Authors
Mostafa Kokabee, Xianhui Wang, Elena Voorand, Eden Alin, Leila Kokabee, Faiza Khan, Sophia Desrosiers, Douglas S Conklin
Publication date
2022/7/1
Journal
Cancer Genomics & Proteomics
Volume
19
Issue
4
Pages
415-427
Publisher
International Institute of Anticancer Research
Description
Background
The alternative transcriptional isoform of Bruton’s tyrosine kinase, BTK-C, is expressed in a wide variety of epithelial tumor types where it impacts apoptosis resistance, therapeutic escape, and glucose uptake. The initial exon in BTK-C encodes a 34 amino acid extension of the amino terminus of the canonical BTK-A isoform. Its function is unknown.
Materials and Methods
Site-directed mutagenesis, acylation assays and expression studies in cancer cell lines were used to determine the effects that the BTK-C first exon sequence has on kinase activity, subcellular localization and cell physiology. Analysis of BTK-C expression in tumors was conducted using genomic databases.
Results
BTK-C is palmitoylated on two cysteine residues. BTK-C localization at the plasma membrane is dependent upon phosphatidylinositol 3,4,5-triphosphate (PIP3) levels as well as palmitoylation. In epithelial cancer cells, both …
Total citations
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