hIL12B/hIL23A
品系全名
C57BL/6JSmo-Il23atm3(hIL23A)Il12btm3(hIL12B)Smoc
目录号
NM-HU-233778
品系状态
活体
品系描述
验证数据
Fig.1 Detection of hIL23 and mIL23 expression in serum by ELISA (n=2).
Abbr. HO, homozygous; WT, wild type.
Note. hIL23A/hIL12B and C57BL/6 mice were i.p. injected with LPS.
Table.1 Blood chemistry examination in 6-week-old HO/HO hIL23A/hIL12B mice (n=3 /group).
Table.2 Blood routine examination in 6-week-old HO/HO hIL23A/hIL12B mice (n=3 /group).
Fig.2 In vivo efficacy evaluation of anti-IL23 (Risankizumab, 20mpk, i.p., Q3D) and anti-IL23/IL12 (Ustekinumab, 20mpk, i.p., Q3D) in imiquimod (IMQ)-induced psoriasis model in hIL23A/hIL12B mice (3-6 mice/group, 6 weeks, female). IMQ treatment induced body weight loss in female hIL23A/hIL12B mice. Neither Risankizumab nor Ustekinumab treatment alleviated this weight loss, with both antibody-treated groups showing final body weight reductions.
Fig.3 In vivo efficacy evaluation of anti-IL23 (Risankizumab, 20mpk, i.p., Q3D) and anti-IL23/IL12 (Ustekinumab, 20mpk, i.p., Q3D) in imiquimod (IMQ)-induced psoriasis model in hIL23A/hIL12B mice (3-6 mice/group, 6 weeks, female). IMQ treatment successfully induced psoriasis-like skin inflammation in female hIL23A/hIL12B mice, characterized by increased skin thickness and elevated PASI scores (including erythema and scaling) over the 7-day observation period. Notably, Risankizumab demonstrated better therapeutic effect than Ustekinumab in lleviating IMQ-induced psoriasis.
Fig.4 In vivo efficacy study of Risankizumab and Ustekinumab in HO hIL23A/hIL12B mice. H&E staining of psoriatic skin lesions in IMQ-induced mice. Compared to the control group (A) , all IMQ-treated groups displayed skin thickening. The IMQ+Vehicle (B) and IMQ+Ustekinumab (D) groups showed progressive and plaque-stage psoriasis symptoms focal parakeratosis, spongiosis, twisted and dilated capillaries (Black), and lymphocytic infiltration in the dermal papillae (Red), whereas the IMQ+Risankizumab group (C) showed reduced epidermal thickness and ameliorated histopathological features. IMQ treatment induced significant psoriasis-like skin thickening and histopathological features, including parakeratosis, spongiosis, dilated capillaries, and lymphocytic infiltration, as seen in the IMQ induced groups. Comparing to Ustekinumab, Risankizumab treatment significantly alleviated these psoriatic symptoms and reduced epidermal thickness, demonstrating its therapeutic effect in this IMQ-induced psoriasis model. Scale bar = [500] µm.
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