Network-based systems pharmacology reveals heterogeneity in LCK and BCL2 signaling and therapeutic sensitivity of T-cell acute lymphoblastic leukemia

被引：106

作者：

Gocho, Yoshihiro ^{[1
]}

Liu, Jingjing ^{[2
]}

Hu, Jianzhong ^{[1
]}

Yang, Wentao ^{[1
]}

Dharia, Neekesh V. ^{[3
,4
,5
]}

Zhang, Jingliao ^{[1
]}

Shi, Hao ^{[6
]}

Du, Guoqing ^{[1
]}

John, August ^{[1
]}

Lin, Ting-Nien ^{[1
]}

Hunt, Jeremy ^{[1
]}

Huang, Xin ^{[2
]}

Ju, Bensheng ^{[2
]}

Rowland, Lauren ^{[1
]}

Shi, Lei ^{[7
]}

Maxwell, Dylan ^{[1
]}

Smart, Brandon ^{[1
]}

Crews, Kristine R. ^{[1
]}

Yang, Wenjian ^{[1
]}

Hagiwara, Kohei ^{[2
]}

Zhang, Yingchi ^{[8
,9
]}

Roberts, Kathryn ^{[10
]}

Wang, Hong ^{[11
,12
,13
]}

Jabbour, Elias ^{[14
]}

Stock, Wendy ^{[15
]}

Eisfelder, Bartholomew ^{[15
]}

Paietta, Elisabeth ^{[16
]}

Newman, Scott ^{[2
]}

Roti, Giovanni ^{[3
,4
,17
]}

Litzow, Mark ^{[18
]}

Easton, John ^{[2
]}

Zhang, Jinghui ^{[2
]}

Peng, Junmin ^{[11
,12
,13
]}

Chi, Hongbo ^{[6
]}

Pounds, Stanley ^{[7
]}

Relling, Mary V. ^{[1
]}

Inaba, Hiroto ^{[19
]}

Zhu, Xiaofan ^{[8
,9
]}

Kornblau, Steven ^{[14
]}

Pui, Ching-Hon ^{[19
]}

Konopleva, Marina ^{[14
]}

Teachey, David ^{[20
]}

Mullighan, Charles G. ^{[10
]}

Stegmaier, Kimberly ^{[3
,4
,5
]}

Evans, William E. ^{[1
]}

Yu, Jiyang ^{[2
]}

Yang, Jun J. ^{[1
,19
]}

机构：

[1] St Jude Childrens Res Hosp, Dept Pharmaceut Sci, 332 N Lauderdale St, Memphis, TN 38105 USA

[2] St Jude Childrens Res Hosp, Dept Computat Biol, 332 N Lauderdale St, Memphis, TN 38105 USA

[3] Dana Farber Canc Inst, Dept Pediat Oncol, Boston, MA 02115 USA

[4] Harvard Med Sch, Boston Childrens Hosp, Boston, MA 02115 USA

[5] Broad Inst MIT & Harvard, Cambridge, MD USA

[6] St Jude Childrens Res Hosp, Dept Immunol, 332 N Lauderdale St, Memphis, TN 38105 USA

[7] St Jude Childrens Res Hosp, Dept Biostat, 332 N Lauderdale St, Memphis, TN 38105 USA

[8] Chinese Acad Med Sci & Peking Union Med Coll, Inst Hematol, Natl Clin Res Ctr Blood Dis, State Key Lab Expt Hematol, Tianjin, Peoples R China

[9] Chinese Acad Med Sci & Peking Union Med Coll, Blood Dis Hosp, Natl Clin Res Ctr Blood Dis, State Key Lab Expt Hematol, Tianjin, Peoples R China

[10] St Jude Childrens Res Hosp, Dept Pathol, 332 N Lauderdale St, Memphis, TN 38105 USA

[11] St Jude Childrens Res Hosp, Dept Biol Struct, 332 N Lauderdale St, Memphis, TN 38105 USA

[12] St Jude Childrens Res Hosp, Dept Dev Neurobiol, 332 N Lauderdale St, Memphis, TN 38105 USA

[13] St Jude Childrens Res Hosp, Ctr Prote & Metabol, 332 N Lauderdale St, Memphis, TN 38105 USA

[14] Univ Texas MD Anderson Canc Ctr, Dept Leukemia, Houston, TX 77030 USA

[15] Univ Chicago, Med Ctr, Chicago, IL 60637 USA

[16] Montefiore Med Ctr, 111 E 210th St, Bronx, NY 10467 USA

[17] Univ Parma, Dept Med & Surg, Parma, Italy

[18] Mayo Clin, Div Hematol, Rochester, MN USA

[19] St Jude Childrens Res Hosp, Dept Oncol, 332 N Lauderdale St, Memphis, TN 38105 USA

[20] Univ Penn, Dept Pediat, Philadelphia, PA 19104 USA

来源：

NATURE CANCER | 2021年 / 2卷 / 03期

基金：

美国国家卫生研究院;

关键词：

COPY-NUMBER ANALYSIS; STRUCTURAL-VARIATION; OPEN-LABEL; CANCER; DASATINIB; EXPRESSION; KINASE; PHOSPHORYLATION; RESISTANCE; INHIBITION;

D O I：

10.1038/s43018-020-00167-4

中图分类号：

R73 [肿瘤学];

学科分类号：

100214 ;

摘要：

Yang and colleagues perform a network system-pharmacology approach and clinical data integration, and identify LCK and BCL2 signaling as the molecular determinants of dasatinib response in pediatric and adult patients with T-ALL. T-cell acute lymphoblastic leukemia (T-ALL) is an aggressive hematological malignancy and new therapeutics are much needed. Profiling patient leukemia drug sensitivities ex vivo, we discovered that 44.4% of childhood and 16.7% of adult T-ALL cases exquisitely respond to dasatinib. Applying network-based systems pharmacology analyses to examine signal circuitry, we identified preTCR-LCK activation as the driver of dasatinib sensitivity and T-ALL-specific LCK dependency was confirmed in genome-wide CRISPR-Cas9 screens. Dasatinib-sensitive T-ALL exhibited high BCL-XL activity, low BCL2 activity and venetoclax resistance. Discordant sensitivity of T-ALL to dasatinib and venetoclax is strongly correlated with T-cell differentiation, particularly with the dynamic shift in LCK versus BCL2 activation. Finally, single-cell analysis identified leukemia heterogeneity in LCK and BCL2 signaling and T-cell maturation stage, consistent with dasatinib response. In conclusion, our results indicate that developmental arrest in T-ALL drives differential activation of preTCR-LCK and BCL2 signaling in this leukemia, providing unique opportunities for targeted therapy.

引用

页码：284 / +

页数：36

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