Biogenetically related caged ent-kaurane diterpenoids from Isodon eriocalyx var. laxiflora

Two novel caged ent-kauranoids, neolaxiflorins D (1) and E (2), along with three other new ent-kauranoids, neolaxiflorins F–H (3–5), and a known one, eriocalyxin B (6), were obtained from Isodon eriocalyx var. laxiflora. Neolaxiflorin D (1) is the first 15,16-seco-16,17-dinor-ent-kaurane diterpenoid, and neolaxiflorin E (2) is the first 15,16-seco-17-homo-ent-kauranoid. The absolute configurations of ent-kauranoids 1 and 2 were determined by single-crystal X-ray diffraction analyses. Structural analysis of intermediate compounds 3–5 indicated that eriocalyxin B (6) is a biogenetic precursor of caged ent-kauranoids 1 and 2 as illustrated. The cytotoxic activity of the new compounds was evaluated by an MTT assay.     

6,7-Seco-ent-kaurane-type diterpenoids from Isodon eriocalyx var. laxiflora

Twenty nine 6,7-seco-ent-kaurane-type diterpenoids including 18 new ones, laxiflorolides C–T (1–18), along with 21 known ones were obtained from Isodon eriocalyx var. laxiflora. Laxiflorolides E–G (3–5) are the first identified naturally occurring 6,7-seco-ent-kauranoids that feature a 3,6-epoxy unit, and laxiflorolide M (11) is the first identified naturally occurring 6-nor-6,7-seco-ent-kauranoid. The absolute configurations of compounds 1, 3, 6, and 11 were determined by single-crystal X-ray diffraction analyses. The cytotoxic activity of the isolates was evaluated by an MTT assay.     

A new rearranged and a new seco-ent-kaurane diterpenoids from Isodon parvifolius

Parvifoline X (1), a new rearranged ent-kaurane diterpenoid, and parvifoline Y (2), a new 8,15-seco-ent-kaurane diterpenoid, were isolated from the leaves of Isodon parvifolius. Their structures were elucidated by spectroscopic methods including 2D NMR analysis, and supported by a biogenetic pathway. Parvifoline X (1), possessing a new 15(8→11)-abeo-7α,20-epoxy-ent-kaurane skeleton, was found from the genus Isodon for the first time. Compounds 1 and 2 were evaluated for their inhibitory activity against A549, HT-29, and K562 cell lines. Parvifoline Y (2) was the most cytotoxic against A549 cells with an IC₅₀ value of 4.97 μM.     

Pd-catalyzed asymmetric synthesis of allylic tert-butyl sulfones and sulfides: Kinetic resolution of the allylic substrate by a chiral Pd-complex

The acyclic and cyclic allylic tert-butyl sulfones 3, ent-3, 11a, 11b and 15a–c of 89–98% ee were synthesized in 40–92% yield by a Pd-catalyzed reaction of the respective allylic acetates and carbonates rac-1a, rac-1b, rac-10a, rac-10b and rac-14a–c with LiO₂St-Bu in the presence of the chiral ligands 2a, ent-2b and 12. Formation of the n-butyl sulfones 13a and 13b of 95% ee was observed. Reactions of rac-1a and 1b/ent-1b with LiO₂St-Bu in the presence of 2a and ent-2b, respectively, in THF under heterogeneous conditions were accompanied by a kinetic resolution of the allylic substrates. The faster reacting allylic substrate and the preferentially formed sulfone had the same absolute configuration. The allylic tert-butyl sulfide 17 of 92% ee was obtained in 63% yield by the Pd-catalyzed reaction of rac-1b with Me₃SiSt-Bu in the presence of ent-2b.     

Antiplasmodial Securinega alkaloids from Phyllanthus fraternus: Discovery of natural (+)-allonorsecurinine

The chemical investigation of the antimalarial plant Phyllanthus fraternus G. L. Webster (Phyllanthaceae) resulted in the discovery of the Securinega alkaloid (+)-allonorsecurinine (1), previously reported as a synthetic compound, together with the known ent-norsecurinine (2), nirurine (3), bubbialine (4), epibubbialine (5) and the lignan phyllanthin (6). The structure and absolute configuration of the new compound were elucidated on the basis of extensive spectroscopic analysis, optical rotation, and GIAO NMR shift calculation followed by CP3 analysis. The antiplasmodial activity of these compounds was evaluated against chloroquine-resistant (W2) and -sensitive (3D7) strains of Plasmodium falciparum. Among them, ent-norsecurinine (2) and (+)-allonorsecurinine (1) showed the strongest activity (IC₅₀: 1.14 ± 0.32 and 2.57 ± 0.53 µM) respectively, against W2 but one of the weakest against 3D7.     

Secu’amamines E-G, new alkaloids from Securinega suffruticosa var. amamiensis

One new ent-neosecurinane-type alkaloid, secu’amamine E (1), and two novel alkaloids consisting of a ent-neosecurinane and a piperidine unit, secu’amamine F (2), and secu’amamine G (3), were isolated from Securinegasuffruticosa var. amamiensis. Their structures and stereochemistry were elucidated on the basis of spectroscopic analyses.     

Total syntheses of chaetocin and ent-chaetocin

The first total synthesis of chaetocin (1), a potent histone methyltransferase inhibitor, is described in detail. Key reactions were radical bromination for α-oxidation of the diketopiperazine ring, and reductive radical coupling for construction of the dimeric core structure. Stereoselective construction of the disulfide bridges was achieved via substitution reaction with H₂S. The total synthesis of 1 was accomplished in nine steps starting from known d-amino acid derivatives. Total synthesis of non-natural ent-chaetocin (ent-1) was also achieved via the established synthetic route, starting from l-amino acid derivatives.     

Sesquiterpene constituents of two liverworts of genus diplophyllum: Novel eudesmanolides and cytotoxicity studies for enantiomeric methylene lactones

The steam distillates (or hexane extracts) of the liverworts Diplophyllum albicans (L.) Dum. and D. taxifolium (Wahl.) Dum. are largely a mixture of sesquiterpenes. Both species elaborate, among the hydrocarbons, mainly ent-α-selinene (8a) and ent-selina-4,11-diene (8b) together with anastreptene (1) and β-elemene (9). The major component of each essential oil was diplophyllin (10), a novel ent-eudesmanolide. The structure of diplophyllin was established by correlation with tetrahydro-isoalantolactone (17). In addition, the enantiomers of diplophyllin and diplophyllolide-A (16) were obtained on acid isomerization of isoalantolacetone (14a). Diplophyllin shows significantly greater activity against human epidermoid carcinoma (KB cell culture, ED₅₀? 8 μ $\text{g}\text{ml}$) than its enantiomer: the first demonstration (to our knowledge) of optical selectivity for this type of cytotoxicity. Among the more polar constituents of D. albicans were 9α-acetoxy-diplophyllin, and several sesquiterpene alcohols including albicanol (22).     

ent-Kaurene diterpenoids from Isodon phyllostachys

Four new ent-kaurene diterpenoids, phyllostachysins M–P (1–4) have been isolated from the aerial parts of Isodon phyllostachys. Compound 1 features a novel dihydro-2H-pyran ring motif, which was formed by an unusual cleavage in ring-A. 2 and 3 bear a rare 20-nor-ent-kaurene structure, but 4 has a rare 7,20-cyclo-ent-kaurene skeleton. Their structures were elucidated on the basis of extensive spectroscopic analyses. Compounds 1, 3, and 4 were evaluated for their cytotoxic activity against five human tumor cell lines.     

Bridged-ring products from the acyloin-like cyclization of diterpenoid keto-esters

Bridged-ring structures are readily formed from acyloin-like cyclization of suitably constituted keto esters. thus reaction of the keto ester ent-seco-kauranoid derivatives 1 and 2 with Na-liquid NH₃ affords mixtures of ent-kaurane, ent-beyerane and dimeric products.     

Ten new calyxins from Alpinia katsumadai: a systematically studies on the stereochemistry of calyxins

Ten new calyxin natural products, named calyxin N (1), ent-calyxin N (2), calyxin O (3), ent-calyxin O (4), calyxin P (5), 9″-epicalyxin P (6), calyxin Q (7), calyxin R (8), calyxin S (9) and 5-epicalyxin S (10), were isolated from the seeds of Alpinia katsumadai. Their planar structures were elucidated by a combination of various spectroscopic methods, primarily NMR and MS, while the absolute configurations of the isolated calyxins were comprehensively studied by the modified Mosher's method, electronic circular dichroism (ECD) and theoretical calculations. This is the first systematically study on the absolute configurations of calyxins. Most of the isolated compounds showed moderate to strong antiproliferative activities against NCI-H460, HeLa, SMMC-7721 and HCT-116 cancer cell lines.     

Exhaustive degradation of the ring D of 3,20-epoxy ent-kaurane-type diterpene maoecrystal A

This study described a new approach for exhaustive degradation of the ring D of maoecrystal A (1), an ent-kaurane-type diterpene from Isodon eriocalyx, in seven steps mainly involving retro-aldol reaction, epoxylation, NaIO₄ oxidation, and Baeyer-Villiger process in a 19% overall yield.     

The acid catalysed rearrangement of a diterpenoid epoxide

A study has been made of the principal rearrangement products resulting from formic acid treatment of 19-hydroxy-ent-beyerene epoxide (3). In concentrated solutions 3 has been found to undergo a deep seated rearrangement to the allylic alcohol (14). A mechanism for the formation of 14 is proposed involving a novel 1,4-hydride shift in the bicyclo[3:2:1]octane C/D ring system following cleavage of the C₁₅O bond. Supporting evidence has been obtained from a study of the specifically labelled epoxide (4), the deuterium in 14 appearing exclusively at C₁₂. Four products (7 and 11–13) emanating from the known beyerane → kaurane interconversion have been identified.     

Efficient synthesis of novel cytotoxic cis-fused α-methylene γ-lactones from 7,14-dihydroxy-ent-kaurenes by transformation under Mitsunobu reaction conditions

Facile transformation of 7,14-dihydroxy-ent-kaurenes such as excisanin A (8), kamebanin (9), and kamebakaurin (10), which are abundant in plants of the genus Rabdosia species (Labiatae), to ent-abietanes was accomplished under the Mitsunobu reaction conditions. The δ, ε-unsaturated cis-fused α-methylene γ-lactones (17, 18, and 25) thus prepared showed a moderate cytotoxic activity on P388 murine leukemia cells.     

Bisleuconins A-D: a pair of epimeric ent-kauranoid dimers and two new asymmetric analogues isolated from Isodonleucophyllus

A phytochemical investigation of Isodon leucophyllus led to the isolation of four novel ent-kauranoid dimers: bisleuconins A-D (1-4), and one known compound, rabdoloxin A (5). It was interesting that the structures of bisleuconins A (1) and B (2) were elucidated as a pair of epimeric ent-kauranoid dimers with unique linkage pattern C-16→C-17′ to connect two monomers. Bisleuconins C (3) and D (4) were two new asymmetric ent-kauranoid dimers. A possible biogenetic pathway of 1 and 2 was also proposed.     

Synthesis of the alkaloid tyroscherin by an aldol/Curtius strategy

The alkaloid tyroscherin (2), which contains a vicinal anti-amino alcohol subunit was prepared from 4-hydroxyphenylpropionic acid (5) and meso-diol 9. After desymmetrization of diol 9 and suitable protecting group manipulations, one terminus was extended via a Claisen rearrangement giving rise to enoate ent-15. The missing carbon on the other end could be incorporated using MeMgCl/CuBr·SMe₂ leading eventually to aldehyde ent-22. The acylated oxazolidinone 32 derived from acid 5 and aldehyde ent-22 were combined in an aldol reaction. A subsequent Curtius rearrangement on the carboxylic group furnished the amino function of tyroscherin (2). In a proof of concept study the same strategy was used to prepare tyroscherin analog 28.     

A synthetic strategy using Witkop's pyrroloindole for (−)-debromoflustramine B, (+)-ent-debromoflustramine B and (+)-ent-debromoflustramide B

While prenylation of (−)-Witkop's pyrroloindole (2), secured from l-tryptophan under standard N-alkylation conditions, led to a ca. 1:1 diastereoisomeric mixture of two C^3a-alkylated indolenines 3 and 4, use of phase-transfer conditions altered this to ca. 1:2. Reduction followed by N-prenylation of the resulting secondary amines gave C,N-dialkylated products. The derived separable diastereoisomeric (−)- and (+)-Barton esters 19a and 19b were then converted into (−)-debromoflustramine B and (+)-ent-debromoflustramine B, respectively. A novel reaction involving oxygen and the carbanion derived from Barton ester 19b led to (+)-ent-debromoflustramide B. Treatment of N⁸-prenylated Witkop's pyrroloindole 5 with Lewis acid (BF₃·Et₂O) uncovered a new clean intramolecular cyclisation involving the prenyl unit.     

An asymmetric ent-kauranoid dimer from Isodon rubescens var. lushanensis

A novel asymmetric ent-kauranoid dimer, lushanrubescensin J (1), was isolated from Isodon rubescens var. lushanensis. Its structure was elucidated by the spectroscopic evidences. The stereochemistry was confirmed by the single crystal X-ray diffraction of its tetraacetate. Compound (1) exhibited potent inhibitory activity against K562 cells with IC₅₀ = 0.93 μg/mL.     

New cyclometalated palladium(II) complexes with iminophosphines: Crystal structures of [Pd(C^N)(o-Ph2PC6H4–CH=NR)][PF6] (C^N=azobenzene,R=Et; C^N=2-phenylpyridine,R=Me)

The synthesis of new cyclometalated compounds of palladium(II) with the mixed-donor bidentate ligands o-Ph₂PC₆H₄–CH=NR is described. Two series of complexes [Pd(C^N)(o-Ph₂PC₆H₄–CH=NR)][PF₆] have been prepared using either azobenzene or 2-phenylpyridine as cyclometalated ligands [C^N=azobenzene (azb); R=Me (1a), Et (2a), ⁿPr (3a), ⁱPr (4a), ^tBu (5a), Ph (6a), NH–Me (7a); C^N=2-phenylpyridine (phpy); R=Me (1b), Et (2b), ⁿPr (3b), ⁱPr (4b), ^tBu (5b), Ph (6b), NH–Me (7b)]. The new complexes were characterized by partial elemental analyses and spectroscopic methods (IR, FAB, ¹H and ³¹P NMR). The molecular structures of compounds 2a (monoclinic, P 2₁/n) and 1b (monoclinic, C 2/c) have been determined by a single-crystal diffraction study. In both cases this technique revealed the relative trans configuration between the phosphorus atom and the nitrogen atom of the ortho-metalated ligand.     

Structurally diverse diterpenoids from Isodon ternifolius collected from three regions

Phytochemical investigation of the aerial parts of Isodon ternifolius from three regions in Yunnan Province afforded 9 new diterpenoids, ternifoliusins A–I (1–9), together with 26 known diterpenoids. Among them, ternifoliusins A–D possess rare 6,7:8,15-diseco-7,20-olide-6,8-cyclo-ent-kaurane diterpenoid scaffold. The structures of all compounds were determined by comprehensive spectroscopic analysis, as well as quantum chemical calculation methods. Moreover, the molecular constitutions and configurations of ternifoliusins A, E, and F (1, 5, 6) were confirmed by single-crystal X-ray diffraction analysis. Ten compounds were assayed for their cytotoxic activity against the HL-60, SMMC-7721, A-549, MCF-7, and SW-480 human tumor cell lines, and compounds 13, 17, 19, 20, 31 and 34 were demonstrated to be active against all of the five human tumor cell lines.