Please use this identifier to cite or link to this item: http://223.31.159.10:8080/jspui/handle/123456789/1819
Title: UBA1-CDK16: A female-specific chimeric RNA emerging through evolution and involved in immune regulation
Authors: Shi, Xinrui
Blackburn, Loryn
Singh, Sandeep
Glowczyk-Gluc, Martyna
Tajammal, Anam
Zahra, Shafaque
Kumar, Shailesh
Cornelison, Robert
Liang, Chen
Qin, Fujun
Liu, Aiqun
Lin, Shitong
Tang, Yue
Elfman, Justin
Manley, Thomas
Bullock, Timothy
Haverstick, Doris M.
Wu, Peng
Li, Hui
Keywords: UBA1-CDK16
female-specific chimeric RNA
immune regulation
Issue Date: 2026
Publisher: American Association for the Advancement of Science
Citation: Science Advances, 12(22): eadz9784
Abstract: Chimeric RNAs resulting from intergenic splicing represent a distinct mechanism for transcriptome expansion. To explore the role of this previously unidentified layer of the transcriptome in sex-specific immunity, we analyzed RNA sequencing data from 425 blood samples and identified a female-specific chimeric RNA, UBA1-CDK16, which was further validated in more than 1200 blood samples. This chimeric RNA forms via cis-splicing between two adjacent X-linked parental genes, UBA1 and CDK16, despite both being expressed in both sexes. We demonstrated that a female-specific chromatin loop at the UBA1-CDK16 junction sites facilitates the intergenic splicing. Evolutionary analysis revealed that UBA1-CDK16 became female specific in humans through at least two independent paths. Functional studies suggested that UBA1-CDK16 is enriched in the myeloid lineage and may regulate myeloid cell development. Notably, its abnormal expression in female patients with COVID-19 correlates with altered neutrophil counts, highlighting its potential role in the disease progression.
Description: Accepted date: April 21, 2026
URI: https://www.science.org/doi/10.1126/sciadv.adz9784
http://223.31.159.10:8080/jspui/handle/123456789/1819
ISSN: 2375-2548
Appears in Collections:Institutional Publications

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