DNA interstrand crosslinking and sequence selectivity of dimethanesulphonates (original) (raw)

• Experimental Oncology
• Published: 01 May 1991

British Journal of Cancer volume 63, pages 743–747 (1991)Cite this article

• 220 Accesses
• 29 Citations
• Metrics details

Abstract

Members of the homologous series of alkanediol dimethanesulphonates of general formula H3C.SO2O.(CH2)n.O.SO2.CH3 have been tested for their ability to produce DNA interstrand crosslinking and DNA sequence selectivity of guanine-N7 alkylation. In a sensitive crosslinking gel assay the efficiency of DNA interstrand crosslink formation, dependent on the ability of the alkylating moiety to span critical nucleophilic distances within the DNA, was found at 6 h to be 1,6-hexanediol dimethanesulphonate (Hexa-DMS) (n = 6) greater than methylene dimethanesulphonate (MDMS) (n = 1) greater than 1,8-octanediol dimethanesulphonate (Octa-DMS) (n = 8) greater than Busulphan (n = 4). The DNA interstrand crosslinking produced by MDMS was not due to either of its hydrolysis products, formaldehyde or methanesulphonic acid (MSA). In contrast the extent of monoalkylation at guanine-N7 as determined by a modified DNA sequencing technique was found to be Busulphan much greater than Hexa-DMS = Octa-DMS, with a sequence selectivity somewhat less than that of other chemotherapeutic alkylating agents such as nitrogen mustards. MDMS at high levels induced a non-specific depurination as a result of the reduction in pH resulting from MSA release. More strikingly MDMS (and MSA) produced a single strong site of guanine reaction (depurination) in a guanine-rich 276 base pair fragment of pBR322 DNA in the sequence of 5'-ATGGTGG-3'. This was observed when non-specific depurination was negligible and was not seen with formic acid. Thus structurally similar alkylating agents can differ in their type and extent of DNA monoalkylation and interstrand crosslinking, and in some cases (e.g. MDMS/MSA) produce reactions with a high degree of selectivity.

This is a preview of subscription content, access via your institution

Access options

Subscribe to this journal

Receive 24 print issues and online access

$259.00 per year

only $10.79 per issue

Buy this article

• Purchase on SpringerLink
• Instant access to full article PDF

Prices may be subject to local taxes which are calculated during checkout

Additional access options:

• Log in
• Learn about institutional subscriptions
• Read our FAQs
• Contact customer support

Similar content being viewed by others

Author information

Authors and Affiliations

1. Department of Oncology, University College and Middlesex School of Medicine, London, UK
   M Ponti

Authors

1. M Ponti
   You can also search for this author inPubMed Google Scholar
2. RL Souhami
   You can also search for this author inPubMed Google Scholar
3. BW Fox
   You can also search for this author inPubMed Google Scholar
4. JA Hartley
   You can also search for this author inPubMed Google Scholar

Rights and permissions

About this article

Cite this article

Ponti, M., Souhami, R., Fox, B. et al. DNA interstrand crosslinking and sequence selectivity of dimethanesulphonates.Br J Cancer 63, 743–747 (1991). https://doi.org/10.1038/bjc.1991.166

Download citation

• Issue Date: 01 May 1991
• DOI: https://doi.org/10.1038/bjc.1991.166