hIL12B/hIL23A/hTL1A(3)

Nomenclature

C57BL/6JSmo-Tnfsf15tm1(hTNFSF15)Il23aem3(hIL23A)Il12btm3(hIL12B)Smoc

Cat. NO.

NM-XA-252106

Strain State

Repository Live

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Model Description

The hTL1A(3) (NM-HU-233157) was crossed with hIL23A/hIL12B(NM-HU-233778) to generate hTL1A(3)/hIL23A/hIL12B mice.

Validation Data

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Fig.1 Body weight and body weight change among time during study. Body weight and body weight change in anti-IL23 treated imiquimod (IMQ)-induced psoriasis in HO hTL1A/hIL23A/hIL12B mice (n=3-4 /group, 6weeks, male). IMQ treatment induced body weight loss in male hTL1A/hIL23A/hIL12B mice. Risankizumab treatment didn’t alleviate the weight loss.

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Fig.2 Psoriasis evaluation among time during study. In vivo efficacy evaluation of anti-IL23 in imiquimod (IMQ)-induced psoriasis in hTL1A/hIL23A/hIL12B mice (n=3-4 /group, 6weeks, male). IMQ treatment successfully induced psoriasis-like skin inflammation in female HO hTL1A/hIL23A/hIL12B mice, characterized by increased elevated PASI scores (including erythema and scaling) over the 7-day observation period. Notably, Risankizumab alleviated IMQ-induced psoriasis.

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Fig.3 H&E staining of psoriatic skin lesions in IMQ-induced mice. Representative H&E staining images of skin from the (A) control, (B) IMQ + vehicle, and (C) IMQ + Risankizumab groups. Scale bar = 500 µm. (D) Baker score based on HE pathology images (n=3/group, 6 weeks old). IMQ treatment induced significant psoriasis-like skin thickening and histopathological features, including parakeratosis, spongiosis, dilated capillaries, and lymphocytic infiltration, as observed in the IMQ-treated groups. Risankizumab treatment slightly alleviated these psoriatic symptoms and reduced epidermal thickness, demonstrating its therapeutic effect in this IMQ-induced psoriasis model.


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