Table 2.
Summary of published KLF14 mouse lines.
| Mouse line | Targeted region | Source | Diet | Sex studied | Phenotypes | Reference |
|---|---|---|---|---|---|---|
| Whole-body Klf14 knockout | 1,035 bp between positions 30907660-30908694 of Chromosome 6 (Genome Build37), including the entire Klf14 open reading frame | KOMP repository | Standard chow and 60% kcal high fat diet (switched at week 8) | Male | No difference in metabolic phenotypes; No difference was observed in whole-body Klf14 KO mice plasma lipoprotein profile, cholesterol, HDL-C. No difference in insulin resistance and adipose gene expression change. | (91) |
| CRISPR-Cas9 whole-body knockout | A 7-bp frameshift insertion-deletion allele was introduced to the 5' end of the Klf14 gene through CRISPR-Cas9 | In house | 45% kcal high fat diet (switched at week 18) | Male | Decrease in HDL-C level in Klf14 whole-body knockout mice | (1) |
| KLF14 null mouse | The loxP sites were added ~1.6 kb upstream of the Klf14 transcriptional start site and 300 bp downstream of the Klf14 3′-UTR separated by a total of 4.9 kb. Male offspring were crossed with Sox2: CRE transgenic females to generate a constitutive null allele | In house | Standard | Phenotypic analysis: female Gene expression analysis: male and female | Placenta is overgrown in Klf14hetKO mice who carry maternal Klf14 allele (Klf14matKO). Fetal size remained unchanged. No morphological change in placenta layers. No abnormal lipid accumulation in Klf14matKO mice. | (94) |
| Klf14-KO mice | Klf14 exon is disrupted by deleting 8-bp sequence using TALEN, which further disrupted the tenth amino acid and resulted in premature termination. | In house | Standard chow | NA | 33.3% of Klf14-KO adult mice developed tumors in lung, spleen, and lymph nodes starting from 11-month-old. No spontaneous tumor was identified in other organs such as the heart, liver, kidney, breast, colon, and thymus. No obvious difference in body weight and serum lipids in KO mice. | (95) |
| Adipose-specific Klf14 KO (AdnKlf14-KO) | Two LoxP sites were inserted at 3,415 bp upstream and 327 bp downstream of Klf14 through CRISPR-Cas9. Offspring with two loxP sequences segregated on the same chromosome were crossed with Adipoq-Cre mice of the same genetic background | In house | Standard chow | Male and female | HDL-C was reduced in female AdnKlf14-KO mice while triglycerides were increased in males. Glucose tolerance and insulin sensitivity were impaired in both sexes | (1) |
| Liver-specific Klf14 KO (Klf14-LKO) | Klf14 exon flanked by LoxP sites (specific targeted region unknown), followed by germline transmission and Flp recombinase removal. Offspring were crossed with Alb-Cre transgenic mice (003574 from Jackson Laboratory) | In house | Standard chow | Male | Pooled blood serum was collected and analyzed by HPLC. Total cholesterol and triglyceride levels were comparable between WT and Klf14-LKO mice. HDL-C level was decreased in Klf14-LKO mice. ApoA-1 level was also decreased in hepatic Klf14 KO mice liver. | (92) |