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Strategy for designing selective α-L-rhamnosidase inhibitors: Synthesis and biological evaluation of DMDP cyclic isothioureas

Abstract:
This study shows that the cyclization of L-DMDP thioureas to bicyclic L-DMDP isothioureas improved a-Lrhamnosidase inhibition which was further enhanced by increasing the length of the alkyl chain. The addition of a long alkyl chain, such as decyl or dodecyl, to the nitrogen led to the production of highly potent inhibitors of a-L-rhamnosidase; it also caused broad inhibition spectrum against b-glucosidase and b-galactosidase. In contrast, the corresponding N-benzyl-L-DMDP cyclic isothioureas display selective inhibition of a-L-rhamnosidase; 30,40-dichlorobenzyl-L-DMDP cyclic isothiourea (3r) was found to display the most potent and selective inhibition of a-L-rhamnosidase, with IC50 value of 0.22 lM, about 46-fold better than the positive control 5-epi-deoxyrhamnojirimycin (5-epi-DRJ; IC50 = 10 lM) and occupied the active-site of this enzyme (Ki = 0.11 lM). Bicyclic isothioureas of ido-L-DMDP did not inhibit a-L-rhamnosidase. These new mimics of L-rhamnose may affect other enzymes associated with the biochemistry of rhamnose including enzymes involved in progression of tuberculosis.*
Publication status:
Published
Peer review status:
Peer reviewed

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Publisher copy:
10.1016/j.bmc.2016.10.015

Authors


More from this funder
Funding agency for:
Adachi, I
Kato, A
Grant:
JP15K08021
JP26460143
More from this funder
Funding agency for:
Fleet, G


Publisher:
Elsevier
Journal:
Bioorganic and Medicinal Chemistry More from this journal
Volume:
25
Issue:
1
Pages:
107-115
Publication date:
2016-10-15
Acceptance date:
2016-10-09
DOI:
EISSN:
1464-3391
ISSN:
0968-0896


Keywords:
Pubs id:
pubs:656430
UUID:
uuid:e9964f96-69d7-41be-8d6e-2feb355f9833
Local pid:
pubs:656430
Source identifiers:
656430
Deposit date:
2016-11-01
ARK identifier:

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