ライフサイエンスコーパス: sodium borohydride

1 DNA complex can be trapped by reduction with sodium borohydride.

2 than the wild-type enzyme in the presence of sodium borohydride.

3 eans of either acetylation or reduction with sodium borohydride.

4 an subsequently be trapped by reduction with sodium borohydride.

5 ] or 2-(3-oxoindolin-2-yl)acetonitriles with sodium borohydride.

6 duction of methylene blue in the presence of sodium borohydride.

7 equential treatment with iodosylbenzene then sodium borohydride.

8 e fractionation and chemical reduction using sodium borohydride.

9 tionality in the same pot by the addition of sodium borohydride.

10 zardous reducing agents such as hydrazine or sodium borohydride.

11 or into 2-amino-1,3-diols by reduction with sodium borohydride.

12 duction of p-nitrophenol to p-aminophenol by sodium borohydride.

13 entical sample after complete reduction with sodium borohydride.

14 lowed by reduction of the adsorbed salt with sodium borohydride.

15 the corresponding alcohols by reduction with sodium borohydride.

16 onverted to active MCRred1 by treatment with sodium borohydride.

17 water sample with a gold nanorod solution in sodium borohydride.

18 her reduced and stabilized by treatment with sodium borohydride.

19 ) and reduced to the corresponding amines by sodium borohydride.

20 d by oxidation and subsequent reduction with sodium borohydride.

21 reduction of an alpha-nitro ester by TiCl(3)/sodium borohydride.

22 henylalkyl halide followed by reduction with sodium borohydride.

23 imilar form can be trapped by reduction with sodium borohydride.

24 ent protein-DNA complexes in the presence of sodium borohydride.

25 eactions were carried out in the presence of sodium borohydride.

26 nts: 1-butyl-3-methylimidazolium bromide and sodium borohydride.

27 base intermediates trapped by reduction with sodium borohydride.

28 Reduction of mitomycin C (40 microm) by sodium borohydride (200 microm) in 20 mm Tris-HCl, 1 mm

29 t enzyme-DNA intermediate in the presence of sodium borohydride, a new finding that supports the grou

30 rocedure, incorporating derivatization using sodium borohydride, allowed the development of a sensiti

31 ing known lactones by one-pot reduction with sodium borohydride and boron trifluoride etherate.

32 e chemical reduction using sodium amalgam or sodium borohydride and enzymatic generation from porphob

33 he 6-bromo substituent was accomplished with sodium borohydride and palladium chloride.

34 (3) SgcC4 is strongly inhibited by sodium borohydride and potassium cyanide, but preincubat

35 ment of the ring-D dienone successively with sodium borohydride and singlet oxygen.

36 -elimination under alkaline conditions using sodium borohydride and sodium hydroxide.

37 n to give materials that upon reduction with sodium borohydride and subsequent hydrolysis decarboxyla

38 in carbonyls were derivatized with tritiated sodium borohydride and the tritiated proteins were separ

39 ososes were stereospecifically reduced using sodium borohydride and then deprotected to give allo- an

40 ducts of their reaction with sodium cyanide, sodium borohydride, and methoxylamine and by the mass sp

41 2'-deoxyuridine, followed by reduction with sodium borohydride as a limiting reagent, produces dTHU

42 zatriphenylenehexacarbonitrile [HAT(CN)(6) ] sodium borohydride as the starting materials.

43 The reducibility of DOM by sodium borohydride (as judged by relative removal of ini

44 Sodium borohydride-based hydride generation was automate

45 when activated with a hydride source such as sodium borohydride, cleanly and selectively dehalogenate

46 ng rates of sugar-aldehyde reduction and the sodium borohydride concentration dependence of the rate

47 ethyl-3-ketoacyl triketide intermediate with sodium borohydride confirmed that in each case the trike

48 ell extract and BER intermediate as bait for sodium borohydride crosslinking.

49 umin (HSA) in vitro; (ii) to determine, by a sodium borohydride-dependent mass peptide mapping method

50 hate did not stimulate and hydroxylamine and sodium borohydride did not inhibit the enzyme activity,

51 in-2(3H)-ones 21a-d, which were converted by sodium borohydride directly into optically active 3-subs

52 ch mutacin 1140 was chemically modified with sodium borohydride followed by ethanethiol, allowing the

53 curial products with O(2) in the presence of sodium borohydride furnished 72, which was readily separ

54 with Grignard reagents, sodium cyanide, and sodium borohydride gave 1,2,3,4-tetrahydropyrrolo[1,2-a]

55 Addition of sodium borohydride generates a hydroquinone derivative t

56 ction of dissolved organic matter (DOM) with sodium borohydride has been used to understand the geogr

57 eridin-1-yl)oxyl (TEMPO), ascorbic acid, and sodium borohydride) have been investigated to eliminate

58 on was determined by chemical reactions with sodium borohydride, hydrogen peroxide, alpha-methoxy-alp

59 ifying band 3 with Woodward's reagent K plus sodium borohydride (i.e., the modification process) expo

60 ketones that are capable of being reduced by sodium borohydride in an aqueous medium.

61 elds an enol ester that cannot be reduced by sodium borohydride in an aqueous solution, while other n

62 bsequently to the dianion was achieved using sodium borohydride in ethanol.

63 typhimurium enzyme by phosphonoacetaldehyde-sodium borohydride-induced inactivation and by site-dire

64 idazol-2-ones 17a-c, which were converted by sodium borohydride into (3S,7aR)-3-substituted-1-(4-nitr

65 ive site, and treatment of such adducts with sodium borohydride irreversibly inactivated the enzyme.

66 rly, reduction of the HemA-PLP complex using sodium borohydride led to > 90% inactivation of the enzy

67 This sodium borohydride-mediated reduction process resulted i

68 oxide, followed by sequential treatment with sodium borohydride, methanesulfonyl chloride, and morpho

69 dified by WR-K and then reduced by tritiated sodium borohydride (NaB[3H]4) showed the presence of a p

70 ohols are obtained in very good yields using sodium borohydride (NaBH(4)) as a reducing agent and a c

71 remove major tRNA modifications, followed by sodium borohydride (NaBH(4)) reduction of m(7)G sites an

72 of HInCl(2) from the reduction of InCl(3) by sodium borohydride (NaBH(4)) was also re-evaluated for c

73 s of 4-nitrophenol (4-NP) in the presence of sodium borohydride (NaBH(4)).

74 using the chemical precipitation method with sodium borohydride (NaBH4) as the reductant in the prese

75 Janus microparticle motors in a solution of sodium borohydride (NaBH4) fuel.

76 tion of AgNPs onto silica using a chitosan + sodium borohydride (NaBH4) method results in higher silv

77 Specifically, we use a sodium borohydride (NaBH4) treatment process to thorough

78 hod with varying amounts of reductant, i.e., sodium borohydride (NaBH4).

79 zole, an alkylating agent (usually MeI), and sodium borohydride (NaBH4).

80 330, which is obtained by reducing F430 with sodium borohydride (NaBH4).

81 tions are performed using dissolving metals, sodium borohydride or hydrogen transfer conditions under

82 of a lipid fraction derived from oxLDL with sodium borohydride or potassium iodide completely abroga

83 tones/aldehydes to alcohols employing excess sodium borohydride produced pronounced and largely, but

84 ent on-line hydride generation with acid and sodium borohydride produces AsH3 and H2, which are separ

85 e removal of the chiral auxiliary in 5 using sodium borohydride, protection of the gamma-cyano alcoho

86 the DAB-enhanced stain was used; it utilizes sodium borohydride, proteinase K, Triton X-100 and xylen

87 ompounds were initially converted to stable, sodium borohydride-reduced 3-aminopyridine conjugates, w

88 eveal regions of the sample matrix where the sodium borohydride-reduced silver colloidal particles ar

89 (GUS) with sodium metaperiodate followed by sodium borohydride reduction (PerT-GUS) eliminated uptak

90 followed by treatment with sodium azide and sodium borohydride reduction gave 5-azido-5-hydroxylmeth

91 Hence, the sodium borohydride reduction of hemiacetals 2a,b can be

92 l oligosaccharides were released by alkaline sodium borohydride reduction of the jelly coating from t

93 Additionally, by predicting the effects of sodium borohydride reduction on the model compounds and

94 Sodium borohydride reduction operates from the beta-face

95 small RNA selection, AlkB demethylation, and sodium borohydride reduction steps to achieve specific a

96 e GalNAc residues by periodate oxidation and sodium borohydride reduction, indicating a requirement f

97 droxymethylcytosine and, in combination with sodium borohydride reduction, single 5-formylcytosine nu

98 glycan release to promote lactonization, and sodium borohydride reduction, that were both optimized t

99 ntly linked to the 8-oxoG oligonucleotide by sodium borohydride reduction.

100 ken at breaking point, both with and without sodium borohydride reduction.

101 bose-5-phosphate-containing DNA substrate by sodium borohydride reduction.

102 ction of MSOX or MTOX with a small excess of sodium borohydride results in immediate flavin reduction

103 In this study, treatment of CBS with sodium borohydride selectively reduced the Schiff base b

104 sis using COS cells lysed in the presence of sodium borohydride showed that: 1) phosphate recovered o

105 to its original state after treatment with a sodium borohydride solution, demonstrating the reversibl

106 Treatment of galactated HSA with sodium borohydride stabilized the condensed sugars on th

107 uggested a cyclic moiety, and reduction with sodium borohydride suggested two reducible oxygen-contai

108 tivated upon exposure to pyridoxal phosphate/sodium borohydride, suggesting a reactive lysine residue

109 1-arylcyclohexadienyliron(1+) complexes with sodium borohydride to access the endo series also gave a

110 can be reduced by either triethyl silane or sodium borohydride to form the corresponding beta- and g

111 atives and could be selectively reduced with sodium borohydride to give unstable benziphlorins.

112 y chemical reduction of the silver ions with sodium borohydride to produce silver particles.

113 he benzene rings, followed by treatment with sodium borohydride to reduce the nitro-groups to primary

114 Schiff base intermediate that can react with sodium borohydride to trap the DNA-enzyme complex.

115 Sodium borohydride trapping of wild-type Fpg and its E3Q

116 x sample matrices was accounted for by using sodium borohydride-treated blanks.

117 t disrupted by increased temperature because sodium borohydride treatment of the enzyme at either 15

118 Sodium borohydride treatment reduces M(1)GdR to the 5,6-

119 1 complex and reactivity to decreased pH and sodium borohydride treatment were suggestive of a struct

120 onment, bioreductants, exogenous thiols, and sodium borohydride were studied.

121 a mixture of 6 M guanidine hydrochloride and sodium borohydride, which stopped the reaction and reduc

122 l was carried out using aqueous solutions of sodium borohydride, which yielded a refractive index sen

123 alyze these imine bonds after reduction with sodium borohydride while under tension and found that th

124 Reduction of thiocolchiocone with sodium borohydride yielded the racemic alcohol 9, the st