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ABT1 modifies SMARD1 pathology via interactions with IGHMBP2 and stimulation of ATPase and helicase activity

JCI Insight. 2023-01; 
Gangadhar P Vadla, Sara M Ricardez Hernandez, Jiude Mao, Mona O Garro-Kacher, Zachary C Lorson, Ronin P Rice, Sarah A Hansen, Christian L Lorson, Kamal Singh, Monique A Lorson
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Molecular Biology Reagents … processing) to position 618 was synthesized (GenScript) and were then in vitro transcribed according … The human U3 snoRNA was synthesized (GenScript) and then in vitro transcribed. … Get A Quote

摘要

SMA with respiratory distress type 1 (SMARD1) and Charcot-Marie-Tooth type 2S (CMT2S) are results of mutations in immunoglobulin mu DNA binding protein 2 (IGHMBP2). IGHMBP2 is a UPF1-like helicase with proposed roles in several cellular processes, including translation. This study examines activator of basal transcription 1 (ABT1), a modifier of SMARD1-nmd disease pathology. Microscale thermophoresis and dynamic light scattering demonstrate that IGHMBP2 and ABT1 proteins directly interact with high affinity. The association of ABT1 with IGHMBP2 significantly increases the ATPase and helicase activity as well as the processivity of IGHMBP2. The IGHMBP2/ABT1 complex interacts with the 47S pre-rRNA 5' external tra... More

关键词

Genetic diseases, Genetics, Molecular genetics, Neurological disorders, Neuroscience