Role of serum interleukin-6 in deciding therapy for multidrug resistant oral lichen planus
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Goel, Sinny; Marwah, Akanksha; Kaushik, Smita; Garg, Vijay K.; Gupta, Sunita
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Aquest document és un/a article, creat/da en: 2015
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Background: Oral lichen planus (OLP) is a T cell mediated immune response. T cells locally present in the involved
tissues release cytokines like interleukin-6 (IL-6), which contributes to pathogenesis of OLP. Also IL-6 has been
associated with multidrug resistance protein (MRP) expression by keratinocytes. Correspondingly, upregulation of
MRP was found in OLP. We conducted this study to evaluate the effects of various drugs on serum IL-6 in OLP; and
correlation of these effects with the nature of clinical response and resistance pattern seen in OLP lesions with various
therapeutic modalities. Thus we evaluated the role of serum IL-6 in deciding therapy for multidrug resistant OLP.
Material and Methods: Serum IL-6 was evaluated in 42 erosive OLP (EOLP) patients and 10 normal mucosa and
10 oral squamous cell carcinoma cases using ELISA technique. OLP patients were randomly divided into 3 groups
of 14 patients each and were subjected to Pimecrolimus local application, oral Mycophenolate Mofetil (MMF)
and Methotrexate (MTX) alongwith Pimecrolimus local application. IL-6 levels were evaluated before and after
treatment.
Results: Serum IL-6 levels were raised above 3pg/ml in 26.19% erosive OLP (EOLP) cases (mean- 3.72±8.14).
EOLP (5%) cases with IL-6 levels above 5pg/ml were resistant in MTX group. However significant decrease in
serum IL-6 corresponding with the clinical resolution was seen in MMF group.
Conclusions: Significantly raised IL-6 levels in EOLP reflect the chronic inflammatory nature of the disease. As
serum IL-6 levels significantly decreased in MMF group, correspondingly no resistance to treatment was noted.
However with MTX there was no significant decrease in IL-6 and resistance to treatment was noted in some, especially plaque type lesions. Thus IL-6 can be a possible biomarker in deciding the best possible therapy for treatment
resistant OLP.
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