The Role Of IL-6 In TMPD-Treated Lupus Arthritis Mice
Abstract
Lupus or systemic lupus erythematosus is a chronic autoimmune disease with
systemic inflammation manifestations mainly in targeted organs. The appropriate
animal model for lupus is necessary. The induction method by using 2,6,10,14
tetramethylpentadecane (TMPD) reveals more complex manifestations than other
hydrocarbons. However, the autophagy of macrophages as an effect of TMPD
makes differences to make the decision in lupus biomarker as a targeted therapy
in lupus arthritis. Thus, this research focused on the role of CD68+IL-6 produced
by macrophages and total IL-6 in lupus in correlation to the arthritis severity. The
naïve and TMPD-treated groups (n=3) were induced by means of 0.5 ml TMPD i.p.
After 6 months, the mice were sacrificed then the fresh spleens were prepared
as isolated cells to be measured by using flow cytometry method. The knee joints
were prepared for histology observation. The statistical analysis was performed
by using T-test SPSS 22 version. The results showed the relative percentage of
CD68+IL-6+ in the TMPD-treated group increased significantly (P<0.05) with the
value of 62.38±9.97 %, compared to naïve group 49.70±2.34 %. Moreover, the total
IL-6 did not increase significantly (P>0.05). Meanwhile, the arthritis severity score of
the TMPD-treated group revealed severe erosion with the grade of 3.7±1.06, higher
significantly (P<0.05) than the naïve group (0.5±0.71). The joint spaces in both groups
were not significantly different. Finally, the observations gave the clear information
that despite the autophagy potency, the CD68+IL-6 and the arthritis severity score
were good markers in lupus preclinical study
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