Large-scale dependency and drug screens to characterize the therapeutic vulnerabilities of multiple myeloma with 1q.

Sklavenitis-Pistofidis, Romanos; Lightbody, Elizabeth D.; Reidy, Mairead; Tsuji, Junko; Alberge, Jean-Baptiste; Aranha, Michelle P.; Heilpern-Mallory, Daniel; Roweth, Harvey G.; Huynh, Daisy; Chong, Stephen J. F.; Chung, Anna Y; Zhang, Jeremy; Hackett, Liam; Haradhvala, Nicholas J.; Wu, Ting; Su, Nang K.; Berrios, Brianna; Belkin, Saveliy; Dutta, Ankit K.; Knudson, Ryan A.; Brandt, Carolyn; Greipp, Patricia T.; Davids, Matthew S.; Papaioannou, Maria; Getz, Gad; Ghobrial, Irene M.; Manier, Salomon

Download

[thumbnail of 2025_Sklavenitis-Pistofidis_Large scale dependency and drug screens to characterize the therapeutic vulnerabilities of multiple myeloma with 1q.pdf]

Text
- Accepted Version
· Restricted to Repository staff only
· The Copyright of this document has not been checked yet. This may affect its availability.

Advice

Please see our End User Agreement.

It is advisable to refer to the publisher's version if you intend to cite from this work. See Guidance on citing.

Tools

Lists

Sklavenitis-Pistofidis, R., Lightbody, E. D., Reidy, M., Tsuji, J., Alberge, J.-B., Aranha, M. P., Heilpern-Mallory, D., Roweth, H. G. ORCID: https://orcid.org/0000-0002-1100-8409, Huynh, D., Chong, S. J. F., Chung, A. Y., Zhang, J., Hackett, L., Haradhvala, N. J., Wu, T., Su, N. K., Berrios, B., Belkin, S., Dutta, A. K., Knudson, R. A., Brandt, C., Greipp, P. T., Davids, M. S., Papaioannou, M., Getz, G., Ghobrial, I. M. and Manier, S. (2025) Large-scale dependency and drug screens to characterize the therapeutic vulnerabilities of multiple myeloma with 1q. Blood, 146 (1). pp. 89-103. ISSN 1528-0020 doi: 10.1182/blood.2024025102

Abstract/Summary

The development of targeted therapy for patients with multiple myeloma (MM) is hampered by the low frequency of actionable genetic abnormalities. Gain or amplification of chromosome 1q (1q+) is the most frequent arm-level copy number gain in patients with MM and is associated with higher risk of progression and death despite recent therapeutic advances. Thus, developing targeted therapy for patients with MM with 1q+ stands to benefit a large portion of patients in need of more effective management. Here, we used large-scale dependency screens and drug screens to systematically characterize the therapeutic vulnerabilities of MM with 1q+ and displayed increased sensitivity to myeloid cell leukemia-1 (MCL1) and phosphatidyl inositol 3-kinase (PI3K) inhibitors. Using single-cell RNA sequencing, we compared subclones with and without 1q+ within the same patient tumors and demonstrated that 1q+ is associated with higher levels of MCL1 and the PI3K pathway. Furthermore, by isolating isogenic clones with different copy number profiles for part of the chromosome 1q arm, we observed increased sensitivity to MCL1 and PI3K inhibitors with arm-level gain. Lastly, we demonstrated synergy between MCL1 and PI3K inhibitors and dissected their mechanism of action in MM with 1q+, uncovering a cytostatic effect. In conclusion, this study highlights that MM with 1q+ may present enhanced sensitivity to MCL1 and PI3K inhibitors, enabling their use at lower doses without sacrificing efficacy, and may thus accelerate the development of targeted therapy for patients with MM and 1q+.

Altmetric Badge

Dimensions Badge

Item Type	Article
URI	https://centaur.reading.ac.uk/id/eprint/128111
Identification Number/DOI	10.1182/blood.2024025102
Refereed	Yes
Divisions	No Reading authors. Back catalogue items Life Sciences > School of Biological Sciences > Biomedical Sciences
Publisher	American Society of Hematology
Download/View statistics	View download statistics for this item

Deposit Details

CORE (COnnecting REpositories)

University Staff: Request a correction | Centaur Editors: Update this record

Date Deposited:	28 Jan 2026 11:59	Date item deposited into CentAUR
Last Modified:	28 Jan 2026 12:00	Date item last modified