An attempt to prepare sulfonyl analogues of fotemustine: unexpected rearrangement to sulfamate during nitrosation step

Zineb Aouf; Sara Boughaba; Rayene Sayad; Jacques Lebreton; Monique Mathe-Allainmat; Nour-Eddine Aouf

doi:10.1039/d3ra07001h

An attempt to prepare sulfonyl analogues of fotemustine: unexpected rearrangement to sulfamate during nitrosation step

RSC Adv. 2023 Dec 11;13(50):35741-35754. doi: 10.1039/d3ra07001h. eCollection 2023 Nov 30.

Authors

Zineb Aouf¹, Sara Boughaba^{1

2}, Rayene Sayad¹, Jacques Lebreton³, Monique Mathe-Allainmat³, Nour-Eddine Aouf¹

Affiliations

¹ Laboratory of Applied Organic Chemistry, Bioorganic Chemistry Group, Sciences Faculty, Chemistry Department, Badji Mokhtar-Annaba University Box 12 Annaba 23000 Algeria aouf.zineb27@gmail.com.
² Higher National School of Forests Khenchela Algeria.
³ Nantes Université, CNRS, CEISAM, UMR 6230 Nantes F-44000 France.

Abstract

This paper describes a flexible strategy to access diethyl ((((N-(2-chloroethyl)-N-nitrososulfamoyl)amino)arylmethyl) phosphonates, as aryl analogues of fotemustine. The new aryl sulfamidophosphonates prepared from 2-chloroethylamine were successfully obtained under eco-environmental conditions using ultrasound irradiation. These compounds did not produce the expected nitroso analogues of fotemustine after the nitrosation reaction but the corresponding sulfamates which were fully characterized. Some attempts to understand this rearrangement reaction were conducted, and particularly the corresponding nitrosoureas analogues could be isolated with good yield. The novel sulfonamidophosphonates as well as their sulfamate derivatives were evaluated for their cytotoxic effect on a panel of tumor cells.