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How human cells form and deliver the redox cofactor FAD in health and diseases
Job Location
it, Italy
Job Description
Organisation/Company: Università degli studi di Bari Research Field: Biological sciences Researcher Profile: Recognised Researcher (R2), Leading Researcher (R4), First Stage Researcher (R1), Established Researcher (R3) Country: Italy Application Deadline: 15 Jan 2025 - 23:59 (UTC) Type of Contract: To be defined Job Status: Not Applicable Is the job funded through the EU Research Framework Programme? Not funded by a EU programme Is the Job related to staff position within a Research Infrastructure? No Offer Description This project deals with investigations on the alterations of FAD synthase (FADS), the last enzyme in FAD biosynthesis, coded by the FLAD1 gene, whose mutations are causative of a mitochondria-affecting neuro-muscular derangement, named LSMFLAD. Therapeutic strategies are needed to treat severe LSMFLAD phenotype. Additionally, increased expression of FLAD1 has been associated with different kinds of tumors, thus prompting research on FADS. To date, three different protein isoforms, generated by FLAD1 alternative splicing, have been characterized: isoform 1, which is destined to mitochondria; isoform 2, localized in the cytosol; and a shortest isoform, an emergency protein crucial for LSMFLAD patients’ survival. The latter enzyme, a single domain protein, is responsible for FAD synthesis; isoforms 1 and 2 consist of two principal domains and a smaller interdomain region involved in protein dimerization. J-18808-Ljbffr
Location: it, IT
Posted Date: 1/12/2025
Location: it, IT
Posted Date: 1/12/2025
Contact Information
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