹H NMR和MS等方法对这些客体进行了表征. ¹H NMR显示, 六元瓜环仅对这些客体的苄基探针部分具有选择性作用, 形成作用比为1∶1的不对称包结配合物; 七元瓜环对客体1和3的苄基探针部分具有选择性作用, 形成作用比为1∶1的不对称包结配合物, 而对客体2的笼状奎宁环啶基部分具有选择性作用, 也形成作用比为1∶1的包结配合物; 八元瓜环也仅对这些客体的苄基探针部分具有选择性作用, 形成作用比为1∶2的对称包结配合物.     

Facile expeditious one-pot synthesis and antifungal evaluation of disubstituted 1,2,3-triazole with two amide linkages

A library of twenty five amide linked 1,4-disubstituted 1,2,3-triazoles have been prepared through a facile expeditious synthetic protocol involving Cu(I) mediated cyclization of N-(2-methylbut-3-yn-2-yl)aromatic amides and in situ generated 2-azido-N-substituted propanamides. Structures of newly synthesized compounds (5a–5y) were confirmed by analytical techniques, such as FTIR, ¹H NMR, ¹³C NMR, and HRMS. In vitro antifungal activity was also examined against two fungal strains Candida albicans and Aspergillus niger by serial dilution method. The compounds 5?m and 5w exhibited appreciable potent activity.     

Synthesis,bioevaluation and molecular docking study of new piperazine and amide linked dimeric 1,2,3-triazoles

Abstract

In search of more potent new antitubercular agents, a library of novel piperazine tethered dimeric 1,2,3-triazoles were designed by assembling 1,2,3-triazoles and piperazine in a single molecular architectural framework. The titled compounds (3a–m) were synthesized by 1,3-dipolar cycloaddition of 1,4-di(prop-2-yn-1-yl)piperazine (1) and various azides (2a–m) using click chemistry approach with good yields. All the synthesized compounds (3a–m) have been screened for their in vitro antitubercular, antifungal and antioxidant activities against their respective strains. Among them, 3b, 3d, and 3i have revealed promising antitubercular activity against Mycobacterium tuberculosis (Mtb) H37Rv with MIC 12.5?µg/mL. Molecular docking results provided well-clustered solutions to the mode of binding for these molecules into the active site of Mtb enoyl reductase (InhA). In addition to this, most of synthesized compounds were found to have potential antifungal as well as antioxidant activity.     

Novel Bioreversible Prodrugs of Clodronate

Abstract

Clodronate (1) belongs to family of bisphosphonates which are used to inhibit mineralization of soft tissues as well as bone formation and resorption disorders.[I] The clinical use of bisphosphonates is limited due to their poor bióvailability which is mostly attributed to their hydrophilic structure. More lipophilic molecules are obtained if some or all of the anionic sites are converted to covalent bonds. We herein report a new prodrug serie for clodronate: the anhydrides 2 and 3. Previously we have reported that the simple alkyl esters 4 do not release clodronate via chemical or enzymatic hydrolysis.[2] The prepared new derivatives are stable in water (pH 5–7.5) but clodronate isrelased rapidly with enzymatic hydrolysis.     

Facile Synthesis of 1,4-Dihydropyridine Monocarboxylic Acids and Unsymmetric Dicarboxylates via Quaternary Ammonium Salts of 2-Aminoethyl 1,4-Dihydropyridine-3,5-dicarboxylates

Useful 1,4-dihydropyridine unsymmetric dicarboxylates [nitrendipine (1), nicardipine (2)] and monocarboxylic acid 4 were prepared from unsymmetric 2-aminoethyl methyl 1,4-dihydropyridine-3,5-dicarboxylates 2 and 3 via their corresponding quaternary ammonium salts 5–9.     

Concise and Efficient Synthesis of Highly Potent and Selective Dipeptidyl Peptidase II Inhibitors

Highly potent and selective DPP II inhibitors N′‐(4‐Chlorobenzyl)‐N′‐methyl‐4‐oxo‐4‐(1‐piperidinyl)‐1,3‐(S)‐butane‐diamine dihydrochloride 1 and N′‐(4‐chlorobenzyl)‐4‐oxo‐4‐(1‐piperidinyl)‐1,3‐(S)‐butanediamine dihydrochloride 2 have been efficiently synthesized starting from L‐glutamine. A short and high yielding route with simple isolation techniques has been disclosed.