Scholars@Duke

Data from Inhibition of Karyopherin β1-Mediated Nuclear Import Disrupts Oncogenic Lineage-Defining Transcription Factor Activity in Small Cell Lung Cancer

Publication ,  Other
Kelenis, DP; Rodarte, KE; Kollipara, RK; Pozo, K; Choudhuri, SP; Spainhower, KB; Wait, SJ; Stastny, V; Oliver, TG; Johnson, JE
March 31, 2023
Published version (DOI) Publisher Link

<div>Abstract<p>Genomic studies support the classification of small cell lung cancer (SCLC) into subtypes based on the expression of lineage-defining transcription factors ASCL1 and NEUROD1, which together are expressed in ∼86% of SCLC. ASCL1 and NEUROD1 activate SCLC oncogene expression, drive distinct transcriptional programs, and maintain the <i>in vitro</i> growth and oncogenic properties of ASCL1 or NEUROD1-expressing SCLC. ASCL1 is also required for tumor formation in SCLC mouse models. A strategy to inhibit the activity of these oncogenic drivers may therefore provide both a targeted therapy for the predominant SCLC subtypes and a tool to investigate the underlying lineage plasticity of established SCLC tumors. However, there are no known agents that inhibit ASCL1 or NEUROD1 function. In this study, we identify a novel strategy to pharmacologically target ASCL1 and NEUROD1 activity in SCLC by exploiting the nuclear localization required for the function of these transcription factors. Karyopherin β1 (KPNB1) was identified as a nuclear import receptor for both ASCL1 and NEUROD1 in SCLC, and inhibition of KPNB1 led to impaired ASCL1 and NEUROD1 nuclear accumulation and transcriptional activity. Pharmacologic targeting of KPNB1 preferentially disrupted the growth of ASCL1<sup>+</sup> and NEUROD1<sup>+</sup> SCLC cells <i>in vitro</i> and suppressed ASCL1<sup>+</sup> tumor growth <i>in vivo</i>, an effect mediated by a combination of impaired ASCL1 downstream target expression, cell-cycle activity, and proteostasis. These findings broaden the support for targeting nuclear transport as an anticancer therapeutic strategy and have implications for targeting lineage-transcription factors in tumors beyond SCLC.</p>Significance:<p>The identification of KPNB1 as a nuclear import receptor for lineage-defining transcription factors in SCLC reveals a viable therapeutic strategy for cancer treatment.</p></div>

Duke Scholars

Trudy G Oliver
Author Trudy G Oliver Pharmacology & Cancer Biology

DOI

10.1158/0008-5472.c.6513996

Publication Date

March 31, 2023
 

Citation

APA
Chicago
ICMJE
MLA
NLM
Kelenis, D. P., Rodarte, K. E., Kollipara, R. K., Pozo, K., Choudhuri, S. P., Spainhower, K. B., … Johnson, J. E. (2023). Data from Inhibition of Karyopherin β1-Mediated Nuclear Import Disrupts Oncogenic Lineage-Defining Transcription Factor Activity in Small Cell Lung Cancer. https://doi.org/10.1158/0008-5472.c.6513996
Kelenis, Demetra P., Kathia E. Rodarte, Rahul K. Kollipara, Karine Pozo, Shreoshi Pal Choudhuri, Kyle B. Spainhower, Sarah J. Wait, Victor Stastny, Trudy G. Oliver, and Jane E. Johnson. “Data from Inhibition of Karyopherin β1-Mediated Nuclear Import Disrupts Oncogenic Lineage-Defining Transcription Factor Activity in Small Cell Lung Cancer,” March 31, 2023. https://doi.org/10.1158/0008-5472.c.6513996.
Kelenis DP, Rodarte KE, Kollipara RK, Pozo K, Choudhuri SP, Spainhower KB, Wait SJ, Stastny V, Oliver TG, Johnson JE. Data from Inhibition of Karyopherin β1-Mediated Nuclear Import Disrupts Oncogenic Lineage-Defining Transcription Factor Activity in Small Cell Lung Cancer. 2023.

DOI

10.1158/0008-5472.c.6513996

Publication Date

March 31, 2023