Isolation, Structure Determination, and Synthesis of Allo‐RA‐V and Neo‐RA‐V, RA‐Series Bicyclic Peptides from <i>Rubia cordifolia</i> L.

Hitotsuyanagi, Yukio; Odagiri, Masumi; Kato, Saori; Kusano, Junichi; Hasuda, Tomoyo; Fukaya, Haruhiko; Takeya, Koichi

doi:10.1002/chem.201103185

Cited by 39 publications

(28 citation statements)

References 52 publications

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“…Just in last year, Y. Hitotsuyanagi etc . got a series of special cyclopeptides from the Genus Rubia [62,63]. …”

Section: Reviewmentioning

confidence: 99%

“…RYs I-III (100–102), RA-700 (104), and RC-18 (105) possessed only medium activities against P388 [56]–[58,60,61]. The newly identified compounds 106–108, and RA-V, VII were evaluated for their cytotoxic activities against HL-60 and HCT-116 while only the latter had potent cytotoxicities [62]. Moreover, compound 109 exhibited cytotoxic effects on HL-60 cells, but which was much weaker than those of RA-XXIV and RA-VII [63].…”

Section: Reviewmentioning

confidence: 99%

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Structural and bioactive studies of terpenes and cyclopeptides from the Genus Rubia

Wang

Yuan

et al. 2013

Chemistry Central Journal

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Genus Rubia fell into about 70 species distributed widely around the world, a total of 36 species and 2 varieties were reported from China. The extracts and phytochemicals of Rubia plants had drawn considerable attention due to their potent bioactivities. As the two major ingredients from these plants, pentacyclic triterpenes and cyclopeptides were becoming a hot topic over the past twenty years for their remarkable anticancer, antioxidant and other effects. This paper compiled all 65 terpenes and 44 cyclopeptides with their distributions, physiological activities and melting points (or optical rotations) as reported in 85 references; besides, structure-activity relationships of these derivatives were briefly discussed. The information involved in this paper was expected to be meaningful for the further studies of the Genus Rubia.

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“…Just in last year, Y. Hitotsuyanagi etc . got a series of special cyclopeptides from the Genus Rubia [62,63]. …”

Section: Reviewmentioning

confidence: 99%

Section: Reviewmentioning

confidence: 99%

Structural and bioactive studies of terpenes and cyclopeptides from the Genus Rubia

Wang

Yuan

et al. 2013

Chemistry Central Journal

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“…[15,16] O-Seco-deoxybouvardin (16)h as been isolated from this plant as ap ossible biosynthetic precursor of deoxybouvardin (4)a nd allo-RA-V (5). [9,17] RA-dimer B( 3)m ay be biosynthesized by oxidative couplingo f16 with 4 to produce dimeric inter-mediate 17 and the subsequento xidative formation of the diphenyle ther ring of the allo-RA-V unit of 3 (Scheme 3). Alternatively, the biosynthesis of peptide 3 may occur by the direct oxidative coupling of deoxybouvardin (4)w ith allo-RA-V (5).…”

Section: Ra-dimer B( 3)h As Unusuals Tructural Featuresmentioning

confidence: 99%

“…[6,7] Peptide 1 hasa lso been shown to induce conformationalc hanges in F-actin, therebys tabilizing actin filaments and inducing G2 arrest. [8] In the present study,w ee xamined in detail the peptidec omponents in the roots of R. cordifolia and isolated an ew dimericp eptide, RA-dimer B( 3), comprising one molecule of deoxybouvardin (4) [1][2][3] and one molecule of allo-RA-V (5) [9] linked by an ether linkage. In this paper,w ed e-scribe the isolation and structured etermination of RA-dimer B (3).…”

Section: Introductionmentioning

confidence: 99%

RA‐dimer B, a New Dimeric RA‐series Cyclopeptide Incorporating Two Different Types of Cycloisodityrosine Units, from Rubia cordifolia L.

Hitotsuyanagi

Tsuchiya

Ohata

et al. 2016

Chemistry An Asian Journal

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RA-dimer B, a new cytotoxic RA-series peptide, was isolated from the roots of Rubia cordifolia L. Its structure was elucidated on the basis of spectroscopic analysis to be a dimeric cyclopeptide composed of deoxybouvardin and allo-RA-V. Those two cyclopeptide units are connected by an ether linkage between the phenolic oxygen atom of deoxybouvardin and the ϵa carbon atom of Tyr-6 of allo-RA-V. RA-dimer B was synthesized by the coupling reaction of deoxybouvardin with the boronic acid derivative of allo-RA-V, and subsequent deprotection, confirming the relative stereochemistry and establishing the absolute configuration of this peptide. RA-dimer B showed cytotoxic activity against human promyelocytic leukaemia HL-60, human colonic carcinoma HCT-116, and human renal cell carcinoma ACHN cells with IC values of 0.59, 0.54, and 0.74 μm, respectively.

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“…Deoxybouvardin ( 4 ) exhibits IC 50 concentrations between 0.001 and 0.014 µg/mL against various cancer cell lines; however, the glycosylated variant, RA‐XII, exhibits IC 50 values substantially higher between 1.8 and 10 µg/mL . Conversely, rubiyunnanin B possesses a glycosylated tyrosine with measured IC 50 values between 3.6 and 31 µg/mL, whereas the aglycon does not possess antitumor activity (IC 50 > 100 µg/mL) , …”

Section: Introductionmentioning

confidence: 99%

Synthesis of the Rubiyunnanin B Core Aglycon

Moschitto

Lewis

2016

Eur J Org Chem

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Rubiyunnanin B possesses an intriguing anticancer profile whose activity is dependent on the glycosylation of a fused tyrosinyl residue. We have developed a rapid synthesis of the rubiyunnanin B dityrosine core using a Suzuki coupling. Furthermore, the atropisomeric and isomeric products obtained were identified and their distribution controlled. The two major products obtained from the dityrosine coupling were discovered to be locked cis/trans isomers of the internal amide with atropisomerization quantifiable on the NMR timescale.

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Isolation, Structure Determination, and Synthesis of Allo‐RA‐V and Neo‐RA‐V, RA‐Series Bicyclic Peptides from Rubia cordifolia L.

Cited by 39 publications

References 52 publications

Structural and bioactive studies of terpenes and cyclopeptides from the Genus Rubia

Structural and bioactive studies of terpenes and cyclopeptides from the Genus Rubia

RA‐dimer B, a New Dimeric RA‐series Cyclopeptide Incorporating Two Different Types of Cycloisodityrosine Units, from Rubia cordifolia L.

Synthesis of the Rubiyunnanin B Core Aglycon

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