Abstract
The mammalian Interferon induced transmembrane protein 1 (Ifitm1) gene was originally identified as a member of a gene family highly inducible by type I and type II interferons. Based on expression analyses, it was suggested to be required for normal primordial germ cell migration. The knockdown of Ifitm1 in mouse embryos provided evidence for a role in somitogenesis. We generated the first targeted knockin allele of the Ifitm1 gene to systematically reassess all inferred functions. Sperm motility and the fertility of male and female mutant mice are as in wild type littermates. Embryonic somites and the adult vertebral column appear normal in homozygous Ifitm1 knockout mice, demonstrating that Ifitm1 is not essential for normal segmentation of the paraxial mesoderm. Proportions of leucocyte subsets, including granulocytes, monocytes, B-cells, T-cells, NK-cells, and NKT-cells, are unchanged in mutant mice. Based on a normal immune response to Listeria monocytogenes infection, there is no evidence for a dysfunction in downstream IFNγ signaling in Ifitm1 mutant mice. Expression from the Ifitm1 locus from E8.5 to E14.5 is highly dynamic. In contrast, in adult mice, Ifitm1 expression is highly restricted and strong in the bronchial epithelium. Intriguingly, IFITM1 is highly overexpressed in tumor epithelia cells of human squamous cell carcinomas and in adenocarcinomas of NSCLC patients. These analyses underline the general importance of targeted in vivo studies for the functional annotation of the mammalian genome. The first comprehensive description of the Ifitm1 expression pattern provides a rational basis for the further examination of Ifitm1 gene functions. Based on our data, the fact that IFITM1 can function as a negative regulator of cell proliferation, and because the gene maps to chromosome band 11p15.5, previously associated with NSCLC, it is likely that IFITM1 in man has a key role in tumor formation.
Highlights
The Interferon induced transmembrane protein 1 (Ifitm1, fragilis2, mil-2, 9–27, Leu-13) gene belongs to a family of at least five sequence related genes (Ifitm1, Ifitm2, Ifitm3, Ifitm5, Ifitm6) located in a 68 kb gene cluster on mouse chromosome 7
We find that Ifitm1, respectively, the human protein IFITM1 are selectively expressed in the bronchial epithelia of mouse and human lung tissue and that IFITM1 is highly overexpressed in human non-small cell lung cancers (NSCLC)
The offspring of these breedings were backcrossed to the C57BL/6J strain for at least five generations and again screened by Southern blot hybridization (Fig. S1, panel B) confirming the proper targeting of the Ifitm1 gene and the deletion of the neomycin selection cassette
Summary
The Interferon induced transmembrane protein 1 (Ifitm, fragilis, mil-2, 9–27, Leu-13) gene belongs to a family of at least five sequence related genes (Ifitm, Ifitm, Ifitm, Ifitm, Ifitm6) located in a 68 kb gene cluster on mouse chromosome 7. Several putative functions have been suggested for the Ifitm genes based either on indirect experimental evidence or inferred from sequence or gene expression data. Ifitm was described as a marker for the prognosis of chronic myeloid leukemia [24]. These observations have led to the suggestion that Ifitm might be expressed as a general response to IFN signaling under various disease conditions [25,26,27]
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