This is where comes into play. Standing for the Database for Annotation, Visualization, and Integrated Discovery , DAVID has become a cornerstone platform for functional genomic analysis. Since its inception at the National Institute of Allergy and Infectious Diseases (NIAID/NIH), DAVID has helped over 40,000 unique users from more than 100 countries transform raw gene lists into meaningful biological hypotheses.
Click "Functional Annotation Tool." A results dashboard will appear. The most important section is the Functional Annotation Clustering . Click "Functional Annotation Clustering Report." david bioinformatics resources
https://david.ncifcrf.gov Keywords: DAVID bioinformatics resources, functional annotation, gene enrichment analysis, GO analysis, KEGG pathway, DAVID 2.0, genomic data interpretation. This is where comes into play
By democratizing access to complex functional annotation, DAVID bridges the gap between high-throughput data and low-throughput validation, ensuring that the time, money, and effort invested in genomics leads to real biological discovery. Click "Functional Annotation Tool
Examine the clusters. A Cluster Enrichment Score > 1.3 is typically considered significant, but scores > 2.0 or > 3.0 indicate very strong biological relevance. Click on each cluster to expand it and see the individual annotation terms (GO terms, KEGG pathways, etc.) along with their raw p-values, Bonferroni-corrected p-values, and Benjamini-Hochberg FDR values. Case Studies: Real-World Applications of DAVID The utility of DAVID spans virtually every domain of life science research. Oncology (Cancer Research) A researcher studying breast cancer metastasis identifies 300 genes upregulated in invasive cells. Using DAVID, they find that the top annotation cluster is "extracellular matrix reorganization" (collagens, MMPs, integrins). A secondary cluster reveals "epithelial-to-mesenchymal transition" (Snail, Twist, Vimentin). These results immediately guide the researcher toward validated hypotheses for drug targeting. Infectious Disease A virologist infects human lung cells with influenza and sequences the host transcriptome. DAVID analysis of downregulated genes identifies a significant enrichment for "ribosomal proteins" and "translation initiation factors," suggesting the virus hijacks or shuts off host translation. This insight directs the lab to investigate specific viral proteins that interact with eIF4G. Plant Biology An agronomist studies drought tolerance in Arabidopsis . After exposing plants to dehydration stress, they submit the resulting gene list to DAVID. The platform returns "response to abscisic acid," "stomatal closure," and "osmolyte biosynthesis" as top clusters, confirming the physiological data and revealing novel regulatory candidates. Limitations and Best Practices While DAVID is powerful, no tool is perfect. Sophisticated users must be aware of its limitations.
Navigate to david.ncifcrf.gov . Paste your gene list (e.g., a column of 200 gene symbols) into the upload window. Select the correct identifier type (e.g., "OFFICIAL_GENE_SYMBOL"). Choose the list type ("Gene List").