ライフサイエンスコーパス: isatin

1 respectively, from the 5- and 1-positions of isatin.

2 the skeleton of the naturally occurring dye isatin.

3 dolines, indolin-2-ones, indolin-3-ones, and isatins.

4 iyama aldol reaction of 2-siloxyindoles with isatins.

5 -ones was synthesized from the corresponding isatins.

6 enyl)-3-phenylurea 9a,b to the corresponding isatin 10a-f in ethanol containing a quantitative amount

7 fluoro phenoxymethyl)-pyrrolidine-1-sulfonyl)isatin ((18)F-ICMT-11), has been developed for use in PE

8 in intermolecular [4+2] cycloadditions with isatins 2a-2f to form 2-oxindole spirolactones 3a-3l.

9 n patterns, and is applicable to unprotected isatins 2b-2f bearing free NH-functionalities.

10 ased around the lead compound NSC73306 (1, 1-isatin-4-(4'-methoxyphenyl)-3-thiosemicarbazone, 4.3-fol

11 Two of these analogues, 1-isatin-4-(4'-nitrophenyl)-3-thiosemicarbazone (22, 8.3-f

12 semicarbazone (22, 8.3-fold selective) and 1-isatin-4-(4'-tert-butyl phenyl)-3-thiosemicarbazone (32,

13 od for making isatoic anhydride-8-amide from isatin-7-carboxylic acid as a tool to easily produce a r

14 ing Lambert salt-initiated hydroarylation of isatin, a diverse array of monoarylated products, symmet

15 Moreover, the 7-position of isatin, a potential cytochrome P450 hydroxylation site,

16 FAD, and this ligand superimposed well with isatin, a reversible inhibitor of MAO-B, when the struct

17 Isatin, a specific ANP receptor antagonist, reversed ANP

18 e have synthesized a novel series of N-alkyl isatin acylhydrazone derivatives and have identified and

19 These novel 6-methoxy-N-alkyl isatin acylhydrazone derivatives exhibited high CB2 func

20 discovered and reported a series of N-alkyl isatin acylhydrazone derivatives that are potent CB2 ago

21 three-component reactions using substituted isatins, alpha-amino acids, and cyclopropenes.

22 3-functionalized 2-oxindoles by varying the isatin, amine, and alcohol components.

23 been established, which efficiently assembly isatins, amino-esters and 2,3-allenoate into enantioenri

24 0 ng/ml), ANP (1 pM to 1 micromol/L), and/or isatin, an ANP receptor antagonist.

25 While the isatin analogues were generally less effective at CE inh

26 e (T(1)) is responsible for cleavage into an isatin and a 1,1-diarylethene by an initial C-C bond sci

27 Synthesis of isatin and iodoisatin from 2'-aminoacetophenone was achi

28 cedure was investigated with a wide range of isatin and phenol derivatives; moreover, the reaction me

29 ith substitution at various positions of the isatin and the 2-siloxyindole being tolerated.

30 eta-unsaturated oxindoles by the reaction of isatins and 2-chloropyridinium salts in EtOH at room tem

31 h catalytic decarbonylative coupling between isatins and alkynes, which provides a unique way to synt

32 ediated tandem reaction of easily accessible isatins and allenoates to functionalized 3-alkenyl-2-oxi

33 ed reaction proceeds via spiro-annulation of isatins and allenoates.

34 ith azomethine ylides generated in situ from isatins and alpha-amino acids has been elaborated, affor

35 of azomethine ylides, generated in situ from isatins and azetidine-2-carboxylic acid, with different

36 cade reaction of 3-alkylidene oxindoles with isatins and o-quinones.

37 tution reaction of 2-chloropyridinium salts, isatins, and amines in ethanol at room temperature.

38 tioselective vinylation of alpha-ketoesters, isatins, and imines to deliver a range of synthetically

39 n scope, scalable, applicable to unprotected isatins, and provides efficient access to 3-hydroxyoxind

40 rent classes of inhibitors: peptidomimetics, isatins, and pyrimidoindolones.

41 Isatins are a class of compounds that target activated c

42 been accomplished from the readily available isatin as a single starting material.

43 has been developed, employing N-substituted isatins as carbonyl substrates, and urea and alkyl aceto

44 c sequence has been demonstrated also for an isatin bearing fluorine substituents on the aromatic rin

45 new compounds having benzothiophene, indole, isatin, benzofuroxan, benzofurazan, benzothiadiazole, an

46 Treatment with the antiviral compound isatin beta-thiosemicarbazone (IBT), a compound that was

47 ults in resistance to the anti-poxvirus drug isatin-beta-thiosemicarbazone (IBT).

48 combinatorial method, variants of the basic isatin-beta-thiosemicarbazone structure were prepared an

49 ncreased resistance to the antipoxviral drug isatin-beta-thiosemicarbazone, suggesting that these mut

50 temperature-sensitive mutant, Cts56, and an isatin-beta-thiosemicarbazone-dependent deletion mutant,

51 nd substitution around the N4-phenyl ring of isatin-beta-thiosemicarbazones (IBTs), to identify compo

52 Several isatin-beta-thiosemicarbazones from our initial study ha

53 Potent and much more selective N-aminomethyl-isatin-beta-thiosemicarbazones were discovered.

54 In contrast, the isatins bind to caspase-3 with significant heat release

55 addition, enzyme activity is abolished upon isatin binding to one active site of the homodimer resul

56 ntrast, the reversible competitive inhibitor isatin binds to all known MAO B and MAO A with similar a

57 nine Ni(II) complex with amides, imides, and isatins catalyzed by base afforded modified Ni(II) compl

58 ddition of terminal ynamides to a variety of isatins, catalyzed by a bisoxazolidine copper complex un

59 The superior performance of isatins compared to other carbonyl based dienophiles was

60 Interestingly, the inhibitory potency of the isatin compounds was related to their hydrophobicity, su

61 harmacologically important thiazolidinedione-isatin conjugates in excellent yields and diastereoselec

62 reaction is compatible with a wide range of isatins containing electron-donating groups (EDGs) and e

63 Functionalization of an isatin-containing Ni(II) complex through a 1,3-cycloaddi

64 The isatin core system is of immense importance due to the h

65 Isatin derivatives also underwent bisarylation with vari

66 ion of N-substituted thiazolidinediones with isatin derivatives has been developed "on water" to affo

67 (Z)-5-arylidene-1,3-thiazolidine-2,4-diones, isatin derivatives, and 1,2,3,4-tetrahydroisoquinoline (

68 pyrazoles, chromones, coumarins, xanthines, isatin derivatives, thiazolidindiones, (thiazol-2-yl)hyd

69 A series of isatin derived difluoronitromethyl substituted tertiary

70 n unprecedented aza-Michael reaction between isatin derived N-Boc ketimines and y-hydroxy enones.

71 uran framework was established starting from isatin-derived aldehydes and 2 equiv of 1,3-dicarbonyl c

72 Herein, we depict an isatin-derived and 3,3'-disubstituted oxindole-appended

73 tric 1,3-dipolar cycloadditions (1,3-DCs) of isatin-derived azomethine ylide with allenes have been e

74 n efficient asymmetric aza-Henry reaction of isatin-derived ketimines has been achieved by using a ch

75 uaternary center (alpha-tertiary amine) from isatin-derived ketimines in the presence of vinyl seleno

76 za-Henry reaction of aryl nitromethanes with isatin-derived ketimines promoted by chiral monoamidine

77 annulation reaction was established between isatin-derived Morita-Baylis-Hillman (Is-MBH) alcohols w

78 Our data suggest that an isatin-derived spirocyclic alpha-methylene-gamma-butyrol

79 em consisting of the core of naphthalene bis-isatin dimer and the terminal moieties of rhodanine, whi

80 is proposed to go through C-C activation of isatins, followed by decarbonylation and alkyne insertio

81 ious N-protected amino acids were coupled to isatin forming N-amino acylisatins.

82 derivatives containing an amide, imide, and isatin fragment through the Michael addition reaction is

83 ar iodine-promoted efficient construction of isatins from 2'-aminophenylacetylenes, 2'-aminostyrenes,

84 s, indazoles, benzotriazoles, indolones, and isatins gave analogues with weaker NR1A/2B activity than

85 steric modulators of potency (i.e., n-benzyl isatins) generated ligands that demonstrated similar or

86 Without alcohol, self-dimerization of isatins gives rise to tryptanthrin and its analogs.

87 e enantioselective allylboration reaction of isatins has also been shown on the basis of a kinetics s

88 ition of alpha,beta-unsaturated aldehydes to isatins has been developed.

89 etalated iridium(III) complexes derived from isatin-hydrazone Schiff bases with nanomolar IC(50) valu

90 Isatin hydrolase converts isatin to isatinate and belong

91 The high resolution crystal structures of isatin hydrolase from Labrenzia aggregata in the apo and

92 The functional proton wire present in isatin hydrolase isoform b represents a unique catalytic

93 The isatin hydrolase orthologues found in human gut bacteria

94 identification of orthologous genes encoding isatin hydrolases within the prokaryotic kingdom.

95 Isatin in a solution of dry N,N-dimethylformamide/NaClO(

96 ifunctional aromatic monomer (biphenyl) with isatin in superacidic media and further derivatization,

97 ng with commercially available 5-substituted isatins in nearly every case.

98 ion provides effective access to a series of isatin-incorporated phosphate-bearing 1,6-adducts having

99 and the cyclic ketones 1H-indole-2,3-dione (isatin), indenoquinoxaline-11-one and acenaphthenequinon

100 Condensation of isatin (indole-2,3-dione) and 2-aminobenzamide led to th

101 assays and kinetic studies demonstrated that isatins (indole-2,3-diones), containing hydrophobic grou

102 ocatalytic method that achieves insertion of isatins into aryl difluoronitromethyl ketones under mild

103 (11) in 10 steps and 11% overall yield from isatin is reported.

104 A novel phosphonium-mediated reaction of isatins is described.

105 MAO B I199F mutant protein of MAO B binds to isatin (K(i) = 3 microM) but not to the three inhibitors

106 ad Ir(III) complex (1), bearing an imidazole-isatin ligand, shows high aqueous stability, maximum cel

107 xindoles was described via readily available isatin, malononitrile, allenoate, and amines.

108 ient five-component condensation reaction of isatin, malononitrile, secondary amines, alcohols, and m

109 nes, which are readily available with use of isatines, malononitrile, and 1,2-phenylenediamines under

110 he thiosemicarbazone and the reliance on the isatin moiety as key bioisosteric contributors.

111 es (3-fluoropropyl and 4-fluorobutyl) at the isatin nitrogen.

112 Assisted by the DG, the C-C cleavage of isatins occurs at room temperature.

113 ncluding benzanilide, acetanilide, oxindole, isatin, quinolinone, and maleimide, affording stable N-

114 ndmeyer reaction, followed by cyclization to isatin, reduction to indole with LiAlH4, and condensatio

115 A focused library incorporating an isatin scaffold was designed and evaluated for inhibitio

116 ion of a methoxy moiety in position 6 of the isatin scaffold.

117 A series of isatin sulfonamide analogs having a Michael acceptor wer

118 A number of isatin sulfonamide analogues were prepared and their pot

119 x between recombinant human caspase 3 and an isatin sulfonamide inhibitor has been solved to 2.8-A re

120 In this study, a series of isatin sulfonamide Michael acceptors having a high nanom

121 r new fluorinated diastereo- and enantiopure isatin sulfonamide-based potent and selective caspase-3

122 ported peptide-based caspase inhibitors, the isatin sulfonamides derive their selectivity for caspase

123 tentially enhance the metabolic stability of isatin sulfonamides.

124 of isatoic-8-secondary amides (IASAs)) from isatin that take advantage of in situ capture of imidic

125 has been shown to generate species (indoxyl, isatin) that couple to yield indigo and indirubin.

126 The isatin-thiazolidine conjugate undergoes a catalyst-free

127 Upon treatment of Isatin, THIQ with (Z)-4-arylidene-5-thioxo-thiazolidin-2

128 ation using the oxidative decarbonylation of isatin to form anthranilic acid as a fluorescent probe.

129 Isatin hydrolase converts isatin to isatinate and belongs to a novel family of met

130 ns were carried out on several 5-substituted isatins to investigate the stability of sulfide adducts

131 addition of aryl acetonitrile to N-protected isatin under mild conditions has been developed.

132 opylenedioxythiophenes (ProDOTs) and N-alkyl isatins under ambient conditions result in isomerically

133 oles were prepared either from corresponding isatins using a three-step synthesis in an average overa

134 alpha-Aryl oxindoles are accessed from isatin via a two-step procedure involving a phospha-Broo

135 The C-2 carbonyl of isatin was envisioned to react in the active site of HRV

136 (HRV-2) 3CP was solved and revealed that the isatin was situated in essentially the same conformation

137 N-tert-butanesulfinyl ketimines derived from isatins was a key step and provided diastereomeric adduc

138 en the structures of MAO-N proline and MAO-B-isatin were overlaid.

139 -(2(S)-(methoxymethyl)pyrrolidinyl)sulf onyl]isatin were synthesized in 140 min with 24% and 10% over

140 n-5-[1-(2-methoxymethylpyrrolidinyl)sulfonyl]isatins were developed as a new group of nonradioactive

141 y in chiral BINOL-catalyzed allylboration of isatins were examined by DFT calculations.

142 A novel series of 2,3-dioxindoles (isatins) were designed that utilized a combination of pr

143 catalytic enantioselective allylboration of isatins with 2-allyl-1,3,2-dioxaborolane in the presence

144 H)-ones via acylation of various substituted isatins with readily available N-Boc-protected aminoacid