Cish-flox Mouse
Common Name
Cish-flox
제품 ID
S-CKO-01734
Backgroud
C57BL/6JCya
품종 계통계통 ID
CKOCMP-12700-Cish-B6J-VA
상태
이 마우스 계통을 논문에서 사용할 경우, “Cish-flox Mouse (카탈로그 번호 S-CKO-01734)은 Cyagen에서 구입하였습니다.”라고 명시해 주시기 바랍니다.
구매 가능한 제품 종류
연령
Genotype
성별
수량
표준 제공 조건은 최소 3마리의 이형접합(heterozygous) 보균자를 보장합니다. 동형접합(homozygous) 보균자 및/또는 특정 성별에 대한 브리딩 서비스도 제공됩니다.
기본 정보
품종 계통
Cish-flox
품종 계통계통 ID
CKOCMP-12700-Cish-B6J-VA
유전자명
제품 ID
S-CKO-01734
유전자 별칭
Cis, F17, F23, CIS1, SOCS, CIS-1
배경
C57BL/6JCya
NCBI ID
변형 내용
Conditional knockout
염색체
Chr 9
Phenotype
Datasheet
적용 분야
--
품종 계통 설명
Ensembl 전사체 ID
ENSMUST00000085102
NCBI 전사체 ID
NM_009895
타겟 영역
Exon 2~3
유효 영역 크기
~3.9 kb
유전자 연구 개요
Cish, also known as cytokine-inducible SH2-containing protein, is a key negative regulator in multiple cytokine signaling pathways. It belongs to the suppressor of cytokine signaling (SOCS) family. Cish plays important roles in immunity, erythropoiesis, and the regulation of cell metabolism, lysosomal function, and cell activation. Genetic models, such as gene knockout (KO) and conditional knockout (CKO) mouse models, have been crucial for studying its functions [1,2,3,4,5,6,7,8,9].
In human iPSC-derived NK cells, deletion of CISH promotes metabolic reprograming, enhancing in vivo persistence and anti-tumor activity through increased IL-15-mediated JAK-STAT signaling and improved metabolic fitness [1]. In T cells from older adults, increased CISH expression impairs lysosomal function, leading to mitochondrial DNA release and inflammaging [2]. Cish knockout mice showed altered hematopoietic responses but similar outcomes to malaria infection [3]. Targeting CISH in NK cells enhances natural cytotoxicity receptor signaling, reduces NK cell exhaustion, and improves solid tumor immunity [4]. During DC development, CISH knockdown affects the expression of key molecules, DC yield, and CTL activation [5]. In alveolar macrophages, Cish deficiency leads to phenotypic changes associated with enhanced cytokine signaling [6]. In ILC2s, global or conditional CISH deficiency increases cell expansion and activation, affecting mucosal immunity [7]. In lung fibroblasts, CISH negatively regulates IL-13-induced CCL26 production related to eosinophilic inflammation in asthma [8]. In mice infected with Mycobacterium tuberculosis, CISH controls bacterial burden early after infection via innate immune mechanisms [9].
In conclusion, Cish acts as a negative regulator in multiple biological processes, including cytokine signaling, cell metabolism, and lysosomal function. KO and CKO mouse models have revealed its roles in various disease-related conditions, such as cancer, aging-related inflammation, malaria, solid tumor immunity, asthma, and tuberculosis. These findings contribute to understanding the underlying mechanisms of these diseases and may provide potential therapeutic targets.
References:
1. Zhu, Huang, Blum, Robert H, Bernareggi, Davide, Malmberg, Karl-Johan, Kaufman, Dan S. 2020. Metabolic Reprograming via Deletion of CISH in Human iPSC-Derived NK Cells Promotes In Vivo Persistence and Enhances Anti-tumor Activity. In Cell stem cell, 27, 224-237.e6. doi:10.1016/j.stem.2020.05.008. https://pubmed.ncbi.nlm.nih.gov/32531207/
2. Jin, Jun, Mu, Yunmei, Zhang, Huimin, Weyand, Cornelia M, Goronzy, Jorg J. 2023. CISH impairs lysosomal function in activated T cells resulting in mitochondrial DNA release and inflammaging. In Nature aging, 3, 600-616. doi:10.1038/s43587-023-00399-w. https://pubmed.ncbi.nlm.nih.gov/37118554/
3. Lakkavaram, Asha L, Maymand, Saeed, Naser, Wasan, Ward, Alister C, de Koning-Ward, Tania F. 2023. Cish knockout mice exhibit similar outcomes to malaria infection despite altered hematopoietic responses. In Frontiers in microbiology, 14, 1288876. doi:10.3389/fmicb.2023.1288876. https://pubmed.ncbi.nlm.nih.gov/38029163/
4. Bernard, Pierre-Louis, Delconte, Rebecca, Pastor, Sonia, Nunes, Jacques, Guittard, Geoffrey. . Targeting CISH enhances natural cytotoxicity receptor signaling and reduces NK cell exhaustion to improve solid tumor immunity. In Journal for immunotherapy of cancer, 10, . doi:10.1136/jitc-2021-004244. https://pubmed.ncbi.nlm.nih.gov/35589278/
5. Miah, Mohammad Alam, Yoon, Cheol-Hee, Kim, Joonoh, Seong, Young-Rim, Bae, Yong-Soo. 2011. CISH is induced during DC development and regulates DC-mediated CTL activation. In European journal of immunology, 42, 58-68. doi:10.1002/eji.201141846. https://pubmed.ncbi.nlm.nih.gov/22002016/
6. Shoger, Karsen E, Cheemalavagu, Neha, Cao, Yuqi M, Singh, Harinder, Gottschalk, Rachel A. 2021. CISH attenuates homeostatic cytokine signaling to promote lung-specific macrophage programming and function. In Science signaling, 14, eabe5137. doi:10.1126/scisignal.abe5137. https://pubmed.ncbi.nlm.nih.gov/34516753/
7. Kotas, Maya E, Mroz, Nicholas M, Koga, Satoshi, Schneider, Christoph, Locksley, Richard M. 2021. CISH constrains the tuft-ILC2 circuit to set epithelial and immune tone. In Mucosal immunology, 14, 1295-1305. doi:10.1038/s41385-021-00430-6. https://pubmed.ncbi.nlm.nih.gov/34290377/
8. Takeshima, Hideyuki, Horie, Masafumi, Mikami, Yu, Nagase, Takahide, Yamauchi, Yasuhiro. 2018. CISH is a negative regulator of IL-13-induced CCL26 production in lung fibroblasts. In Allergology international : official journal of the Japanese Society of Allergology, 68, 101-109. doi:10.1016/j.alit.2018.08.005. https://pubmed.ncbi.nlm.nih.gov/30197185/
9. Carow, Berit, Gao, Yu, Terán, Graciela, Yoshimura, Akihiko, Rottenberg, Martin E. 2017. CISH controls bacterial burden early after infection with Mycobacterium tuberculosis in mice. In Tuberculosis (Edinburgh, Scotland), 107, 175-180. doi:10.1016/j.tube.2017.09.007. https://pubmed.ncbi.nlm.nih.gov/29050767/
품질 관리 기준
정자 검사
동결 보존 전: 정자 농도 측정 및 정자 생존율 평가.
동결 보존 후: 각 배치에서 동결 보존된 정자 바이알 1개를 선택하여 체외수정(in vitro fertilization)에 사용합니다.
Environmental Standards:
SPFAvailable Region:
GlobalSource:
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