Syn vs. Anti? What Controls Addition Stereochemistry in Chlorolactonization

Emily R Dzurka Camelio; Mitchell Maday; Aritra Sarkar; James E Jackson; Babak Borhan

doi:10.1002/chem.202403108

Syn vs. Anti? What Controls Addition Stereochemistry in Chlorolactonization

Chemistry. 2024 Oct 21:e202403108. doi: 10.1002/chem.202403108. Online ahead of print.

Authors

Emily R Dzurka Camelio¹, Mitchell Maday¹, Aritra Sarkar¹, James E Jackson¹, Babak Borhan²

Affiliations

¹ Michigan State University, Chemistry, UNITED STATES OF AMERICA.
² Michigan State University, Department of Chemisty, Department of Chemistry, 48824, East Lansing, UNITED STATES OF AMERICA.

PMID: 39429093
DOI: 10.1002/chem.202403108

Abstract

The stereochemistry of the uncatalyzed chlorolactonization of 4-phenylpent-4-enoic acid at room temperature was examined to probe the reaction's intrinsic diastereoselectivities as a function of chlorenium ion donor, solvent polarity, and reactant concentration ranges. Kinetic studies using Variable Time Normalization Analysis (VTNA) revealed differing reaction orders for the syn and anti alkene addition processes. Aided and illustrated by quantum chemical modeling, this detailed mechanistic analysis of the substrate's intrinsic chlorolactonization reactions points to concerted AdE3-type paths for both syn and anti additions. By illuminating the factors selecting for syn- vs anti-addition paths, the results provide key reference points for future studies of stereocontrol in halofunctionalization reactions.

Keywords: VTNA; chlorolactonization; deuterium labeling; halogenation; stereochemistry.