02032nas a2200349 4500000000100000008004100001260001300042653002400055653003800079653001600117653001100133653002300144653001200167653001500179653002400194100001300218700001300231700001300244700001200257700001800269700000900287700001100296700000900307700000900316700001300325245013800338856007200476300001100548490000600559520110300565022001401668 2001 d c2001 Jan10aAntigens, Bacterial10aEnzyme-Linked Immunosorbent Assay10aGlycolipids10aHumans10aLeprostatic Agents10aleprosy10atratamento10aProspective Studies1 aBalagon 1 aCellona 1 aFajardo 1 aAbalos 1 aVillahermosa 1 aTan 1 aWalsh 1 aCho 1 aKim 1 aBrennan 00aDetection of phenolic glycolipid I of Mycobacterium leprae in sera from leprosy patients before and after start of multidrug therapy. uhttps://www.ncbi.nlm.nih.gov/pmc/articles/PMC96023/pdf/cd000138.pdf a138-420 v83 a
A total of 100 untreated new leprosy patients were recruited prospectively and examined for the presence of phenolic glycolipid I (PGL-I) antigen in their serum specimens by dot enzyme-linked immunosorbent assay (ELISA) using rabbit anti-PGL-I antiserum. The presence of circulating PGL-I antigen was closely related to the bacterial indices (BI) of the patients. The PGL-I antigen was detectable in 27 (93.1%) of 29 patients with a BI of 4.0 or above and in 15 (68.2%) of 22 patients with a BI of 3.0 to 3.9. However, none of the 37 patients with a BI of less than 1.9 had detectable PGL-I antigen by the methods used in this study. The level of PGL-I in serum declined rapidly by about 90% 1 month after the start of multidrug therapy. This study showed clearly that anti-PGL-I IgM antibodies and circulating PGL-I antigen levels reflect the bacterial loads in untreated leprosy patients. The serological parameters based on the PGL-I antigen may therefore be useful in the assessment of leprosy patients at the time of diagnosis and possibly in monitoring patients following chemotherapy.
a1071-412X