<HashMap><database>GEO</database><file_versions><headers><Content-Type>application/xml</Content-Type></headers><body><files><Other>ftp://ftp.ncbi.nlm.nih.gov/geo/series/GSE307nnn/GSE307905/</Other></files><type>primary</type></body><statusCode>OK</statusCode><statusCodeValue>200</statusCodeValue></file_versions><scores/><additional><omics_type>Transcriptomics</omics_type><species>Homo sapiens</species><gds_type>Expression profiling by high throughput sequencing</gds_type><full_dataset_link>https://www.ncbi.nlm.nih.gov/geo/query/acc.cgi?acc=GSE307905</full_dataset_link><repository>GEO</repository><entry_type>GSE</entry_type></additional><is_claimable>false</is_claimable><name>Tandem bispecific IL-7 receptor agonist antibody</name><description>Interleukin-7 (IL-7) is essential for T cell immunity, but the therapeutic application of existing IL-7 therapies is limited by narrow therapeutic window and suboptimal pharmacokinetics. To address this, we engineered a fully human tandem bispecific antibody, TB4, that functions as a potent IL-7 receptor (IL-7R) agonist by cross-linking the IL-7Rα and γc subunits. In primary human T cells, TB4 exhibited potent bispecific binding and induced sustained STAT5 signaling, a feature potentially associated with its slow antibody internalization rate. TB4 promoted T cell survival and the preferential expansion of CD4⁺ memory T cells. Notably, transcriptomic analysis revealed that TB4 induces a unique transcriptional signature enriched in genes associated with antiviral and innate immune responses, distinguishing it from native IL-7. These findings highlight TB4 as a promising IL-7R agonist with the potential to act as a subset-specific T cell immunomodulator, shaping both the expansion and functional profile of T cells.</description><dates><publication>2026/06/29</publication></dates><accession>GSE307905</accession><cross_references><GSM>GSM9233780</GSM><GSM>GSM9233782</GSM><GSM>GSM9233781</GSM><GSM>GSM9233777</GSM><GSM>GSM9233776</GSM><GSM>GSM9233787</GSM><GSM>GSM9233779</GSM><GSM>GSM9233778</GSM><GSM>GSM9233784</GSM><GSM>GSM9233783</GSM><GSM>GSM9233786</GSM><GSM>GSM9233785</GSM><GPL>21697</GPL><GSE>307905</GSE><taxon>Homo sapiens</taxon></cross_references></HashMap>