hCRBN
모델명
C57BL/6JSmo-Crbntm1(hCRBN)Smoc
카탈로그
NM-HU-225071
모델 상태
Repository Live
유전자 요약
Gene Symbol
Crbn
모델 설명
검증 데이터
Fig.1 Detection of CRBN expression in spleen, brain, liver, intestine and muscle tissues by RT-PCR.
Wild type: only one band at 185 bp with primers F1/R1 (mCrbn);
Homozygous: one band at 262 bp with primers F2/R2 (hCRBN) and one band at 374 bp with primers F3/R3 (hCRBN);
Abbr. M, DNA marker; HO, homozygous; WT, wild type.
Fig.2 Expression characterization of hCRBN in homozygous hCRBN mice by Western blot.
Fig.3 The degradation of GSPT1, CK1a and Myc by Lenalidomide and CC-885 in hCRBN knockin mice were determined by western blot.
The splenocytes derived from wild-type C57BL/6 (WT) and homozygous hCRBN KI (HO) mice were treated with 1% DMSO, Lenalidomide (10 nM, 100 nM, 1000 nM) and CC-885 (10 nM, 100 nM, 1000 nM) ,respectively, in RPMI-1640 cell culture medium for 18 hours ex vivo.
Tabel 1. Body weight and organs weight of WT C57BL/6 mice and hCRBN knockin mice. Values are shown as Mean±SME.
Abbr. HO, homozygous; WT, wild type.
Table 2. Blood routine examination of hCRBN knockin mice. Values are expressed as mean±SEM.
Abbr. HO, homozygous; WT, wild type.
Table 3. Biochemical test of serum from hCRBN knockin mice. Values are expressed as mean±SEM.
Abbr. HO, homozygous; WT, wild type.
Fig.4 Detection of myeloid cell subsets (A) and myeloid cell subsets (B) in the Blood and Spleen of hCRBN knockin mice by FACS (n=3 in all groups, 7-9 weeks old).
Abbr. WT, wild type; HO, homozygous.
Fig.5 Blood concentration curves of Lenalidomidein in C57BL/6 and HO hCRBN mice (female, 10wks, n=3).
(In cooperation with a client)
Fig.6 Blood concentration of CC-885 in C57BL/6 and hCRBN mice 1h after first administration (female, 10wks).
(In cooperation with a client)
Fig.7 Mean body weight (A) and survival curve (B) of C57BL/6 and HO hCRBN KI mice treated with CC-885 or vehicle (n=8/group).
All hCRBN mice treated with CC-885 dead within 2 days, while mice from other groups survived. The result indicates that CC-885 exhibits significant toxicity only in hCRBN humanized mice (In cooperation with a client).
Fig.8 The degradation of GSPT1, CK1a and Myc by CC-885 in C57BL/6 and hom hCRBN knockin mice in vivo (In cooperation with a client).
The wild-type C57BL/6 (WT, group 1&2) and homozygous hCRBN KI (HO, group 3&4) mice were treated with vehicle (group 1&3) and 5 mg/kg CC-885 (group 2&4) , respectively. The mice were anesthetized, perfused, and tissues were harvested at 6 hr post the 2nd administration.
Fig.9 Partial representative pictures of small intestine pathology (Magnification: 200x).
(In cooperation with a client)
Fig.10 Partial representative pictures of liver pathology (Magnification: 200x).
(In cooperation with a client)
Fig.11 Partial representative pictures of spleen pathology (Magnification: 200x).
(In cooperation with a client)
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Shanghai Model Organisms Center Inc has licensed CRISPR-Cas9 technology from Broad Institute
On Dec 16, 2018, Broad Institute and Shanghai Model Organisms Center Inc (SMOC) has entered into a non-exclusive license agreement under which Broad has granted SMOC worldwide rights to commercialize a service platform for genetically modified mouse models under Broad's intellectual property.
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