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Apoe Knockout mouse models

Apoe influences lipoprotein metabolism and is a cornerstone of cardiovascular and Alzheimer disease research. The humanized alleles at this locus helped translate diet studies and immunotherapy ideas into preclinical formats that match human isoforms. Knockout and tissue restricted designs still matter when the question is receptor biology in liver versus microglia. Many cohorts now combine humanized Apoe with pathological transgenes for head to head comparisons.

Whole body loss of Apoe gives the clearest readout when the question is whether the gene is required at all. Follow up tissue work may still move to a conditional allele if lethality or compensation appears.

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Catalog table

A conventional knockout answers whether the gene is required broadly. When your target tissue is the organ of interest, a global null can still be informative if viability is acceptable and you want the simplest genotype. If the null is harsh, a floxed allele with a regional Cre is the safer long term platform.

A conventional knockout answers whether the gene is required broadly. When liver is the organ of interest, a global null can still be informative if viability is acceptable and you want the simplest genotype. If the null is harsh, a floxed allele with a regional Cre is the safer long term platform.

ModelTypeCategoryAvailabilityCatalog #Action
Apoe-KO(2)KnockoutKO/CKO mice, disease model miceliveKO 190565Inquire

Why this approach

A conventional knockout answers whether the gene is required broadly. When your target tissue is the organ of interest, a global null can still be informative if viability is acceptable and you want the simplest genotype. If the null is harsh, a floxed allele with a regional Cre is the safer long term platform.

A conventional knockout answers whether the gene is required broadly. When liver is the organ of interest, a global null can still be informative if viability is acceptable and you want the simplest genotype. If the null is harsh, a floxed allele with a regional Cre is the safer long term platform.

Build timeline and pricing

Typical custom projects target study ready cohorts near twenty six weeks from contract start when breeding is direct. Quotes return in about twenty four hours with milestones, pricing, and options for cryo or live dispatch.

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FAQ

How long does a Apoe knockout project take?

Most custom knockout projects run near twenty six weeks from contract activation to study ready animals when breeding is straightforward. Complex humanization or multi allele stacks can add time. We return detailed quotes within about twenty four hours so you can align cohort start dates with grant or IND milestones.

Is Apoe knockout embryonic lethal in mice?

Lethality depends on genetic background and exact allele design. Some Apoe germline knockouts are viable, others require conditional alleles or mixed backgrounds. We review publications and our own experience, then recommend floxed versus null approaches before you commit.

Which Cre driver is best for experiments?

Driver choice depends on onset timing, recombination efficiency, and known leak patterns. We map your organ and cell type to a short list of proven Cre lines, then discuss reporter crosses and controls. We prioritize drivers with strong community validation for your tissue.

Do you ship live Apoe animals?

When catalog lines are live, we ship with health certificates and QC documentation. If your exact combo is not listed, we quote a custom project with cryo or live dispatch options depending on cohort timing and geography.

How do I request a quote for Apoe?

Use the catalog inquire buttons or the request quote form with your allele goal, Cre plan if any, strain background, and cohort size. A PhD led team responds with pricing, milestones, and the fastest path to experimental animals.

Related models and routes

All Apoe models
Apoa1 KnockoutApoa2 KnockoutApoa4 KnockoutApob KnockoutApobec3 KnockoutApoc1 KnockoutApoc3 KnockoutApoc4 Knockout

Citations