ライフサイエンスコーパス: chemical genetics

1 atic chemical approach to exploring biology (chemical genetics).

2 leads and tools to dissect function through chemical genetics.

3 unction through small-molecule evolution and chemical genetics.

4 ncluding zebrafish, a model for genetics and chemical genetics.

5 proaches to modulate neuronal activity using chemical genetics.

6 yet present challenging targets for reverse chemical genetics.

7 activity towards MEK1 by in vitro assays and chemical genetics.

8 nce, we dissect their activation pathways by chemical genetics.

9 lk1-depleted cells, is readily revealed with chemical genetics.

10 all molecules has been a technical hurdle of chemical genetics.

11 small molecules in conjunction with genetics-chemical genetics.

12 ay with genetic screens, targeted LC-MS, and chemical genetics.

13 chanisms of cellular events-a process termed chemical genetics.(1) Unfortunately, the majority of cur

14 Here we demonstrate, using chemical genetics, a mutually agonistic interaction betw

15 Thus, our chemical genetics analysis demonstrates the utility of t

16 Our studies exemplify the combined power of chemical genetics and biochemical analyses for discoveri

17 Utilizing chemical genetics and chemoproteomics, we validate that

18 loped screen takes advantage of the power of chemical genetics and combines it with the known substra

19 n (BET) proteins in DLBCL, using integrative chemical genetics and functional epigenomics.

20 Therefore, by combining chemical genetics and homologous gene replacement in som

21 We further employed chemical genetics and identified NDR1/2 substrates in th

22 Here we use chemical genetics and optogenetic techniques to dissect

23 Our results illustrate the combined use of chemical genetics and proteomics in biological discovery

24 Here, we use chemical genetics and report the generation of an analog

25 ctivity in RPE1 human epithelial cells using chemical genetics and verifying results in additional li

26 erichia coli against 15 different AMPs using chemical-genetics and compare to the cross-resistance sp

27 Using chemical-genetics and mass spectrometry, we identified s

28 nge of novel applications in drug discovery, chemical genetics, and proteomics research.

29 nt modifiers of diverse protein families for chemical genetics applications.

30 Here, we have initiated a chemical genetics approach and isolated compounds that i

31 ns in Phytophthora infestans, we initiated a chemical genetics approach by screening for a stage-spec

32 Our analysis illustrates the power of a chemical genetics approach for the analysis of signal tr

33 Therefore, our cell-based chemical genetics approach for the discovery of apoptosi

34 bulky N(6)-substituted ATP analogs, using a chemical genetics approach initially pioneered with v-Sr

35 A chemical genetics approach revealed pronounced species d

36 Here we describe a chemical genetics approach that overcomes this limitatio

37 We report here a chemical genetics approach to identify host cellular fac

38 We used a chemical genetics approach to identify SIR1, a regulator

39 In summary, we used a chemical genetics approach to reveal STAT3 as a novel ne

40 Here we use a chemical genetics approach using knock-in mice in which

41 To overcome this barrier, a chemical genetics approach was employed in which 43,783

42 Using a chemical genetics approach, the Saccharomyces cerevisiae

43 Using a chemical genetics approach, the small molecule [5-(3,4-d

44 This was achieved by utilizing a chemical genetics approach, where ectopically expressed

45 Using a chemical genetics approach, which combined a pH-homeosta

46 t might be encountered upon adopting a given chemical genetics approach.

47 iosynthesis in Arabidopsis thaliana, using a chemical genetics approach.

48 Using this chemical-genetics approach, we assign particular amino a

49 Combining chemical manipulations and chemical genetics at the photoautotrophic transition che

50 imed at promoting the development and use of chemical genetics by scientists worldwide.

51 We have used a combination of chemical genetics, chromatin proteomics, and imaging to

52 Chemical genetics employs diverse small-molecule compoun

53 Our forward chemical genetics followed by biophysical analyses eluci

54 d compounds, we applied phage-based, reverse chemical genetics for the discovery of caveolin-1 ligand

55 Using chemical genetics, here, we report the identification of

56 To study neurobiology using chemical genetics, high-throughput cell and organismal a

57 Cancer Institute created the Initiative for Chemical Genetics (ICG), to enable public research using

58 Here, we have used chemical genetics in a human cell line to address these

59 al changes that promote cytokinesis, we used chemical genetics in Dictyostelium to identify genetic s

60 Specific inhibition by chemical genetics in MEFs confirmed the involvement of J

61 ng approaches followed by drug optimization, chemical genetics in plant systems tends to be fueled by

62 ovide an overview of the current progress in chemical genetics in plants, with a focus on the discove

63 For instance, chemical genetics involves the discovery of small-molecu

64 Chemical genetics is a biochemical approach to develop s

65 pound affecting plant immunity indicate that chemical genetics is a powerful tool to study whole-orga

66 Chemical genetics is an emerging technology for revealin

67 The National Cancer Institute Initiative in Chemical Genetics is designed to encourage the developme

68 ful screening campaigns in drug discovery or chemical genetics is the availability of structurally an

69 Chemical genetics, or the specific modulation of cellula

70 Here we developed a CRISPR interference chemical-genetics platform to titrate the expression of

71 ation of deep metric learning to large-scale chemical genetics projects highlights the utility of thi

72 Here, we combine chemical genetics, proximity labeling, and proteome-wide

73 in this issue of Cell in which a new type of chemical genetics revealed the function of a new outer m

74 Here, a chemical genetics screen of kinase inhibitors revealed p

75 ll infection, we performed a high-throughput chemical genetics screen of known inhibitors and agonist

76 Therefore, results from a chemical genetics screen suggest that intersections of t

77 Here we use a chemical genetics screen to identify direct substrates o

78 ated immunity, we designed and carried out a chemical genetics screen to search for small molecules t

79 In a chemical genetics screen we identified the small-molecul

80 Using a chemical genetics screen, in this study we report the id

81 ing insulin activity, we performed a forward chemical-genetics screen based on translocation of a glu

82 Here, we have used forward chemical genetics screening to identify DFPM-insensitive

83 In contrast to RID(WT) and RID(D1114G), chemical genetics shows that the interaction of RID(Delt

84 Using a chemical genetics strategy wherein Bur1 kinase was engin

85 conserved cysteines and data from different chemical genetics studies, we suggest that CYSTM protein

86 Using chemical genetics, super resolution microscopy, and live

87 uman Aurora A kinase (as-AurA) engineered by chemical genetics techniques.

88 Using chemical genetics, the systematic screening of chemical

89 ryonic tissues with genetic manipulation and chemical genetics thus provides a powerful approach to u

90 We used chemical genetics to control the activity of budding yea

91 so demonstrate the feasibility of exploiting chemical genetics to define the pathways that govern ver

92 We previously used chemical genetics to dissect auxin-signaling mechanisms

93 e exploited Mycobacterium tuberculosis (Mtb) chemical genetics to identify pathways influencing antib

94 We used chemical genetics to interrogate human DDK with maximum

95 Using chemical genetics to reversibly inhibit Cdk1, we find th

96 In this study, we use chemical genetics to show that the protein kinase Mps1 r

97 have applications in medicinal chemistry and chemical genetics too.

98 We implemented cortistatin A, chemical genetics, transcriptomics, and other methods to

99 Chemical genetics uncovered requirements for the metazoa

100 mimicked the effects of BRD0476, and reverse chemical genetics using a known inhibitor of USP9X block

101 Using chemical genetics, we discovered thirteen candidate MST3

102 Using chemical genetics, we show that kinase inhibitors bypass

103 Using chemical genetics, we show that kinase-active Plk4 is in

104 ic synthesis offers the promise of advancing chemical genetics, where small molecules are used to exp

105 pike-induced syncytium formation, we combine chemical genetics with 4D confocal imaging to establish

106 Combining chemical genetics with comparative genomics of Mtb clini

107 By combining chemical genetics with multimodal imaging, we have ident