Concise, Asymmetric, Stereocontrolled Total Synthesis of Stephacidins A, B and otoamide B (+)-avrainvillamine (+)-notoamide B 20 51 21 55 (-)-stephacidin B In 2002, Bristol-Myers Squibb reported the biologically active metabolites isolated from a fermentation broth of Aspergillius ochraceus. The stephacidins A and B were identified as potent inhibitors of several human tumor cell lines with the complex alkaloid (-)-stephacidin B exhibiting a high cytotoxic potency against testosterone-dependent prostate LCaP lymphoma. (+)-Avrainvillamide were in evidence, suggesting a simple dimerization-based biogenesis of (-)-stephacidin B if the bonds between C20-C51 and C21-55 of 2 are broken. The Baran group reported the first total synthesis of stephacidin A using a novel oxidative enolate coupling to form the [2.2.2] bridged bicyclic ring system followed by an unusual cascade reaction for the formation of the natural product in 29 total steps from commercially available starting materials in 2005.
Fragment I & II: CCl 3 1 1) CCl 3 2 2) a 3) Cl, 3 1. Preparation of product 3 is a gram-scale process, please finish this process: What is the precursor/transformation might you use for the preparation of starting material 1; and what kind of reagent/condition could be employed for the transformation of 1 to give 2? Bn 4 4) 5) 5 BC C 2 DBU, CuCl 2 C 0 o C -> rt 6 2. Please suggest the reagents for step 4 and 5. 3. Propose the structure of product 6. 6 C, W 180 o C 7 2 2 C Ac rt 8 n Bu 3 P, C W, 140 o C 9 + 10 C 2 Et + 2 C 2 Et 1 Cl C 2 Cl 2 (one pot ) C 6) 7) 11 12 4. Please suggest the reaction mechanism for formation of product 7 and what is the name of this reaction called? 5. With 7 in hand, it is treated with 2 and formaldehyde under acidic condition to furnish 8. What is this conversion named? And what is the structure of 8? 6. To form the intermediate 10, compound 8 was treated with 9 accelerated by microwave. What is 9? And propose the reaction mechanism for the formation of intermediate 10. [int: elimination followed by nucleophilic addition] 7. Intermediate 10 was subsequently treated with 1 Cl to give 11, please finish the final steps from 11 to 12.
Concise, Asymmetric, Stereocontrolled Total Synthesis of Stephacidins A, B and otoamide B (continued) Combination of fragment I and II (3 & 12) C + Cl C 2 1) ATU, DIEA C, rt 13 2) W, C 150 o C 14 (syn:anti = 1:1) 12 3 8. By combination fragment 12 and 3, ATU and DIEA was employed to form compound 13. What does ATU stand for and please draw the mechanism and product for this transformation. 9. Compound 13 was then subjected to microwave reaction condition at 150 o in C to give compound 14. What is the structure of 14? ( int: W assists cyclization reaction). 14 3) 3 + BF 4 - Cs 2 C 3, C 2 Cl 2 4) 2, DMAP TEA, TF 15 10. Protecting of 14 with lactim ether and protection group in 15, compound 14 was treated with 3 + BF 4 -, please suggest reasonable mechanism for this reaction. 11. Please suggest reagents, catalysts or conditions to furnish aldehyde 16. 16 5) C 6) ab 4, 7) MsCl, TEA, C 2 Cl 2 17 12. By treating aldehyde 16 with ab 4 followed by treating with MsCl, 17 was formed. What is the structure of compound 17? 16 C
8) a, W, 120 o C 17 or a,, sealed tube 130 o C 18 9) Pd(TFA) 2 5eq C then ab 4 10) 0.1 Cl wash 11) W, C, 180 o C 13. [2,2,2]-Bicyclic system on 18 was established by treating 17 with a under microwave condition. What is the reaction mechanism? 14. To finish one of the natural product, compound 18 was treated with 5 eq of Pd(TFA) 2 in C to give a palladium intermediate. What s the structure of the pd-intermediate you will expect to? Please specify the regioselectivity. After reduced the pd-intermediate by ab 4, followed by acidic wash (0.1 Cl) and then heating at 180 o C, was formed as an amorphous white powder. 12 ) acb 3, Ac, rt 19 13) cat. Se 2 (0.25 eq) 35 % 2 2 (35 eq) dioxane, rt 72 h Bu S 20 2 C 2 Cl 2, rt (-)-avrainvillamine Et 3 C rt 1 h (+)-notoamide B (+)-stephacidin B
15. (+)-otoamide B was synthesised by treating with oxaziridine 20 in C 2 Cl 2 at rt. Please draw the reaction mechanism for this reaction. 16. n the other hand, reduction of with acb 3 under Ac condition gave compound 19 followed by oxidation under cat. Se 2 / 2 2 system to afford a precursor (-)-avrainvillamide. What is the intermediate 19 and please suggest the mechanism of cat. Se 2 / 2 2 oxidation. 17. Please suggest a reasonable electron flow for the final dimerisation process to affoed (+)-stephacidin B.