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B6-hLPA (CKI) /Alb-cre Mouse
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B6-hLPA (CKI) /Alb-cre Mouse
제품명
B6-hLPA (CKI) /Alb-cre Mouse
제품 ID
C001522
품종 계통
C57BL/6NCya-Gt(ROSA)26Sorem1(CAG-LSL-hLPA)Tg(Alb-Cre)/Cya
Backgroud
C57BL/6NCya
상태
이 마우스 계통을 논문에서 사용할 경우, “B6-hLPA (CKI) /Alb-cre Mouse (카탈로그 번호 C001522)은 Cyagen에서 구입하였습니다.”라고 명시해 주시기 바랍니다.
Metabolic Target Humanized Mouse Models
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.
가격 문의
Metabolic Target Humanized Mouse Models
기본 정보
검증 데이터
관련 자료
기본 정보
유전자명
유전자 별칭
LP, AK38, APOA
NCBI ID
염색체
Chr 6
MGI ID
--
Datasheet
품종 계통 설명
Lipoprotein A (LPA) is a type of particle similar to low-density lipoprotein (LDL) that is considered one of the risk factors for cardiovascular disease (CVD), such as atherosclerosis, coronary heart disease, stroke, etc [1]. LP(a) is similar in size and lipid content to LDL (low-density lipoprotein) and also contains the lipoprotein ApoB-100. However, unlike LDL, LP(a) additionally contains a variable-length lipoprotein called Apo(a), which covalently binds to ApoB-100 through a single disulfide bond. LP(a) plays an important role in systemic lipid transport, guiding inflammatory cells into blood vessel walls and leading to smooth muscle cell proliferation. Furthermore, it is involved in wound healing and tissue repair, interacting with the components of blood vessel walls and the extracellular matrix [2]. However, LP(a) can also cause arterial narrowing by adhering to the arterial wall, accelerating the formation of blood clots, and thereby triggering a series of pathological changes related to coronary heart disease, cardiovascular disease, atherosclerosis, thrombus formation, and stroke [3].
The plasma concentration of LP(a) is closely related to genetic factors and is primarily regulated by the LPA gene. Therefore, the LPA gene is an important potential target for cardiovascular disease treatment. The LPA gene encodes a serine protease that inhibits the activity of tissue-type plasminogen activator I. Fragments of this protein, generated through protein hydrolysis, can adhere to atherosclerotic lesions in arteries, promoting blood clot formation. The LPA gene is expressed in both humans and non-human primates but is not expressed in mice. Constructing mouse models expressing the human LPA gene is of significant importance for developing lipid-lowering drugs, which can drive the development of novel therapies for cardiovascular diseases. Currently, various novel therapies targeting the transcription rate of the LPA gene are under development, including small interfering RNA (siRNA) and antisense oligonucleotides (ASO) [4].
This strain was generated by mating B6-hLPA(CKI) mice (catalog number: C001521) with Alb-Cre mice (liver-specific Cre-expressing mice), resulting in a mouse model with liver-specific overexpression of the human LPA gene. B6-hLPA(CKI)/Alb-cre mice can be used to study the relationship between the LPA gene and hyperlipidemia and related cardiovascular diseases.
Reference
Kronenberg F. Lipoprotein(a). Handb Exp Pharmacol. 2022;270:201-232.
Brown MS, Goldstein JL. Plasma lipoproteins: teaching old dogmas new tricks. Nature. 1987 Nov 12-18;330(6144):113-4.
Kamstrup PR, Tybjærg-Hansen A, Nordestgaard BG. Lipoprotein(a) and risk of myocardial infarction--genetic epidemiologic evidence of causality. Scand J Clin Lab Invest. 2011 Apr;71(2):87-93.
Alebna, P. L., & Mehta, A. (2023, September 19). An Update on Lipoprotein(a): The Latest on Testing, Treatment, and Guideline Recommendations. American College of Cardiology. https://www.acc.org/latest-in-cardiology/articles/2023/09/19/10/54/an-update-on-lipoprotein-a
Nicholls SJ. Therapeutic Potential of Lipoprotein(a) Inhibitors. Drugs. 2024 Jun;84(6):637-643.
변형 전략
To obtain B6-hLPA(CKI)/Alb-cre mice with liver-specific overexpression of the human LPA gene, B6-hLPA(CKI) mice (catalog number: C001521) were bred with Alb-Cre mice (liver-specific Cre-expressing mice).
응용 분야
Research on atherosclerosis, hyperlipidemia, thrombotic cardiovascular diseases, etc;
Preclinical evaluation of human LPA-targeted drugs.
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