Stereocontrolled synthesis of enantiopure cis- and trans-3,4,4a,5,8,8a-hexahydro-1H-quinolin-2-ones

## Abstract A short and efficient protocol for the asymmetric synthesis of __cis__‐ and __trans__‐3,4‐dihydro‐2,4,8‐trihydroxynaphthalen‐1(2__H__)‐one (**1** and **2**, resp.) is described, with a phthalide annulation as the key step. Introduction of a OH substituent at position 2 was performed by

## Abstract The stereochemistry of __trans__‐ and __cis__‐2, 4‐dimethyl‐tetrahydroquinolines, **6** and **7** were derived from ^1^H‐NMR. studies. These were converted respectively into __trans__‐ and __cis__‐5, 6‐dihydro‐4, 6‐dimethyl‐4__H__, 8__H__‐pyrido [3, 2, 1‐de]phenanthridin‐8‐ones **18** a

## Abstract magnified image A short and efficient protocol for the stereoselective synthesis of racemic __trans‐__ and __cis‐__3,4‐dihydro‐3,4,8‐trihydroxynaphthalen‐1(2__H__)‐one (**1** and **2**, resp.), is described, comprising nine and eight steps starting from commercial juglone (=5‐hydroxyna

The electron-impact (EI) and collision-induced dissociation (CID) spectra of the title compounds were studied. The main fragmentation routes of M" ions included losses of hydrocarbon species and the formation of ArCNH' cations. The geometry of ring annelation predictably affected the stabilities of