Your search keyword '"Koshi Akahane"' showing total 106 results

1. Involvement of BCR::ABL1 in laminin adhesion of Philadelphia chromosome‐positive acute lymphoblastic leukemia through upregulation of integrin α6

Author

Kazuya Takahashi, Thao Thu Thi Nguyen, Atsushi Watanabe, Hiroki Sato, Kinuko Saito, Minori Tamai, Daisuke Harama, Shin Kasai, Koshi Akahane, Kumiko Goi, Keiko Kagami, Masako Abe, Chiaki Komatsu, Yasuhiro Maeda, Kanji Sugita, and Takeshi Inukai

Subjects

ALL, CD49f, imatinib, integrin α6, Philadelphia chromosome, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Background Adhesion of cancer cells to extracellular matrix laminin through the integrin superfamily reportedly induces drug resistance. Heterodimers of integrin α6 (CD49f) with integrin β1 (CD29) or β4 (CD104) are major functional receptors for laminin. Higher CD49f expression is reportedly associated with a poorer response to induction therapy in childhood B‐cell precursor acute lymphoblastic leukemia (BCP‐ALL). Moreover, a xenograft mouse model transplanted with primary BCP‐ALL cells revealed that neutralized antibody against CD49f improved survival after chemotherapy. Aims Considering the poor outcomes in Philadelphia chromosome (Ph)‐positive ALL treated with conventional chemotherapy without tyrosine kinase inhibitors, we sought to investigate an involvement of the laminin adhesion. Methods and results Ph‐positive ALL cell lines expressed the highest levels of CD49f among the BCP‐ALL cell lines with representative translocations, while CD29 and CD104 were ubiquitously expressed in BCP‐ALL cell lines. The association of Ph‐positive ALL with high levels of CD49f gene expression was also confirmed in two databases of childhood ALL cohorts. Ph‐positive ALL cell lines attached to laminin and their laminin‐binding properties were disrupted by blocking antibodies against CD49f and CD29 but not CD104. The cell surface expression of CD49f, but not CD29 and CD104, was downregulated by imatinib treatment in Ph‐positive ALL cell lines, but not in their T315I‐acquired sublines. Consistently, the laminin‐binding properties were disrupted by the imatinib pre‐treatment in the Ph‐positive ALL cell line, but not in its T315I‐acquired subline. Conclusion BCR::ABL1 plays an essential role in the laminin adhesion of Ph‐positive ALL cells through upregulation of CD49f.

Published

2024

2. Targeting Poly(ADP)ribose polymerase in BCR/ABL1-positive cells

Author

Haruka Hiroki, Yuko Ishii, Jinhua Piao, Yui Namikawa, Mitsuko Masutani, Hiroaki Honda, Koshi Akahane, Takeshi Inukai, Tomohiro Morio, and Masatoshi Takagi

Subjects

Medicine, Science

Abstract

Abstract BCR/ABL1 causes dysregulated cell proliferation and is responsible for chronic myelogenous leukemia (CML) and Philadelphia chromosome-positive acute lymphoblastic leukemia (Ph1-ALL). In addition to the deregulatory effects of its kinase activity on cell proliferation, BCR/ABL1 induces genomic instability by downregulating BRCA1. PARP inhibitors (PARPi) effectively induce cell death in BRCA-defective cells. Therefore, PARPi are expected to inhibit growth of CML and Ph1-ALL cells showing downregulated expression of BRCA1. Here, we show that PARPi effectively induced cell death in BCR/ABL1 positive cells and suppressed colony forming activity. Prevention of BCR/ABL1-mediated leukemogenesis by PARP inhibition was tested in two in vivo models: wild-type mice that had undergone hematopoietic cell transplantation with BCR/ABL1-transduced cells, and a genetic model constructed by crossing Parp1 knockout mice with BCR/ABL1 transgenic mice. The results showed that a PARPi, olaparib, attenuates BCR/ABL1-mediated leukemogenesis. One possible mechanism underlying PARPi-dependent inhibition of leukemogenesis is increased interferon signaling via activation of the cGAS/STING pathway. This is compatible with the use of interferon as a first-line therapy for CML. Because tyrosine kinase inhibitor (TKI) monotherapy does not completely eradicate leukemic cells in all patients, combined use of PARPi and a TKI is an attractive option that may eradicate CML stem cells.

Published

2023

3. Combination of tyrosine kinase inhibitors and the MCL1 inhibitor S63845 exerts synergistic antitumorigenic effects on CML cells

Author

Alena Malyukova, Dorina Ujvari, Elham Yektaei-Karin, Ana Zovko, Harsha S. Madapura, Marton Keszei, Noemi Nagy, Kourosh Lotfi, Niclas Björn, Jonas Wallvik, Minori Tamai, Thao T. T. Nguyen, Koshi Akahane, Takeshi Inukai, Leif Stenke, and Daniel Salamon

Subjects

Cytology, QH573-671

Abstract

Abstract Tyrosine kinase inhibitor (TKI) treatment has dramatically improved the survival of chronic myeloid leukemia (CML) patients, but measurable residual disease typically persists. To more effectively eradicate leukemia cells, simultaneous targeting of BCR-ABL1 and additional CML-related survival proteins has been proposed. Notably, several highly specific myeloid cell leukemia 1 (MCL1) inhibitors have recently entered clinical trials for various hematologic malignancies, although not for CML, reflecting the insensitivity of CML cell lines to single MCL1 inhibition. Here, we show that combining TKI (imatinib, nilotinib, dasatinib, or asciminib) treatment with the small-molecule MCL1 inhibitor S63845 exerted strong synergistic antiviability and proapoptotic effects on CML lines and CD34+ stem/progenitor cells isolated from untreated CML patients in chronic phase. Using wild-type BCR-ABL1-harboring CML lines and their T315I-mutated sublines (generated by CRISPR/Cas9-mediated homologous recombination), we prove that the synergistic proapoptotic effect of the drug combination depended on TKI-mediated BCR-ABL1 inhibition, but not on TKI-related off-target mechanisms. Moreover, we demonstrate that colony formation of CML but not normal hematopoietic stem/progenitor cells became markedly reduced upon combination treatment compared to imatinib monotherapy. Our results suggest that dual targeting of MCL1 and BCR-ABL1 activity may efficiently eradicate residual CML cells without affecting normal hematopoietic stem/progenitors.

Published

2021

4. IMiDs uniquely synergize with TKIs to upregulate apoptosis of Philadelphia chromosome-positive acute lymphoblastic leukemia cells expressing a dominant-negative IKZF1 isoform

Author

Daisuke Harama, Takashi Yahata, Keiko Kagami, Masako Abe, Norie Ando, Shin Kasai, Minori Tamai, Koshi Akahane, Takeshi Inukai, Nobutaka Kiyokawa, Abd Aziz Ibrahim, Kiyoshi Ando, and Kanji Sugita

Subjects

Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282, Cytology, QH573-671

Abstract

Abstract The long-term prognosis of Philadelphia chromosome-positive acute lymphoblastic leukemia (Ph + ALL) is still unsatisfactory even after the emergence of tyrosine kinase inhibitors (TKIs) against chimeric BCR-ABL, and this is associated with the high incidence of genetic alterations of Ikaros family zinc finger 1 (IKZF1), most frequently the hemi-allelic loss of exons 4–7 expressing a dominant-negative isoform Ik6. We found that lenalidomide (LEN), a representative of immunomodulatory drugs (IMiDs), which have been long used for the treatment of multiple myeloma, specifically induced accumulation of Ik6 with the disappearance of functional isoforms within 24 h (i.e., abrupt and complete shut-down of the IKZF1 activity) in Ik6-positive Ph+ALL cells in a neddylation-dependent manner. The functional IKZF3 isoforms expression was also abruptly and markedly downregulated. The LEN treatment specifically suppressed proliferation of Ik6-positive-Ph+ALL cells by inducing cell cycle arrest via downregulation of cyclins D3 and E and CDK2, and of importance, markedly upregulated their apoptosis in synergy with the TKI imatinib (IM). Apoptosis of IM-resistant Ph+ALL cells with T315I mutation of BCR-ABL was also upregulated by LEN in the presence of the newly developed TKI ponatinib. Analyses of flow cytometry, western blot, and oligonucleotide array revealed that apoptosis was caspase-/p53-dependent and associated with upregulation of pro-apoptotic Bax/Bim, enhanced dephosphorylation of BCR-ABL/Akt, and downregulation of oncogenic helicase genes HILLS, CDC6, and MCMs4 and 8. Further, the synergism of LEN with IM was clearly documented as a significant prolongation of survival in the xenograft mice model. Because this synergism was further potentiated in vitro by dexamethasone, a key drug for ALL treatment, the strategy of repositioning IMiDs for the treatment of Ik6-positive Ph+ALL patients certainly shed new light on an outpatient-based treatment option for achieving their long-term durable remission and higher QOL, particularly for those who are not tolerable to intensified therapeutic approaches.

Published

2021

5. BCL6 inhibition ameliorates resistance to ruxolitinib in CRLF2-rearranged acute lymphoblastic leukemia

Author

Shinobu Tsuzuki, Takahiko Yasuda, Hiroaki Goto, Naoko Maeda, Koshi Akahane, Takeshi Inukai, Hideyuki Yamamoto, Sivasundaram Karnan, Akinobu Ota, Toshinori Hyodo, Hiroyuki Konishi, Yoshitaka Hosokawa, Hitoshi Kiyoi, and Fumihiko Hayakawa

Subjects

Diseases of the blood and blood-forming organs, RC633-647.5

Abstract

Philadelphia chromosome-like acute lymphoblastic leukemia (Ph-like ALL) is an intractable disease and most cases harbor genetic alterations that activate JAK or ABL signaling. The commonest subtype of Ph-like ALL exhibits a CRLF2 gene rearrangement that brings about JAK1/2-STAT5 pathway activation. However, JAK1/2 inhibition alone is insufficient as a treatment, so combinatorial therapies targeting multiple signals are needed. To better understand the mechanisms underlying the insufficient efficacy of JAK inhibition, we explored gene expression changes upon treatment with a JAK1/2 inhibitor (ruxolitinib) and found that elevated BCL6 expression was one such mechanism. Upregulated BCL6 suppressed the expression of TP53 along with its downstream cell cycle inhibitor p21 (CDKN2A) and pro-apoptotic molecules, such as FAS, TNFRSF10B, BID, BAX, BAK, PUMA, and NOXA, conferring cells some degree of resistance to therapy. BCL6 inhibition (with FX1) alone was able to upregulate TP53 and restore the TP53 expression that ruxolitinib had diminished. In addition, ruxolitinib and FX1 concertedly downregulated MYC. As a result, FX1 treatment alone had growth-inhibitory and apoptosis- sensitizing effects, but the combination of ruxolitinib and FX1 more potently inhibited leukemia cell growth, enhanced apoptosis sensitivity, and prolonged the survival of xenografted mice. These findings provide one mechanism for the insufficiency of JAK inhibition for the treatment of CRLF2-rearranged ALL and indicate BCL6 inhibition as a potentially helpful adjunctive therapy combined with JAK inhibition.

Published

2022

6. Association of relapse-linked ARID5B single nucleotide polymorphisms with drug resistance in B-cell precursor acute lymphoblastic leukemia cell lines

Author

Minori Tamai, Meixian Huang, Keiko Kagami, Masako Abe, Shinpei Somazu, Tamao Shinohara, Daisuke Harama, Atsushi Watanabe, Koshi Akahane, Kumiko Goi, Kanji Sugita, Hiroaki Goto, Masayoshi Minegishi, Shotaro Iwamoto, and Takeshi Inukai

Subjects

ARID5B, B-cell precursor acute lymphoblastic leukemia, Drug sensitivities, Single nucleotide polymorphism, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282, Cytology, QH573-671

Abstract

Abstract Background The genetic variants of the ARID5B gene have recently been reported to be associated with disease susceptibility and treatment outcome in childhood acute lymphoblastic leukemia (ALL). However, few studies have explored the association of ARID5B with sensitivities to chemotherapeutic agents. Methods We genotyped susceptibility-linked rs7923074 and rs10821936 as well as relapse-linked rs4948488, rs2893881, and rs6479778 of ARDI5B by direct sequencing of polymerase chain reaction (PCR) products in 72 B-cell precursor-ALL (BCP-ALL) cell lines established from Japanese patients. We also quantified their ARID5B expression levels by real-time reverse transcription PCR, and determined their 50% inhibitory concentration (IC50) values by alamarBlue assays in nine representative chemotherapeutic agents used for ALL treatment. Results No significant associations were observed in genotypes of the susceptibility-linked single nucleotide polymorphisms (SNPs) and the relapsed-linked SNPs with ARID5B gene expression levels. Of note, IC50 values of vincristine (VCR) (median IC50: 39.6 ng/ml) in 12 cell lines with homozygous genotype of risk allele (C) in the relapse-linked rs4948488 were significantly higher (p = 0.031 in Mann–Whitney U test) than those (1.04 ng/ml) in 60 cell lines with heterozygous or homozygous genotypes of the non-risk allele (T). Furthermore, the IC50 values of mafosfamide [Maf; active metabolite of cyclophosphamide (CY)] and cytarabine (AraC) tended to be associated with the genotype of rs4948488. Similar associations were observed in genotypes of the relapse-linked rs2893881 and rs6479778, but not in those of the susceptibility-linked rs7923074 and rs10821936. In addition, the IC50 values of methotrexate (MTX) were significantly higher (p = 0.023) in 36 cell lines with lower ARID5B gene expression (median IC50: 37.1 ng/ml) than those in the other 36 cell lines with higher expression (16.9 ng/ml). Conclusion These observations in 72 BCP-ALL cell lines suggested that the risk allele of the relapse-linked SNPs of ARID5B may be involved in a higher relapse rate because of resistance to chemotherapeutic agents such as VCR, CY, and AraC. In addition, lower ARID5B gene expression may be associated with MTX resistance.

Published

2020

7. ASCL1 is a MYCN- and LMO1-dependent member of the adrenergic neuroblastoma core regulatory circuitry

Author

Lu Wang, Tze King Tan, Adam D. Durbin, Mark W. Zimmerman, Brian J. Abraham, Shi Hao Tan, Phuong Cao Thi Ngoc, Nina Weichert-Leahey, Koshi Akahane, Lee N. Lawton, Jo Lynne Rokita, John M. Maris, Richard A. Young, A. Thomas Look, and Takaomi Sanda

Subjects

Science

Abstract

Polymorphisms in LMO1 are associated with increased susceptibility to develop neuroblastoma. Here, the authors show that LMO1 directly induces the transcription factor ASCL1, which regulates the differentiation of neurons, demonstrating that ASCL1 is part of the adrenergic neuroblastoma core regulatory circuit.

Published

2019

8. Resistance of t(17;19)‐acute lymphoblastic leukemia cell lines to multiagents in induction therapy

Author

Atsushi Watanabe, Takeshi Inukai, Keiko Kagami, Masako Abe, Masatoshi Takagi, Takashi Fukushima, Hiroko Fukushima, Toru Nanmoku, Kiminori Terui, Tatsuya Ito, Tsutomu Toki, Etsuro Ito, Junya Fujimura, Hiroaki Goto, Mikiya Endo, Thomas Look, Mark Kamps, Masayoshi Minegishi, Junko Takita, Toshiya Inaba, Hiroyuki Takahashi, Akira Ohara, Daisuke Harama, Tamao Shinohara, Shinpei Somazu, Hiroko Oshiro, Koshi Akahane, Kumiko Goi, and Kanji Sugita

Subjects

chemotherapy, hematalogical cancer, leukemia, pediatric cancer, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract t(17;19)(q21‐q22;p13), responsible for TCF3‐HLF fusion, is a rare translocation in childhood B‐cell precursor acute lymphoblastic leukemia(BCP‐ALL). t(1;19)(q23;p13), producing TCF3‐PBX1 fusion, is a common translocation in childhood BCP‐ALL. Prognosis of t(17;19)‐ALL is extremely poor, while that of t(1;19)‐ALL has recently improved dramatically in intensified chemotherapy. In this study, TCF3‐HLF mRNA was detectable at a high level during induction therapy in a newly diagnosed t(17;19)‐ALL case, while TCF3‐PBX1 mRNA was undetectable at the end of induction therapy in most newly diagnosed t(1;19)‐ALL cases. Using 4 t(17;19)‐ALL and 16 t(1;19)‐ALL cell lines, drug response profiling was analyzed. t(17;19)‐ALL cell lines were found to be significantly more resistant to vincristine (VCR), daunorubicin (DNR), and prednisolone (Pred) than t(1;19)‐ALL cell lines. Sensitivities to three (Pred, VCR, and l‐asparaginase [l‐Asp]), four (Pred, VCR, l‐Asp, and DNR) and five (Pred, VCR, l‐Asp, DNR, and cyclophosphamide) agents, widely used in induction therapy, were significantly poorer for t(17;19)‐ALL cell lines than for t(1;19)‐ALL cell lines. Consistent with poor responses to VCR and DNR, gene and protein expression levels of P‐glycoprotein (P‐gp) were higher in t(17;19)‐ALL cell lines than in t(1;19)‐ALL cell lines. Inhibitors for P‐gp sensitized P‐gp‐positive t(17;19)‐ALL cell lines to VCR and DNR. Knockout of P‐gp by CRISPRCas9 overcame resistance to VCR and DNR in the P‐gp‐positive t(17;19)‐ALL cell line. A combination of cyclosporine A with DNR prolonged survival of NSG mice inoculated with P‐gp‐positive t(17;19)‐ALL cell line. These findings indicate involvement of P‐gp in resistance to VCR and DNR in Pgp positive t(17;19)‐ALL cell lines. In all four t(17;19)‐ALL cell lines, RAS pathway mutation was detected. Furthermore, among 16 t(1;19)‐ALL cell lines, multiagent resistance was usually observed in the cell lines with RAS pathway mutation in comparison to those without it, suggesting at least a partial involvement of RAS pathway mutation in multiagent resistance of t(17;19)‐ALL.

Published

2019

9. Clofarabine exerts antileukemic activity against cytarabine‐resistant B‐cell precursor acute lymphoblastic leukemia with low deoxycytidine kinase expression

Author

Meixian Huang, Takeshi Inukai, Kunio Miyake, Yoichi Tanaka, Keiko Kagami, Masako Abe, Hiroaki Goto, Masayoshi Minegishi, Shotaro Iwamoto, Eiji Sugihara, Atsushi Watanabe, Shinpei Somazu, Tamao Shinohara, Hiroko Oshiro, Koshi Akahane, Kumiko Goi, and Kanji Sugita

Subjects

Acute lymphoblastic leukemia, clofarabine, cytosine arabinoside, deoxycytidine kinase, drug resistance, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Cytosine arabinoside (Ara‐C) is one of the key drugs for the treatment of acute myeloid leukemia. It is also used for consolidation therapy of acute lymphoblastic leukemia (ALL). Ara‐C is a deoxyadenosine analog and is phosphorylated to form cytosine arabinoside triphosphate (Ara‐CTP) as an active form. In the first step of the metabolic pathway, Ara‐C is phosphorylated to Ara‐CMP by deoxycytidine kinase (DCK). However, the current cumulative evidence in the association of the Ara‐C sensitivity in ALL appears inconclusive. We analyzed various cell lines for the possible involvement of DCK in the sensitivities of B‐cell precursor ALL (BCP‐ALL) to Ara‐C. Higher DCK expression was associated with higher Ara‐C sensitivity. DCK knockout by genome editing with a CRISPR‐Cas9 system in an Ara‐C‐sensitive‐ALL cell line induced marked resistance to Ara‐C, but not to vincristine and daunorubicin, indicating the involvement of DCK expression in the Ara‐C sensitivity of BCP‐ALL. DCK gene silencing due to the hypermethylation of a CpG island and reduced DCK activity due to a nonsynonymous variant allele were not associated with Ara‐C sensitivity. Clofarabine is a second‐generation deoxyadenosine analog rationally synthesized to improve stability and reduce toxicity. The IC50 of clofarabine in 79 BCP‐ALL cell lines was approximately 20 times lower than that of Ara‐C. In contrast to Ara‐C, although the knockout of DCK induced marked resistance to clofarabine, sensitivity to clofarabine was only marginally associated with DCK gene expression level, suggesting a possible efficacy of clofarabine for BCP‐ALL that shows relative Ara‐C resistance due to low DCK expression.

Published

2018

10. Anti-leukemic activity of bortezomib and carfilzomib on B-cell precursor ALL cell lines.

Author

Kazuya Takahashi, Takeshi Inukai, Toshihiko Imamura, Mio Yano, Chihiro Tomoyasu, David M Lucas, Atsushi Nemoto, Hiroki Sato, Meixian Huang, Masako Abe, Keiko Kagami, Tamao Shinohara, Atsushi Watanabe, Shinpei Somazu, Hiroko Oshiro, Koshi Akahane, Kumiko Goi, Jiro Kikuchi, Yusuke Furukawa, Hiroaki Goto, Masayoshi Minegishi, Shotaro Iwamoto, and Kanji Sugita

Subjects

Medicine, Science

Abstract

Prognosis of childhood acute lymphoblastic leukemia (ALL) has been dramatically improved. However, prognosis of the cases refractory to primary therapy is still poor. Recent phase 2 study on the efficacy of combination chemotherapy with bortezomib (BTZ), a proteasome inhibitor, for refractory childhood ALL demonstrated favorable clinical outcomes. However, septic death was observed in over 10% of patients, indicating the necessity of biomarkers that could predict BTZ sensitivity. We investigated in vitro BTZ sensitivity in a large panel of ALL cell lines that acted as a model system for refractory ALL, and found that Philadelphia chromosome-positive (Ph+) ALL, IKZF1 deletion, and biallelic loss of CDKN2A were associated with favorable response. Even in Ph-negative ALL cell lines, IKZF1 deletion and bilallelic loss of CDKN2A were independently associated with higher BTZ sensitivity. BTZ showed only marginal cross-resistance to four representative chemotherapeutic agents (vincristine, dexamethasone, l-asparaginase, and daunorubicin) in B-cell precursor-ALL cell lines. To improve the efficacy and safety of proteasome inhibitor combination chemotherapy, we also analyzed the anti-leukemic activity of carfilzomib (CFZ), a second-generation proteasome inhibitor, as a substitute for BTZ. CFZ showed significantly higher activity than BTZ in the majority of ALL cell lines except for the P-glycoprotein-positive t(17;19) ALL cell lines, and IKZF1 deletion was also associated with a favorable response to CFZ treatment. P-glycoprotein inhibitors effectively restored the sensitivity to CFZ, but not BTZ, in P-glycoprotein-positive t(17;19) ALL cell lines. P-glycoprotein overexpressing ALL cell line showed a CFZ-specific resistance, while knockout of P-glycoprotein by genome editing with a CRISPR/Cas9 system sensitized P-glycoprotein-positive t(17;19) ALL cell line to CFZ. These observations suggested that IKZF1 deletion could be a useful biomarker to predict good sensitivity to CFZ and BTZ, and that CFZ combination chemotherapy may be a new therapeutic option with higher anti-leukemic activity for refractory ALL that contain P-glycoprotein-negative leukemia cells.

Published

2017

11. Synergy between loss of NF1 and overexpression of MYCN in neuroblastoma is mediated by the GAP-related domain

Author

Shuning He, Marc R Mansour, Mark W Zimmerman, Dong Hyuk Ki, Hillary M Layden, Koshi Akahane, Evisa Gjini, Eric D de Groh, Antonio R Perez-Atayde, Shizhen Zhu, Jonathan A Epstein, and A Thomas Look

Subjects

nf1, neuroblastoma, zebrafish, peripheral sympathetic nervous system, Medicine, Science, Biology (General), QH301-705.5

Abstract

Earlier reports showed that hyperplasia of sympathoadrenal cell precursors during embryogenesis in Nf1-deficient mice is independent of Nf1’s role in down-modulating RAS-MAPK signaling. We demonstrate in zebrafish that nf1 loss leads to aberrant activation of RAS signaling in MYCN-induced neuroblastomas that arise in these precursors, and that the GTPase-activating protein (GAP)-related domain (GRD) is sufficient to suppress the acceleration of neuroblastoma in nf1-deficient fish, but not the hypertrophy of sympathoadrenal cells in nf1 mutant embryos. Thus, even though neuroblastoma is a classical “developmental tumor”, NF1 relies on a very different mechanism to suppress malignant transformation than it does to modulate normal neural crest cell growth. We also show marked synergy in tumor cell killing between MEK inhibitors (trametinib) and retinoids (isotretinoin) in primary nf1a-/- zebrafish neuroblastomas. Thus, our model system has considerable translational potential for investigating new strategies to improve the treatment of very high-risk neuroblastomas with aberrant RAS-MAPK activation.

Published

2016

12. Synergistic effect of combined PI3 kinase inhibitor and PARP inhibitor treatment on BCR/ABL1-positive acute lymphoblastic leukemia cells

Author

Haruka Hiroki, Koshi Akahane, Takeshi Inukai, Tomohiro Morio, and Masatoshi Takagi

Subjects

Hematology

Abstract

Poly (ADP-ribose) polymerase (PARP) inhibitors (PARPi) function by inhibiting base excision repair and inducing synthetic lethality in homologous recombination repair-deficient cells, such as BRCA1/2-mutated cancer cells. The BCR/ABL1 fusion protein causes dysregulated cell proliferation and is responsible for chronic myelogenous leukemia and Philadelphia chromosome-positive acute lymphoblastic leukemia (Ph

Published

2022

13. The orally bioavailable GSPT1/2 degrader SJ6986 exhibits in vivo efficacy in acute lymphoblastic leukemia

Author

Yunchao Chang, Fatemeh Keramatnia, Pankaj S Ghate, Gisele Nishiguchi, Qingsong Gao, Ilaria Iacobucci, Lei Yang, Divyabharathi Chepyala, Ashutosh Mishra, Anthony Andrew High, Hiroaki Goto, Koshi Akahane, Junmin Peng, Jun J. Yang, Marcus Fischer, Zoran Rankovic, and Charles G. Mullighan

Subjects

Immunology, Cell Biology, Hematology, Biochemistry

Abstract

Advancing cure rates for high-risk acute lymphoblastic leukemia (ALL) has been limited by the lack of agents that effectively kill leukemic cells sparing normal hematopoietic tissue. Molecular glues direct the cellular ubiquitin ligase cellular machinery to target neosubstrates for protein degradation. We developed a novel Cereblon modulator, SJ6986 that exhibited potent and selective degradation of GSPT1 and GSPT2, and cytotoxic activity against childhood cancer cell lines. Here we report in vitro and in vivo testing of the activity of this agent in a panel of ALL cell lines and xenografts. SJ6986 exhibited similar cytotoxicity to the previously described GSPT1 degrader CC-90009 in a panel of leukemia cell lines in vitro, resulting in apoptosis and perturbation of cell cycle progression. SJ6986 was more effective than CC-90009 in suppressing leukemic cell growth in vivo, partly attributable to favorable pharmacokinetic properties, and did not significantly impair differentiation of human CD34+ cells ex vivo. Genome wide CRISPR/Cas9 screening of ALL cell lines treated with SJ6986 confirmed components of the CRL4CRBN complex, associated adaptors, regulators and effectors were integral in mediating the action of SJ6986. SJ6986 is a potent, selective, orally bioavailable GSPT1/2 degrader that shows broad antileukemic activity and has potential for clinical development.

Published

2023

14. FGFR1 tyrosine kinase domain duplication in infantile soft tissue spindle cell tumor

Author

Koshi Akahane, Shin Kasai, Atsushi Watanabe, Keiko Kagami, Chiaki Komatsu, Minori Tamai, Kumiko Goi, Naoki Oishi, Akihiko Yoshida, Chitose Ogawa, Eisuke Kobayashi, and Takeshi Inukai

Subjects

Oncology, Pediatrics, Perinatology and Child Health, Hematology

Published

2023

15. Data from Targeting MEF2D-fusion Oncogenic Transcriptional Circuitries in B-cell Precursor Acute Lymphoblastic Leukemia

Author

Fumihiko Hayakawa, Hiroyuki Mano, Yoshitaka Hosokawa, Hitoshi Kiyoi, Itaru Matsumura, Yasushi Miyazaki, Yoshiyuki Takahashi, Hideki Muramatsu, Kyogo Suzuki, Akihiro Tomita, Keizo Horibe, Hirokazu Nagai, Masashi Sanada, Hiroyuki Konishi, Toshinori Hyodo, Akinobu Ota, Sivasundaram Karnan, Toshihide Ueno, Koichi Miyamura, Takanobu Morishita, Masue Imaizumi, Takeshi Inukai, Koshi Akahane, Masahito Kawazu, Shinya Kojima, Takahiko Yasuda, and Shinobu Tsuzuki

Abstract

The cellular context that integrates gene expression, signaling, and metabolism dictates the oncogenic behavior and shapes the treatment responses in distinct cancer types. Although chimeric fusion proteins involving transcription factors (TF) are hallmarks of many types of acute lymphoblastic leukemia (ALL), therapeutically targeting the fusion proteins is a challenge. In this work, we characterize the core regulatory circuitry (CRC; interconnected autoregulatory loops of TFs) of B-ALL involving MEF2D-fusions and identify MEF2D-fusion and SREBF1 TFs as crucial CRC components. By gene silencing and pharmacologic perturbation, we reveal that the CRC integrates the pre-B-cell receptor (BCR) and lipid metabolism to maintain itself and govern malignant phenotypes. Small-molecule inhibitors of pre-BCR signaling and lipid biosynthesis disrupt the CRC and silence the MEF2D fusion in cell culture and show therapeutic efficacy in xenografted mice. Therefore, pharmacologic disruption of CRC presents a potential therapeutic strategy to target fusion protein–driven leukemia.Significance:Cancer type–specific gene expression is governed by transcription factors involved in a highly interconnected autoregulatory loop called CRC. Here, we characterized fusion protein–driven CRC and identified its pharmacologic vulnerabilities, opening therapeutic avenues to indirectly target fusion-driven leukemia by disrupting its CRC.See related commentary by Sadras and Müschen, p. 18.This article is highlighted in the In This Issue feature, p. 5

Published

2023

16. Supplementary Data from Targeting MEF2D-fusion Oncogenic Transcriptional Circuitries in B-cell Precursor Acute Lymphoblastic Leukemia

Author

Fumihiko Hayakawa, Hiroyuki Mano, Yoshitaka Hosokawa, Hitoshi Kiyoi, Itaru Matsumura, Yasushi Miyazaki, Yoshiyuki Takahashi, Hideki Muramatsu, Kyogo Suzuki, Akihiro Tomita, Keizo Horibe, Hirokazu Nagai, Masashi Sanada, Hiroyuki Konishi, Toshinori Hyodo, Akinobu Ota, Sivasundaram Karnan, Toshihide Ueno, Koichi Miyamura, Takanobu Morishita, Masue Imaizumi, Takeshi Inukai, Koshi Akahane, Masahito Kawazu, Shinya Kojima, Takahiko Yasuda, and Shinobu Tsuzuki

Abstract

SupplementaryFigures

Published

2023

17. Supplementary Figure from Specific Antileukemic Activity of PD0332991, a CDK4/6 Inhibitor, against Philadelphia Chromosome–Positive Lymphoid Leukemia

Author

Takeshi Inukai, Kanji Sugita, Toshio Heike, Tatsutoshi Nakahata, Kenichiro Watanabe, Akira Niwa, Seiichi Okabe, Yuko Sato, Shinya Kimura, Keiko Kagami, Kumiko Goi, Hiroko Honna-Oshiro, Koshi Akahane, Yasuhiro Maeda, Yusuke Furukawa, Jiro Kikuchi, Itaru Kato, Satoshi Saida, and Atsushi Nemoto

Abstract

Supplementary Fig. S1-S5. Fig. S1. Anti-leukemic activity of PD0332991 against Ph+ lymphoid leukemia cell lines. Fig. S2. Effect of cytokines and PD0332991 on cell growth of Ph+ lymphoid leukemia cell lines. Fig. S3. Anti-leukemic activity of PD0332991 against a Ph+ALL cell lines with a T315I mutation of BCR-ABL in vitro. Fig. S4. Anti-leukemic activity of PD0332991 against a Ph+ ALL cell line with a T315I mutation of BCR-ABL in a xenograft model using NOG mice. Fig. S5. Expression of cell cycle regulators in Ph+ lymphoid leukemia cells.

Published

2023

18. Data from Specific Antileukemic Activity of PD0332991, a CDK4/6 Inhibitor, against Philadelphia Chromosome–Positive Lymphoid Leukemia

Author

Takeshi Inukai, Kanji Sugita, Toshio Heike, Tatsutoshi Nakahata, Kenichiro Watanabe, Akira Niwa, Seiichi Okabe, Yuko Sato, Shinya Kimura, Keiko Kagami, Kumiko Goi, Hiroko Honna-Oshiro, Koshi Akahane, Yasuhiro Maeda, Yusuke Furukawa, Jiro Kikuchi, Itaru Kato, Satoshi Saida, and Atsushi Nemoto

Abstract

S-phase progression of the cell cycle is accelerated in tumors through various genetic abnormalities, and, thus, pharmacologic inhibition of altered cell-cycle progression would be an effective strategy to control tumors. In the current study, we analyzed the antileukemic activity of three available small molecules targeting CDK4/CDK6 against lymphoid crisis of chronic myeloid leukemia (CML-LC) and Philadelphia chromosome–positive acute lymphoblastic leukemia (Ph+ ALL), and found that all three molecules showed specific activities against leukemic cell lines derived from CML-LC and Ph+ ALL. In particular, PD0332991 exhibited extremely high antileukemic activity against CML-LC and Ph+ ALL cell lines in the nanomolar range by the induction of G0–G1 arrest and partially cell death through dephosphorylation of pRb and downregulation of the genes that are involved in S-phase transition. As an underlying mechanism for favorable sensitivity to the small molecules targeting CDK4/CDK6, cell-cycle progression of Ph+ lymphoid leukemia cells was regulated by transcriptional and posttranscriptional modulation of CDK4 as well as Cyclin D2 gene expression under the control of BCR-ABL probably through the PI3K pathway. Consistently, the gene expression level of Cyclin D2 in Ph+ lymphoid leukemia cells was significantly higher than that in Ph− lymphoid leukemia cells. Of note, three Ph+ ALL cell lines having the T315I mutation also showed sensitivity to PD0332991. In a xenograft model, PD0332991, but not imatinib, suppressed dissemination of Ph+ ALL having the T315I mutation and prolonged survival, demonstrating that this reagent would be a new therapeutic modality for relapsed CML-LC and Ph+ ALL patients after treatment with tyrosine kinase inhibitors. Mol Cancer Ther; 15(1); 94–105. ©2015 AACR.

Published

2023

19. Supplementary Table from Specific Antileukemic Activity of PD0332991, a CDK4/6 Inhibitor, against Philadelphia Chromosome–Positive Lymphoid Leukemia

Author

Takeshi Inukai, Kanji Sugita, Toshio Heike, Tatsutoshi Nakahata, Kenichiro Watanabe, Akira Niwa, Seiichi Okabe, Yuko Sato, Shinya Kimura, Keiko Kagami, Kumiko Goi, Hiroko Honna-Oshiro, Koshi Akahane, Yasuhiro Maeda, Yusuke Furukawa, Jiro Kikuchi, Itaru Kato, Satoshi Saida, and Atsushi Nemoto

Abstract

Supplementary Table S1-S5. Table S1. Characteristics leukemia cell lines. Table S2. List of primary antibodies used for Western blot analysis. Table S3. List of Taqman probe for real-time RT-PCR analysis. Table S4. Sequences of siRNA. Table S5. Sensitivity to PD0332991 of B-precursor cell lines and their gene expression level of components for CDK4/6-cyclin D pathway and gene status of p16.

Published

2023

20. Data from Fms-like Tyrosine Kinase 3 Ligand Stimulation Induces MLL-Rearranged Leukemia Cells into Quiescence Resistant to Antileukemic Agents

Author

Kanji Sugita, Shinpei Nakazawa, Kenichi Harigaya, Yasuhide Hayashi, Keiko Kagami, Xiaochun Zhang, Itaru Kuroda, Hiroko Honna, Kinuko Hirose, Koshi Akahane, Kazuya Takahashi, Atsushi Nemoto, Hiroki Sato, Takeshi Inukai, Kumiko Goi, and Yoshiyuki Furuichi

Abstract

Fms-like tyrosine kinase 3 (FLT3) is highly expressed in acute lymphoblastic leukemia with the mixed-lineage leukemia (MLL) gene rearrangement refractory to chemotherapy. We examined the biological effect of FLT3-ligand (FL) on 18 B-precursor leukemic cell lines with variable karyotypic abnormalities, and found that nine of nine MLL-rearranged cell lines with wild-type FLT3, in contrast to other leukemic cell lines, are significantly inhibited in their proliferation in a dose-dependent manner by FL. This inhibition was due to induction of the G0-G1 arrest. A marked up-regulation of p27 by suppression of its protein degradation and an abrogation of constitutive signal transducers and activators of transcription 5 phosphorylation were revealed in arrested leukemia cells after FL stimulation. Importantly, FL treatment rendered not only cell lines but also primary leukemia cells with MLL rearrangement resistant to chemotherapeutic agents. MLL-rearranged leukemia cells adhering to the bone marrow stromal cell line, which expresses FL as the membrane-bound form, were induced to quiescent state resistant to chemotherapeutic agents, but their chemosensitivity was significantly restored in the presence of neutralizing anti-FL antibody. The FL/FLT3 interaction between leukemia cells and bone marrow stromal cells expressing FL at high levels should contribute, at least in part, to persistent minimal-residual disease of MLL-rearranged leukemia in bone marrow. [Cancer Res 2007;67(20):9852–61]

Published

2023

21. Supplementary Figures 1-4 from Fms-like Tyrosine Kinase 3 Ligand Stimulation Induces MLL-Rearranged Leukemia Cells into Quiescence Resistant to Antileukemic Agents

Author

Kanji Sugita, Shinpei Nakazawa, Kenichi Harigaya, Yasuhide Hayashi, Keiko Kagami, Xiaochun Zhang, Itaru Kuroda, Hiroko Honna, Kinuko Hirose, Koshi Akahane, Kazuya Takahashi, Atsushi Nemoto, Hiroki Sato, Takeshi Inukai, Kumiko Goi, and Yoshiyuki Furuichi

Abstract

Supplementary Figures 1-4 from Fms-like Tyrosine Kinase 3 Ligand Stimulation Induces MLL-Rearranged Leukemia Cells into Quiescence Resistant to Antileukemic Agents

Published

2023

22. Genome-wide CRISPR-Cas9 screen identifies rationally designed combination therapies for CRLF2-rearranged Ph-like ALL

Author

Hiroshi Imanaga, Tatsuya Terasaki, Koichi Akashi, Kensuke Sasaki, Fumihiko Nakao, Takeshi Inukai, Jumpei Nogami, Takahiro Maeda, Els Verhoeyen, Takuji Yamauchi, Koshi Akahane, Yuichiro Semba, 大賀, 正一, 新井, 文用, and 馬場, 義裕

Subjects

Ruxolitinib, Immunology, Cell, Biochemistry, Viral vector, Mice, Transduction (genetics), Cell Line, Tumor, hemic and lymphatic diseases, Antineoplastic Combined Chemotherapy Protocols, Nitriles, medicine, Animals, Humans, Philadelphia Chromosome, Receptors, Cytokine, STAT3, Protein Kinase Inhibitors, Gene Rearrangement, Trametinib, Lymphoid Neoplasia, biology, Kinase, Cell Biology, Hematology, Precursor Cell Lymphoblastic Leukemia-Lymphoma, CRKL, Pyrimidines, medicine.anatomical_structure, biology.protein, Cancer research, Pyrazoles, CRISPR-Cas Systems, Signal Transduction, medicine.drug

Abstract

Acute lymphoblastic leukemia (ALL) harboring the IgH-CRLF2 rearrangement (IgH-CRLF2-r) exhibits poor clinical outcomes and is the most common subtype of Philadelphia chromosome-like acute lymphoblastic leukemia (Ph-like ALL). While multiple chemotherapeutic regimens, including ruxolitinib monotherapy and/or its combination with chemotherapy, are being tested, their efficacy is reportedly limited. To identify molecules/pathways relevant for IgH-CRLF2-r ALL pathogenesis, we performed genome-wide CRISPR-Cas9 dropout screens in the presence or absence of ruxolitinib using 2 IgH-CRLF2-r ALL lines that differ in RAS mutational status. To do so, we employed a baboon envelope pseudotyped lentiviral vector system, which enabled, for the first time, highly efficient transduction of human B cells. While single-guide RNAs (sgRNAs) targeting CRLF2, IL7RA, or JAK1/2 significantly affected cell fitness in both lines, those targeting STAT5A, STAT5B, or STAT3 did not, suggesting that STAT signaling is largely dispensable for IgH-CRLF2-r ALL cell survival. We show that regulators of RAS signaling are critical for cell fitness and ruxolitinib sensitivity and that CRKL depletion enhances ruxolitinib sensitivity in RAS wild-type (WT) cells. Gilteritinib, a pan-tyrosine kinase inhibitor that blocks CRKL phosphorylation, effectively killed RAS WT IgH-CRLF2-r ALL cells in vitro and in vivo, either alone or combined with ruxolitinib. We further show that combining gilteritinib with trametinib, a MEK1/2 inhibitor, is an effective means to target IgH-CRLF2-r ALL cells regardless of RAS mutational status. Our study delineates molecules/pathways relevant for CRLF2-r ALL pathogenesis and could suggest rationally designed combination therapies appropriate for disease subtypes.

Published

2022

23. Association of allele-specific methylation of the ASNS gene with asparaginase sensitivity and prognosis in T-ALL

Author

Kunio Miyake, Nobutaka Kiyokawa, Koshi Akahane, Tamao Shinohara, Atsushi Watanabe, Kumiko Goi, Katsuyoshi Koh, Toshihiko Imamura, Junko Takita, Shunsuke Kimura, A. Thomas Look, Kentaro Yoshimura, Takeshi Inukai, Masayoshi Minegishi, Shin Kasai, Kanji Sugita, Keiko Kagami, Kenichiro Hata, Daisuke Harama, Tomoko Kawai, and Keizo Horibe

Subjects

Asparaginase, Asparagine synthetase, Biology, Precursor T-Cell Lymphoblastic Leukemia-Lymphoma, chemistry.chemical_compound, Cell Line, Tumor, medicine, Gene silencing, Humans, Child, Alleles, Lymphoid Neoplasia, Aspartate-Ammonia Ligase, Hematology, Methylation, DNA Methylation, medicine.disease, Prognosis, Leukemia, CpG site, chemistry, DNA methylation, Cancer research, Carbon-Nitrogen Ligases with Glutamine as Amide-N-Donor, Asparagine, Genomic imprinting

Abstract

Key Points Allele-specific methylation of the ASNS gene is associated with asparaginase sensitivity and therapeutic outcome in T-ALL.Pediatric T-ALL patients with poor prognostic SPI1 fusion exclusively exhibited ASNS hypomethylation status., Visual Abstract, Asparaginase therapy is a key component of chemotherapy for patients with T-cell acute lymphoblastic leukemia (T-ALL). Asparaginase depletes serum asparagine by deamination into aspartic acid. Normal hematopoietic cells can survive due to asparagine synthetase (ASNS) activity, whereas leukemia cells are supposed to undergo apoptosis due to silencing of the ASNS gene. Because the ASNS gene has a typical CpG island in its promoter, its methylation status in T-ALL cells may be associated with asparaginase sensitivity. Thus, we investigated the significance of ASNS methylation status in asparaginase sensitivity of T-ALL cell lines and prognosis of childhood T-ALL. Sequencing of bisulfite polymerase chain reaction products using next-generation sequencing technology in 22 T-ALL cell lines revealed a stepwise allele-specific methylation of the ASNS gene, in association with an aberrant methylation of a 7q21 imprinted gene cluster. T-ALL cell lines with ASNS hypermethylation status showed significantly higher in vitro l-asparaginase sensitivity in association with insufficient asparaginase-induced upregulation of ASNS gene expression and lower basal ASNS protein expression. A comprehensive analysis of diagnostic samples from pediatric patients with T-ALL in Japanese cohorts (N = 77) revealed that methylation of the ASNS gene was associated with an aberrant methylation of the 7q21 imprinted gene cluster. In pediatric T-ALL patients in Japanese cohorts (n = 75), ASNS hypomethylation status was significantly associated with poor therapeutic outcome, and all cases with poor prognostic SPI1 fusion exclusively exhibited ASNS hypomethylation status. These observations show that ASNS hypomethylation status is associated with asparaginase resistance and is a poor prognostic biomarker in childhood T-ALL.

Published

2022

24. [Application of genome editing technology for the validation of pharmacogenomics in acute lymphoblastic leukemia]

Author

Koshi, Akahane

Subjects

Gene Editing, Technology, Pharmacogenetics, Humans, Precursor Cell Lymphoblastic Leukemia-Lymphoma

Abstract

Therapeutic outcome in childhood acute lymphocytic leukemia has been dramatically improved by recent developments in treatment. However, disease relapse is still observed in approximately 10-15% of the patients. Moreover, adverse effects associated with intensified chemotherapy and hematopoietic stem cell transplantation remain important clinical issues for some survivors. Personalized medicine is valuable, under these circumstances, to reduce adverse effects and further improve the therapeutic outcome. Thus, identifying pharmacogenomic backgrounds associated with individual variation in drug sensitivity of leukemia cells and chemotherapy-induced adverse effects is important for precision medicine development. Recent advances in genome-editing technologies, such as CRISPR/Cas9 system, enable direct confirmation of associations between drug sensitivities and genetic backgrounds, such as polymorphisms and mutations, in the intrinsic genes of leukemia cells. Consequently, genome-editing systems are an ideal tool to develop in vitro and in vivo experimental models of drug sensitivity or resistance. The usefulness of the CRISPR/Cas9 system for the validation of pharmacogenomics in the selection of chemotherapeutic agents for acute lymphocytic leukemia has been discussed with specific examples in this review.

Published

2022

25. Decreased incidence of acute immune thrombocytopenia in children during the COVID-19 pandemic

Author

Daisuke Harama, Kumiko Goi, Kinuko Saito, Hiroki Sato, Shinpei Somazu, Yoshiyuki Furuichi, Kazuya Takahashi, Hiroko Oshiro, Makoto Nakamura, Emi Sawanobori, Kazumasa Sato, Makoto Tsuruta, Yasushi Murakami, Tamao Shinohara, Atsushi Nemoto, Shin Kasai, Minori Tamai, Atsushi Watanabe, Koshi Akahane, Satoru Kojika, Kanji Sugita, and Takeshi Inukai

Subjects

Hematology

Published

2023

26. Prominence of NUDT15 genetic variation associated with 6-mercaptopurine tolerance in a genome-wide association study of Japanese children with acute lymphoblastic leukaemia

Author

Yoichi Tanaka, Kevin Y. Urayama, Makiko Mori, Yuki Arakawa, Daisuke Hasegawa, Yasushi Noguchi, Masakatsu Yanagimachi, Dai Keino, Setsuo Ota, Koshi Akahane, Takeshi Inukai, Mayumi Hangai, Takahisa Kawaguchi, Masatoshi Takagi, Katsuyoshi Koh, Fumihiko Matsuda, and Atsushi Manabe

Subjects

Antimetabolites, Antineoplastic, Japan, Mercaptopurine, Humans, Hematology, Methyltransferases, Precursor Cell Lymphoblastic Leukemia-Lymphoma, Pyrophosphatases, Child, Polymorphism, Single Nucleotide, Genome-Wide Association Study

Abstract

Inherited genetic variation is associated with 6-mercaptopurine (6-MP) dose reduction and frequent toxicities induced by 6-MP. However, the tolerable dose for 6-MP is not fully predicted by the known variation in NUDT15 and TPMT among Asian children with acute lymphoblastic leukaemia (ALL). We performed a genome-wide association study (GWAS) related to 6-MP dose among Japanese children with ALL. This GWAS comprised 224 patients previously enrolled in Tokyo Children's Cancer Study Group clinical studies with replication attempted in 55 patients. Genome-wide single nucleotide polymorphism (SNP) genotypes were evaluated for association with average 6-MP dose during the initial 168 days of maintenance therapy. Possible associations were observed across five gene-coding regions, among which only variants at 13q14.2 were significant and replicated genome-wide (rs116855232, NUDT15, β = -10.99, p = 3.7 × 10

Published

2022

27. Creation of Philadelphia chromosome by CRISPR/Cas9-mediated double cleavages on BCR and ABL1 genes as a model for initial event in leukemogenesis

Author

Minori Tamai, Shinichi Fujisawa, Thao T. T. Nguyen, Chiaki Komatsu, Keiko Kagami, Kenji Kamimoto, Kohei Omachi, Shin Kasai, Daisuke Harama, Atsushi Watanabe, Koshi Akahane, Kumiko Goi, Kazuhito Naka, Tadashi Kaname, Takanori Teshima, and Takeshi Inukai

Subjects

Cancer Research, Molecular Medicine, Molecular Biology

Abstract

The Philadelphia (Ph) chromosome was the first translocation identified in leukemia. It is supposed to be generated by aberrant ligation between two DNA double-strand breaks (DSBs) at the BCR gene located on chromosome 9q34 and the ABL1 gene located on chromosome 22q11. Thus, mimicking the initiation process of translocation, we induced CRISPR/Cas9-mediated DSBs simultaneously at the breakpoints of the BCR and ABL1 genes in a granulocyte-macrophage colony-stimulating factor (GM-CSF) dependent human leukemia cell line. After transfection of two single guide RNAs (sgRNAs) targeting intron 13 of the BCR gene and intron 1 of the ABL1 gene, a factor-independent subline was obtained. In the subline, p210 BCR::ABL1 and its reciprocal ABL1::BCR fusions were generated as a result of balanced translocation corresponding to the Ph chromosome. Another set of sgRNAs targeting intron 1 of the BCR gene and intron 1 of the ABL1 gene induced a factor-independent subline expressing p190 BCR::ABL1. Both p210 and p190 BCR::ABL1 induced factor-independent growth by constitutively activating intracellular signaling pathways for transcriptional regulation of cell cycle progression and cell survival that are usually regulated by GM-CSF. These observations suggested that simultaneous DSBs at the BCR and ABL1 gene breakpoints are initiation events for oncogenesis in Ph + leukemia. (200/200 words)

Published

2022

28. Inherited genetic variants associated with glucocorticoid sensitivity in leukaemia cells

Author

Hiroaki Goto, Koshi Akahane, Yukinori Okada, Kanji Sugita, Keiko Kagami, Meixian Huang, Shotaro Iwamoto, Atsushi Watanabe, Masako Abe, Kevin Y. Urayama, Takeshi Inukai, Tamao Shinohara, Masayoshi Minegishi, and Kumiko Goi

Subjects

0301 basic medicine, acute lymphoblastic leukaemia, Genotype, Prednisolone, Single-nucleotide polymorphism, Genome-wide association study, Biology, Polymorphism, Single Nucleotide, genome‐wide association studies, Dexamethasone, 03 medical and health sciences, Inhibitory Concentration 50, 0302 clinical medicine, Glucocorticoid receptor, Glucocorticoid Sensitivity, Receptors, Glucocorticoid, Japan, Cell Line, Tumor, Gene expression, glucocorticoid sensitivity, SNP, Humans, Gene, Glucocorticoids, Gene Expression Regulation, Leukemic, Gene Expression Profiling, Genetic Variation, Cell Biology, Original Articles, Precursor Cell Lymphoblastic Leukemia-Lymphoma, Molecular biology, 030104 developmental biology, Pharmacogenetics, 030220 oncology & carcinogenesis, Molecular Medicine, Original Article, Drug Screening Assays, Antitumor

Abstract

Identification of genetic variants associated with glucocorticoids (GC) sensitivity of leukaemia cells may provide insight into potential drug targets and tailored therapy. In the present study, within 72 leukaemic cell lines derived from Japanese patients with B‐cell precursor acute lymphoblastic leukaemia (ALL), we conducted genome‐wide genotyping of single nucleotide polymorphisms (SNP) and attempted to identify genetic variants associated with GC sensitivity and NR3C1 (GC receptor) gene expression. IC50 measures for prednisolone (Pred) and dexamethasone (Dex) were available using an alamarBlue cell viability assay. IC50 values of Pred showed the strongest association with rs904419 (P = 4.34 × 10−8), located between the FRMD4B and MITF genes. The median IC50 values of prednisolone for cell lines with rs904419 AA (n = 13), AG (n = 31) and GG (n = 28) genotypes were 0.089, 0.139 and 297 µmol/L, respectively. For dexamethasone sensitivity, suggestive association was observed for SNP rs2306888 (P = 1.43 × 10−6), a synonymous SNP of the TGFBR3 gene. For NR3C1 gene expression, suggestive association was observed for SNP rs11982167 (P = 6.44 × 10−8), located in the PLEKHA8 gene. These genetic variants may affect GC sensitivity of ALL cells and may give rise to opportunities in personalized medicine for effective and safe chemotherapy in ALL patients.

Published

2020

29. High prevalence of <scp> MEF2D </scp> fusion in human B‐cell precursor acute lymphoblastic leukemia cell lines

Author

Kumiko Goi, Fumihiko Hayakawa, Keiko Kagami, Masafumi Abe, Shinya Kojima, Masahito Kawazu, Hiroaki Goto, Kanji Sugita, Toshiya Inaba, Hiroshi Hojo, Hiroyuki Mano, Koshi Akahane, Takahiko Yasuda, Shotaro Iwamoto, Daisuke Harama, Nobutaka Kiyokawa, Atsushi Watanabe, Shinobu Tsuzuki, Shinpei Somazu, Toshihiko Imamura, Masako Abe, Takeshi Inukai, and Masayoshi Minegishi

Subjects

Cancer Research, High prevalence, Oncogene Proteins, Fusion, MEF2 Transcription Factors, business.industry, Lymphoblastic Leukemia, Hematology, General Medicine, Human b cell, Oncology, Cell culture, Cell Line, Tumor, Precursor B-Cell Lymphoblastic Leukemia-Lymphoma, Cancer research, Humans, Medicine, business

Published

2020

30. BCL6 inhibition ameliorates ruxolitinib resistance in CRLF2-rearranged acute lymphoblastic leukemia

Author

Shinobu, Tsuzuki, Takahiko, Yasuda, Hiroaki, Goto, Naoko, Maeda, Koshi, Akahane, Takeshi, Inukai, Hideyuki, Yamamoto, Sivasundaram, Karnan, Akinobu, Ota, Toshinori, Hyodo, Hiroyuki, Konishi, Yoshitaka, Hosokawa, Hitoshi, Kiyoi, and Fumihiko, Hayakawa

Abstract

Philadelphia chromosome-like acute lymphoblastic leukemia (Ph-like ALL) is intractable and mostly harbors genetic alterations that activate JAK or ABL signaling. The commonest subtype of Ph-like ALL exhibits the CRLF2 gene arrangement that brings about JAK1/2-STAT5 pathway activation. However, JAK1/2 inhibition alone is insufficient for treatment, necessitating combinatorial therapies targeting multiple signals. To better understand the mechanisms underlying the insufficient efficacy of JAK inhibition, this study explored gene expression changes upon treatment with a JAK1/2 inhibitor (ruxolitinib) and revealed BCL6 elevation as one such mechanism. Upregulated BCL6 suppressed TP53 expression along with its downstream cell cycle inhibitor p21 (CDKN2A) and proapoptotic molecules, such as FAS, TNFRSF10B, BID, BAX, BAK, PUMA, and NOXA, conferring cells in part with therapy resistance. The BCL6 inhibition (FX1) alone was able to upregulate TP53 and restore TP53 expression that ruxolitinib had diminished. In addition, ruxolitinib and FX1 concertedly downregulated MYC. As a result, FX1 treatment alone had growth-inhibitory and apoptosis-sensitizing effects, but the combination of ruxolitinib and FX1 more potently inhibited leukemia cell growth, enhanced apoptosis sensitivity, and prolonged xenografted mice survival. These findings provide one mechanism for the insufficiency of JAK inhibition for CRLF2-rearranged ALL treatment and BCL6 inhibition as a potentially helpful adjunctive therapy combined with JAK inhibition.

Published

2022

31. Successful treatment of intractable gastrointestinal tract graft-vs-host disease with oral beclomethasone dipropionate in pediatric and young adult patients: Case reports

Author

Koshi Akahane, Atsushi Watanabe, Shinpei Somazu, Daisuke Harama, Tamao Shinohara, Shin Kasai, Hiroko Oshiro, Kumiko Goi, Norio Hasuda, Chihiro Ozawa, Kanji Sugita, and Takeshi Inukai

Subjects

Young Adult, Gastrointestinal Diseases, Beclomethasone, Hematopoietic Stem Cell Transplantation, Graft vs Host Disease, Humans, General Medicine, Child

Abstract

The gastrointestinal (GI) tract is a common target organ of graft-vs-host disease (GVHD) in hematopoietic stem cell transplantation (HSCT) patients, and GI tract GVHD is often resistant to standard treatments such as corticosteroids. Moreover, longterm use of systemic corticosteroids sometimes induces adverse events such as infection. Beclomethasone dipropionate (BDP) is a potent, topically active corticosteroid, which is metabolized to an active derivative in the intestinal mucosa. Oral BDP therapy is reportedly effective against GI tract GVHD in adult HSCT patients, but its efficacy and safety in pediatric patients remain undefined. Here, we report three pediatric and young adult cases who were treated with oral BDP.Three (6-, 7-, and 18-year-old) patients developed stage 2 to 4 lower GI tract GVHD, which was resistant to standard immunosuppressive therapies.Lower GI tract GVHD in these patients was histopathologically proven by endoscopic biopsy.Oral administration of enteric-coated capsules of BDP (3-8 mg/day) was started for the treatment of lower GI tract GVHD.With the introduction of oral BDP therapy, their GI tract symptoms promptly resolved (abdominal pain, within 3-7 days; diarrhea, within 2-3 weeks). Subsequently, systemic immunosuppressive agents such as corticosteroids and mycophenolate mofetil were successfully tapered off. During oral BDP therapy, although cytomegalovirus antigenemia and Acinetobacter Iwoffii sepsis developed in 2 cases, both were curable with conventional treatments. In a young adult case, concomitant BK virus-associated hemorrhagic cystitis resolved after oral BDP was introduced and systemic immunosuppressive agents were reduced. Transient growth restriction was observed in a pediatric case who was treated with oral BDP for approximately 300days.Our experiences suggest that oral BDP therapy is an effective approach for GI tract GVHD that is resistant to standard immunosuppressive therapies. Of clinical importance, our case suggests the possibility that oral BDP therapy may improve the immunosuppressive condition in GI tract GVHD patients by contributing to the reduction of systemic immunosuppressive medications as a result of prompt improvement of GI tract GVHD symptoms.

Published

2022

32. Gastrointestinal tract involvement of Epstein–Barr virus‐associated post‐transplant lymphoproliferative disorder after cord blood transplantation

Author

Hiromi Wakamatsu, Koshi Akahane, Shin Kasai, Atsushi Watanabe, and Kumiko Goi

Subjects

Gastrointestinal Tract, Epstein-Barr Virus Infections, Herpesvirus 4, Human, Pediatrics, Perinatology and Child Health, Hematopoietic Stem Cell Transplantation, Humans, Cord Blood Stem Cell Transplantation, Rituximab, Lymphoproliferative Disorders

Published

2022

33. ASCL1 is a MYCN- and LMO1-dependent member of the adrenergic neuroblastoma core regulatory circuitry

Author

Jo Lynne Rokita, Brian J. Abraham, Shi Hao Tan, Mark W. Zimmerman, Richard A. Young, Nina Weichert-Leahey, Takaomi Sanda, Tze King Tan, Koshi Akahane, Lu Wang, Phuong Cao Thi Ngoc, Lee N. Lawton, John M. Maris, Adam D. Durbin, and A. Thomas Look

Subjects

0301 basic medicine, Cellular differentiation, Science, Gene regulatory network, General Physics and Astronomy, Article, General Biochemistry, Genetics and Molecular Biology, Paediatric cancer, Neuroblastoma, 03 medical and health sciences, Adrenergic Agents, 0302 clinical medicine, Cell Line, Tumor, Basic Helix-Loop-Helix Transcription Factors, medicine, Humans, Gene Regulatory Networks, lcsh:Science, neoplasms, Transcription factor, Regulation of gene expression, N-Myc Proto-Oncogene Protein, Multidisciplinary, biology, Proto-Oncogene Proteins c-ret, Cell Differentiation, Oncogenes, General Chemistry, LIM Domain Proteins, medicine.disease, Survival Analysis, Cell biology, DNA-Binding Proteins, Gene Expression Regulation, Neoplastic, ASCL1, 030104 developmental biology, Regulatory sequence, 030220 oncology & carcinogenesis, biology.protein, lcsh:Q, HAND2, Transcription, Transcription Factors

Abstract

A heritable polymorphism within regulatory sequences of the LMO1 gene is associated with its elevated expression and increased susceptibility to develop neuroblastoma, but the oncogenic pathways downstream of the LMO1 transcriptional co-regulatory protein are unknown. Our ChIP-seq and RNA-seq analyses reveal that a key gene directly regulated by LMO1 and MYCN is ASCL1, which encodes a basic helix-loop-helix transcription factor. Regulatory elements controlling ASCL1 expression are bound by LMO1, MYCN and the transcription factors GATA3, HAND2, PHOX2B, TBX2 and ISL1—all members of the adrenergic (ADRN) neuroblastoma core regulatory circuitry (CRC). ASCL1 is required for neuroblastoma cell growth and arrest of differentiation. ASCL1 and LMO1 directly regulate the expression of CRC genes, indicating that ASCL1 is a member and LMO1 is a coregulator of the ADRN neuroblastoma CRC., Polymorphisms in LMO1 are associated with increased susceptibility to develop neuroblastoma. Here, the authors show that LMO1 directly induces the transcription factor ASCL1, which regulates the differentiation of neurons, demonstrating that ASCL1 is part of the adrenergic neuroblastoma core regulatory circuit.

Published

2019

34. CN470 is a BET/CBP/p300 multi-bromodomain inhibitor and has an anti-tumor activity against MLL-rearranged acute lymphoblastic leukemia

Author

Natsuki Imayoshi, Makoto Yoshioka, Kuniaki Tanaka, Shyh-Ming Yang, Koshi Akahane, Yuki Toda, Shigekuni Hosogi, Takeshi Inukai, Seiji Okada, David J. Maloney, Tatsutoshi Nakahata, Junko Takita, Itaru Kato, and Eishi Ashihara

Subjects

Gene Rearrangement, Gene Expression Regulation, Leukemic, Biophysics, Antineoplastic Agents, Apoptosis, Cell Biology, Cell Cycle Checkpoints, Histone-Lysine N-Methyltransferase, Precursor Cell Lymphoblastic Leukemia-Lymphoma, Biochemistry, Survival Analysis, Xenograft Model Antitumor Assays, Article, Mice, Cell Line, Tumor, Animals, Humans, RNA, Messenger, Molecular Biology, E1A-Associated p300 Protein, Myeloid-Lymphoid Leukemia Protein, Cell Proliferation

Abstract

Acute lymphoblastic leukemia with chromosomal rearrangements involving the mixed-lineage leukemia (MLL) gene (MLL-r ALL) remains an incurable disease. Thus, development of a safe and effective therapeutic agent to treat this disease is crucial to address this unmet medical need. BRD4, a member of the bromodomain and extra-terminal domain (BET) protein family, and cyclic AMP response element binding protein binding protein (CBP) and p300, two paralogous histone acetyltransferases, are all considered cancer drug targets and simultaneous targeting of these proteins may have therapeutic advantages. Here, we demonstrate that a BET/CBP/p300 multi-bromodomain inhibitor, CN470, has anti-tumor activity against MLL-r ALL in vitro and in vivo. CN470, potently inhibited ligand binding to the bromodomains of BRD4, CBP, and p300 and suppressed the growth of MLL-r ALL cell lines and patient-derived cells with MLL rearrangements. CN470 suppressed mRNA and protein expression of MYC and induced apoptosis in MLL-r ALL cells, following a cell cycle arrest in the G1 phase. Moreover, CN470 reduced BRD4 binding to acetylated histone H3. The in vivo effects of CN470 were investigated using SEM(Luc/GFP) cells expressing luminescent markers in an orthotopic mouse model. Mice administered CN470 daily had prolonged survival compared to the vehicle group. Further, CN470 also showed anti-tumor effects against an MLL-r ALL patient-derived xenograft model. These findings suggest that inhibition of BET/CBP/p300 by the multi-bromodomain inhibitor, CN470, represents a promising therapeutic approach against MLL-r ALL.

Published

2021

35. Introduction of the T315I gatekeeper mutation of BCR/ABL1 into a Philadelphia chromosome-positive lymphoid leukemia cell line using the CRISPR/Cas9 system

Author

Thao T. T. Nguyen, Minori Tamai, Daisuke Harama, Keiko Kagami, Shin Kasai, Atsushi Watanabe, Koshi Akahane, Kumiko Goi, and Takeshi Inukai

Subjects

Nucleotides, Dasatinib, Fusion Proteins, bcr-abl, Poly (ADP-Ribose) Polymerase-1, Antineoplastic Agents, Hematology, Precursor Cell Lymphoblastic Leukemia-Lymphoma, Cell Line, Oligodeoxyribonucleotides, Drug Resistance, Neoplasm, CRISPR-Associated Protein 9, Leukemia, Myelogenous, Chronic, BCR-ABL Positive, Mutation, Imatinib Mesylate, Humans, Philadelphia Chromosome, CRISPR-Cas Systems, Protein Kinase Inhibitors, RNA, Guide, Kinetoplastida

Abstract

Imatinib and second-generation tyrosine kinase inhibitors (TKIs) have dramatically improved the prognosis of Philadelphia chromosome-positive (Ph+) acute lymphoblastic leukemia (ALL). However, overcoming TKI resistance due to the T315I gatekeeper mutation of BCR/ABL1 is crucial for further improving the prognosis. The clustered regularly interspaced short palindromic repeats (CRISPR)/Cas9 system is appropriate for establishing a human model of Ph+ ALL with the T315I mutation, because it can induce specific mutations via homologous recombination (HR) repair in cells with intact endogenous HR pathway. Here we used CRISPR/Cas9 to introduce the T315I mutation into the Ph+ lymphoid leukemia cell line KOPN55bi, which appeared to have an active HR pathway based on its resistance to a poly (ADP-Ribose) polymerase-1 inhibitor. Single-guide RNA targeting at codon 315 and single-strand oligodeoxynucleotide containing ACT to ATT nucleotide transition at codon 315 were electroporated with recombinant Cas9 protein. Dasatinib-resistant sublines were obtained after one-month selection with the therapeutic concentration of dasatinib, leading to T315I mutation acquisition through HR. T315I-acquired sublines were highly resistant to imatinib and second-generation TKIs but moderately sensitive to the therapeutic concentration of ponatinib. This authentic human model is helpful for developing new therapeutic strategies overcoming TKI resistance in Ph+ ALL due to T315I mutation.

Published

2021

36. Combination of tyrosine kinase inhibitors and the MCL1 inhibitor S63845 exerts synergistic antitumorigenic effects on CML cells

Author

Harsha S Madapura, Jonas Wallvik, Elham Yektaei-Karin, Niclas Björn, Takeshi Inukai, Koshi Akahane, Leif Stenke, Daniel Salamon, Kourosh Lotfi, Minori Tamai, Ana Zovko, Noémi Nagy, Dorina Ujvari, Marton Keszei, Alena Malyukova, and Thao T. T. Nguyen

Subjects

Cancer Research, Medical Biotechnology (with a focus on Cell Biology (including Stem Cell Biology), Molecular Biology, Microbiology, Biochemistry or Biopharmacy), Antigens, CD34, Apoptosis, Tyrosine-kinase inhibitor, hemic and lymphatic diseases, Antineoplastic Combined Chemotherapy Protocols, Caspase 7, Caspase 3, Cancer stem cells, Chemistry, Myeloid leukemia, Drug Synergism, Hematology, Neoplasm Proteins, Dasatinib, Leukemia, Imatinib Mesylate, Poly(ADP-ribose) Polymerases, Tyrosine kinase, medicine.drug, Pore Forming Cytotoxic Proteins, Cell Survival, medicine.drug_class, Immunology, bcl-X Protein, Antineoplastic Agents, Thiophenes, Article, Small Molecule Libraries, Cellular and Molecular Neuroscience, Targeted therapies, Cell Line, Tumor, Leukemia, Myelogenous, Chronic, BCR-ABL Positive, Pyroptosis, medicine, Humans, Hematologi, Progenitor cell, Medicinsk bioteknologi (med inriktning mot cellbiologi (inklusive stamcellsbiologi), molekylärbiologi, mikrobiologi, biokemi eller biofarmaci), neoplasms, Protein Kinase Inhibitors, Cancer och onkologi, QH573-671, Imatinib, Cell Biology, Phosphate-Binding Proteins, Hematopoietic Stem Cells, medicine.disease, Clone Cells, Pyrimidines, Nilotinib, Drug Resistance, Neoplasm, Preclinical research, Cancer and Oncology, Cancer research, Myeloid Cell Leukemia Sequence 1 Protein, Cytology

Abstract

Tyrosine kinase inhibitor (TKI) treatment has dramatically improved the survival of chronic myeloid leukemia (CML) patients, but measurable residual disease typically persists. To more effectively eradicate leukemia cells, simultaneous targeting of BCR-ABL1 and additional CML-related survival proteins has been proposed. Notably, several highly specific myeloid cell leukemia 1 (MCL1) inhibitors have recently entered clinical trials for various hematologic malignancies, although not for CML, reflecting the insensitivity of CML cell lines to single MCL1 inhibition. Here, we show that combining TKI (imatinib, nilotinib, dasatinib, or asciminib) treatment with the small-molecule MCL1 inhibitor S63845 exerted strong synergistic antiviability and proapoptotic effects on CML lines and CD34+ stem/progenitor cells isolated from untreated CML patients in chronic phase. Using wild-type BCR-ABL1-harboring CML lines and their T315I-mutated sublines (generated by CRISPR/Cas9-mediated homologous recombination), we prove that the synergistic proapoptotic effect of the drug combination depended on TKI-mediated BCR-ABL1 inhibition, but not on TKI-related off-target mechanisms. Moreover, we demonstrate that colony formation of CML but not normal hematopoietic stem/progenitor cells became markedly reduced upon combination treatment compared to imatinib monotherapy. Our results suggest that dual targeting of MCL1 and BCR-ABL1 activity may efficiently eradicate residual CML cells without affecting normal hematopoietic stem/progenitors. Funding Agencies|Cancer Research Funds of Radiumhemmet [174283]; Thorsmans Stiftelse for Pre-leukemi Forskning; Gunnar Grimfors Gavofond for Hematologisk Forskning; Cathrine Everts Research Foundation; Lars Hierta Memorial Foundation; Emil Anderson Fund for Medical Research; Swedish Research CouncilSwedish Research CouncilEuropean Commission [2013-08807]; Karolinska Institute Foundation and Funds; Karolinska InstituteKarolinska Institutet

Published

2021

37. Utility of ASNS gene methylation evaluated with the HPLC method as a pharmacogenomic biomarker to predict asparaginase sensitivity in BCP-ALL.

Author

Atsushi Watanabe, Kunio Miyake, Yuriko Yamada, Ei-Ichiro Sunamura, Takuya Yotani, Keiko Kagami, Shin Kasai, Minori Tamai, Daisuke Harama, Koshi Akahane, Kumiko Goi, Kimiyoshi Sakaguchi, Hiroaki Goto, Shinichiro Kitahara, and Takeshi Inukai

Subjects

PHARMACOGENOMICS, ASPARAGINASE, HIGH performance liquid chromatography, METHYLATION, BIOMARKERS, LYMPHOBLASTIC leukemia

Abstract

Asparaginase is an important agent for the treatment of acute lymphoblastic leukaemia (ALL), but it is occasionally associated with severe adverse events. Thus, for safer and more efficacious therapy, a clinical biomarker predicting asparaginase sensitivity is highly anticipated. Asparaginase depletes serum asparagine by deaminating asparagine into aspartic acid, and ALL cells are thought to be sensitive to asparaginase due to reduced asparagine synthetase (ASNS) activity. We have recently shown that allele-specific methylation of the ASNS gene is highly involved in asparaginase sensitivity in B-precursor ALL (BCP-ALL) by using next-generation sequence (NGS) analysis of bisulphite PCR products of the genomic DNA. Here, we sought to confirm the utility of methylation status of the ASNS gene evaluated with high-performance liquid chromatography (HPLC) analysis of bisulphite PCR products for future clinical applications. In the global methylation status of 23 CpG sites at the boundary region of promoter and exon 1 of the ASNS gene, a strong positive correlation was confirmed between the mean percent methylation evaluated with the HPLC method and that with the NGS method in 79 BCP-ALL cell lines (R2 = 0.85, p = 1.3 × 10-33) and in 63 BCP-ALL clinical samples (R2 = 0.84, p = 5.0 × 10-26). Moreover, methylation status of the ASNS gene evaluated with the HPLC method was significantly associated with in vitro asparaginase sensitivities as well as gene and protein expression levels of ASNS. These observations indicated that the ASNS gene methylation status evaluated with the HPLC method is a reliable biomarker for predicting the asparaginase sensitivity of BCP-ALL. [ABSTRACT FROM AUTHOR]

Published

2023

38. KIR3DL1 Allotype-Dependent Modulation of NK Cell Immunity against Chronic Myeloid Leukemia

Author

Thao T. T. Nguyen, Ai Kawana-Tachikawa, Akifumi Takaori-Kondo, Minori Tamai, Takeshi Inukai, Kaori Nakayama-Hosoya, Takero Shindo, Huong Thi Ngo, Koshi Akahane, and Kiyotaka Izumi

Subjects

Cytotoxicity, Immunologic, medicine.drug_class, Immunology, Cell, Dasatinib, Fusion Proteins, bcr-abl, Biology, Lymphocyte Activation, Tyrosine-kinase inhibitor, hemic and lymphatic diseases, Cell Line, Tumor, Leukemia, Myelogenous, Chronic, BCR-ABL Positive, medicine, Immunology and Allergy, Humans, Receptor, Protein Kinase Inhibitors, Alleles, Gene Expression Regulation, Leukemic, Myeloid leukemia, Receptors, KIR3DL1, General Medicine, Killer Cells, Natural, medicine.anatomical_structure, Cell culture, HLA-B Antigens, Mutation, Cancer research, KIR3DL1, K562 Cells, K562 cells, medicine.drug

Abstract

Tyrosine kinase inhibitor (TKI)–treated chronic myeloid leukemia (CML) patients with increased NK cell number have a better prognosis, and thus, NK cells may suppress CML. However, the efficacy of TKIs varies for reasons yet to be fully elucidated. As NK cell activity is modulated by interactions between their killer cell Ig-like receptors (KIRs) and HLAs of target cells, the combination of their polymorphisms may have functional significance. We previously showed that allelic polymorphisms of KIR3DL1 and HLAs were associated with the prognosis of TKI-treated CML patients. In this study, we focus on differential NK cell activity modulation through KIR3DL1 allotypes. KIR3DL1 expression levels varied according to their alleles. The combination of KIR3DL1 expression level and HLA-Bw4 motifs defined NK cell activity in response to the CML-derived K562 cell line, and Ab-mediated KIR3DL1 blocking reversed this activity. The TKI dasatinib enhanced NK cell activation and cytotoxicity in a KIR3DL1 allotype-dependent manner but did not significantly decrease effector regulatory T cells, suggesting that it directly activated NK cells. Dasatinib also enhanced NK cell cytotoxicity against K562 bearing the BCR-ABL1 T315I TKI resistance–conferring mutation, depending on KIR3DL1/HLA-Bw4 allotypes. Transduction of KIR3DL1*01502 into the NK cell line NK-92 resulted in KIR3DL1 expression and suppression of NK-92 activity by HLA-B ligation, which was reversed by anti-KIR3DL1 Ab. Finally, KIR3DL1 expression levels also defined activation patterns in CML patient–derived NK cells. Our findings raise the possibility of a novel strategy to enhance antitumor NK cell immunity against CML in a KIR3DL1 allotype-dependent manner.

Published

2021

39. IMiDs uniquely synergize with TKIs to upregulate apoptosis of Philadelphia chromosome-positive acute lymphoblastic leukemia cells expressing a dominant-negative IKZF1 isoform

Author

Nobutaka Kiyokawa, Norie Ando, Shin Kasai, Takeshi Inukai, Masako Abe, Abd Aziz Ibrahim, Takashi Yahata, Kanji Sugita, Minori Tamai, Koshi Akahane, Keiko Kagami, Kiyoshi Ando, and Daisuke Harama

Subjects

0301 basic medicine, Cancer Research, Immunology, Article, Flow cytometry, 03 medical and health sciences, Cellular and Molecular Neuroscience, chemistry.chemical_compound, 0302 clinical medicine, Downregulation and upregulation, hemic and lymphatic diseases, Medicine, Protein kinase B, RC254-282, QH573-671, medicine.diagnostic_test, business.industry, Ponatinib, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Imatinib, Cell Biology, IKZF3, 030104 developmental biology, chemistry, Apoptosis, 030220 oncology & carcinogenesis, Cancer research, Cytology, business, Tyrosine kinase, medicine.drug

Abstract

The long-term prognosis of Philadelphia chromosome-positive acute lymphoblastic leukemia (Ph + ALL) is still unsatisfactory even after the emergence of tyrosine kinase inhibitors (TKIs) against chimeric BCR-ABL, and this is associated with the high incidence of genetic alterations of Ikaros family zinc finger 1 (IKZF1), most frequently the hemi-allelic loss of exons 4–7 expressing a dominant-negative isoform Ik6. We found that lenalidomide (LEN), a representative of immunomodulatory drugs (IMiDs), which have been long used for the treatment of multiple myeloma, specifically induced accumulation of Ik6 with the disappearance of functional isoforms within 24 h (i.e., abrupt and complete shut-down of the IKZF1 activity) in Ik6-positive Ph+ALL cells in a neddylation-dependent manner. The functional IKZF3 isoforms expression was also abruptly and markedly downregulated. The LEN treatment specifically suppressed proliferation of Ik6-positive-Ph+ALL cells by inducing cell cycle arrest via downregulation of cyclins D3 and E and CDK2, and of importance, markedly upregulated their apoptosis in synergy with the TKI imatinib (IM). Apoptosis of IM-resistant Ph+ALL cells with T315I mutation of BCR-ABL was also upregulated by LEN in the presence of the newly developed TKI ponatinib. Analyses of flow cytometry, western blot, and oligonucleotide array revealed that apoptosis was caspase-/p53-dependent and associated with upregulation of pro-apoptotic Bax/Bim, enhanced dephosphorylation of BCR-ABL/Akt, and downregulation of oncogenic helicase genes HILLS, CDC6, and MCMs4 and 8. Further, the synergism of LEN with IM was clearly documented as a significant prolongation of survival in the xenograft mice model. Because this synergism was further potentiated in vitro by dexamethasone, a key drug for ALL treatment, the strategy of repositioning IMiDs for the treatment of Ik6-positive Ph+ALL patients certainly shed new light on an outpatient-based treatment option for achieving their long-term durable remission and higher QOL, particularly for those who are not tolerable to intensified therapeutic approaches.

Published

2021

40. Resistance of t(17;19)‐acute lymphoblastic leukemia cell lines to multiagents in induction therapy

Author

Kumiko Goi, Tatsuya Ito, Hiroko Fukushima, Mark P. Kamps, Masatoshi Takagi, Masako Abe, Toshiya Inaba, Etsuro Ito, Kiminori Terui, Kanji Sugita, Koshi Akahane, Shinpei Somazu, Takeshi Inukai, Tsutomu Toki, Thomas Look, Junko Takita, Tamao Shinohara, Masayoshi Minegishi, Akira Ohara, Junya Fujimura, Daisuke Harama, Atsushi Watanabe, Hiroyuki Takahashi, Hiroaki Goto, Mikiya Endo, Takashi Fukushima, Hiroko Oshiro, Keiko Kagami, and Toru Nanmoku

Subjects

0301 basic medicine, Cancer Research, Vincristine, Neoplasm, Residual, Genotype, Cyclophosphamide, Daunorubicin, medicine.medical_treatment, Antineoplastic Agents, Chromosomal translocation, Biology, chemotherapy, lcsh:RC254-282, Translocation, Genetic, Cell Line, Immunophenotyping, Mice, 03 medical and health sciences, 0302 clinical medicine, Gene Frequency, medicine, Animals, Humans, Radiology, Nuclear Medicine and imaging, ATP Binding Cassette Transporter, Subfamily B, Member 1, Alleles, Original Research, Cancer Biology, Chemotherapy, Dose-Response Relationship, Drug, leukemia, Precursor Cell Lymphoblastic Leukemia-Lymphoma, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, medicine.disease, Pediatric cancer, pediatric cancer, Disease Models, Animal, Leukemia, 030104 developmental biology, Oncology, Drug Resistance, Neoplasm, Cell culture, 030220 oncology & carcinogenesis, Cancer research, hematalogical cancer, Female, Chromosomes, Human, Pair 19, Chromosomes, Human, Pair 17, medicine.drug

Abstract

t(17;19)(q21‐q22;p13), responsible for TCF3‐HLF fusion, is a rare translocation in childhood B‐cell precursor acute lymphoblastic leukemia(BCP‐ALL). t(1;19)(q23;p13), producing TCF3‐PBX1 fusion, is a common translocation in childhood BCP‐ALL. Prognosis of t(17;19)‐ALL is extremely poor, while that of t(1;19)‐ALL has recently improved dramatically in intensified chemotherapy. In this study, TCF3‐HLF mRNA was detectable at a high level during induction therapy in a newly diagnosed t(17;19)‐ALL case, while TCF3‐PBX1 mRNA was undetectable at the end of induction therapy in most newly diagnosed t(1;19)‐ALL cases. Using 4 t(17;19)‐ALL and 16 t(1;19)‐ALL cell lines, drug response profiling was analyzed. t(17;19)‐ALL cell lines were found to be significantly more resistant to vincristine (VCR), daunorubicin (DNR), and prednisolone (Pred) than t(1;19)‐ALL cell lines. Sensitivities to three (Pred, VCR, and l‐asparaginase [l‐Asp]), four (Pred, VCR, l‐Asp, and DNR) and five (Pred, VCR, l‐Asp, DNR, and cyclophosphamide) agents, widely used in induction therapy, were significantly poorer for t(17;19)‐ALL cell lines than for t(1;19)‐ALL cell lines. Consistent with poor responses to VCR and DNR, gene and protein expression levels of P‐glycoprotein (P‐gp) were higher in t(17;19)‐ALL cell lines than in t(1;19)‐ALL cell lines. Inhibitors for P‐gp sensitized P‐gp‐positive t(17;19)‐ALL cell lines to VCR and DNR. Knockout of P‐gp by CRISPRCas9 overcame resistance to VCR and DNR in the P‐gp‐positive t(17;19)‐ALL cell line. A combination of cyclosporine A with DNR prolonged survival of NSG mice inoculated with P‐gp‐positive t(17;19)‐ALL cell line. These findings indicate involvement of P‐gp in resistance to VCR and DNR in Pgp positive t(17;19)‐ALL cell lines. In all four t(17;19)‐ALL cell lines, RAS pathway mutation was detected. Furthermore, among 16 t(1;19)‐ALL cell lines, multiagent resistance was usually observed in the cell lines with RAS pathway mutation in comparison to those without it, suggesting at least a partial involvement of RAS pathway mutation in multiagent resistance of t(17;19)‐ALL.

Published

2019

41. Eradication of Central Nervous System Leukemia of T-Cell Origin with a Brain-Permeable LSD1 Inhibitor

Author

Takeshi Inukai, Yoshiaki Kuroda, Shiori Saito, Daisuke Koyama, Shin Sato, Takashi Umehara, Koshi Akahane, Jiro Kikuchi, Naoki Osada, Hiroo Koyama, and Yusuke Furukawa

Subjects

0301 basic medicine, Cancer Research, Central nervous system, Antineoplastic Agents, Apoptosis, Biology, Precursor T-Cell Lymphoblastic Leukemia-Lymphoma, Article, Central Nervous System Neoplasms, Mice, 03 medical and health sciences, In vivo, Cell Line, Tumor, Biomarkers, Tumor, medicine, Animals, Humans, Progenitor cell, Cytotoxicity, Receptor, Notch3, T-Cell Acute Lymphocytic Leukemia Protein 1, Cell Proliferation, Histone Demethylases, Xenograft Model Antitumor Assays, In vitro, Gene Expression Regulation, Neoplastic, Disease Models, Animal, 030104 developmental biology, medicine.anatomical_structure, Oncology, Blood-Brain Barrier, Cell culture, Cancer research, TAL1

Abstract

Purpose: Lysine-specific demethylase 1 (LSD1) regulates several biological processes via the bifunctional modulation of enhancer functions. Recently, we reported that LSD1 overexpression is a founder abnormality of T-cell leukemogenesis and is maintained in fully transformed T-cell acute lymphoblastic leukemia (T-ALL) cells. On the basis of this finding, we attempted to develop novel LSD1 inhibitors effective for T-ALL with central nervous system (CNS) involvement. Experimental Design: We chemically modified the prototype LSD inhibitor tranylcypromine (TCP) and screened for cytotoxicity against TCP-resistant T-ALL cell lines. In vivo efficacy of novel LSD1 inhibitors was examined in immunodeficient mice transplanted with luciferase-expressing T-ALL cell lines, which faithfully reproduce human T-ALL with CNS involvement. Results: We found robust cytotoxicity against T-ALL cells, but not normal bone marrow progenitors, for two N-alkylated TCP derivatives, S2116 and S2157. The two compounds induced apoptosis in TCP-resistant T-ALL cells in vitro and in vivo by repressing transcription of the NOTCH3 and TAL1 genes through increased H3K9 methylation and reciprocal H3K27 deacetylation at superenhancer regions. Both S2116 and S2157 significantly retarded the growth of T-ALL cells in xenotransplanted mice and prolonged the survival of recipients as monotherapy and in combination with dexamethasone. Notably, S2157 could almost completely eradicate CNS leukemia because of its ability to efficiently pass through the blood–brain barrier. Conclusions: These findings provide a molecular basis and rationale for the inclusion of a brain-permeable LSD1 inhibitor, S2157, in treatment strategies for T-ALL with CNS involvement.

Published

2019

42. Glucocorticoid receptor gene mutations confer glucocorticoid resistance in B-cell precursor acute lymphoblastic leukemia

Author

Minori Tamai, Shin Kasai, Koshi Akahane, Thao Nguyen Thu, Keiko Kagami, Chiaki Komatsu, Masako Abe, Atsushi Watanabe, Kumiko Goi, Kunio Miyake, Toshiya Inaba, Junko Takita, Hiroaki Goto, Masayoshi Minegishi, Shotaro Iwamoto, Kanji Sugita, and Takeshi Inukai

Subjects

Endocrinology, Diabetes and Metabolism, Clinical Biochemistry, Cell Biology, Precursor Cell Lymphoblastic Leukemia-Lymphoma, Biochemistry, Receptors, Glucocorticoid, Endocrinology, Recurrence, Mutation, Humans, Molecular Medicine, Glucocorticoids, Molecular Biology, Metabolism, Inborn Errors

Abstract

Glucocorticoid (GC) is a key drug in the treatment of B-cell precursor acute lymphoblastic leukemia (BCP-ALL), and the initial GC response is an important prognostic factor. GC receptors play an essential role in GC sensitivity, and somatic mutations of the GC receptor gene, NR3C1, are reportedly identified in some BCP-ALL cases, particularly at relapse. Moreover, associations of somatic mutations of the CREB-binding protein (CREBBP) and Wolf-Hirschhorn syndrome candidate 1 (WHSC1) genes with the GC-resistance of ALL have been suggested. However, the significance of these mutations in the GC sensitivity of BCP-ALL remains to be clarified in the intrinsic genes. In the present study, we sequenced NR3C1, WHSC1, and CREBBP genes in 99 BCP-ALL and 22 T-ALL cell lines (32 and 67 cell lines were known to be established at diagnosis and at relapse, respectively), and detected their mutations in 19 (2 cell lines at diagnosis and 15 cell lines at relapse), 26 (6 and 15), and 38 (11 and 15) cell lines, respectively. Of note, 14 BCP-ALL cell lines with the NR3C1 mutations were significantly more resistant to GC than those without mutations. In contrast, WHSC1 and CREBBP mutations were not associated with GC resistance. However, among the NR3C1 unmutated BCP-ALL cell lines, WHSC1 mutations tended to be associated with GC resistance and lower NR3C1 gene expression. Finally, we successfully established GC-resistant sublines of the GC-sensitive BCP-ALL cell line (697) by disrupting ligand binding and DNA binding domains of the NR3C1 gene using the CRISPR/Cas9 system. These observations demonstrated that somatic mutations of the NR3C1 gene, and possibly the WHSC1 gene, confer GC resistance in BCP-ALL.

Published

2022

43. Association of relapse-linked ARID5B single nucleotide polymorphisms with drug resistance in B-cell precursor acute lymphoblastic leukemia cell lines

Author

Masako Abe, Tamao Shinohara, Takeshi Inukai, Kanji Sugita, Minori Tamai, Masayoshi Minegishi, Keiko Kagami, Meixian Huang, Shotaro Iwamoto, Kumiko Goi, Daisuke Harama, Hiroaki Goto, Atsushi Watanabe, Koshi Akahane, and Shinpei Somazu

Subjects

Cancer Research, Vincristine, Drug sensitivities, Single-nucleotide polymorphism, Biology, lcsh:RC254-282, 03 medical and health sciences, 0302 clinical medicine, Genotype, Gene expression, Genetics, medicine, Allele, lcsh:QH573-671, B cell, lcsh:Cytology, ARID5B, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Molecular biology, Single nucleotide polymorphism, Reverse transcription polymerase chain reaction, B-cell precursor acute lymphoblastic leukemia, medicine.anatomical_structure, Oncology, 030220 oncology & carcinogenesis, Cytarabine, Primary Research, medicine.drug

Abstract

Background The genetic variants of the ARID5B gene have recently been reported to be associated with disease susceptibility and treatment outcome in childhood acute lymphoblastic leukemia (ALL). However, few studies have explored the association of ARID5B with sensitivities to chemotherapeutic agents. Methods We genotyped susceptibility-linked rs7923074 and rs10821936 as well as relapse-linked rs4948488, rs2893881, and rs6479778 of ARDI5B by direct sequencing of polymerase chain reaction (PCR) products in 72 B-cell precursor-ALL (BCP-ALL) cell lines established from Japanese patients. We also quantified their ARID5B expression levels by real-time reverse transcription PCR, and determined their 50% inhibitory concentration (IC50) values by alamarBlue assays in nine representative chemotherapeutic agents used for ALL treatment. Results No significant associations were observed in genotypes of the susceptibility-linked single nucleotide polymorphisms (SNPs) and the relapsed-linked SNPs with ARID5B gene expression levels. Of note, IC50 values of vincristine (VCR) (median IC50: 39.6 ng/ml) in 12 cell lines with homozygous genotype of risk allele (C) in the relapse-linked rs4948488 were significantly higher (p = 0.031 in Mann–Whitney U test) than those (1.04 ng/ml) in 60 cell lines with heterozygous or homozygous genotypes of the non-risk allele (T). Furthermore, the IC50 values of mafosfamide [Maf; active metabolite of cyclophosphamide (CY)] and cytarabine (AraC) tended to be associated with the genotype of rs4948488. Similar associations were observed in genotypes of the relapse-linked rs2893881 and rs6479778, but not in those of the susceptibility-linked rs7923074 and rs10821936. In addition, the IC50 values of methotrexate (MTX) were significantly higher (p = 0.023) in 36 cell lines with lower ARID5B gene expression (median IC50: 37.1 ng/ml) than those in the other 36 cell lines with higher expression (16.9 ng/ml). Conclusion These observations in 72 BCP-ALL cell lines suggested that the risk allele of the relapse-linked SNPs of ARID5B may be involved in a higher relapse rate because of resistance to chemotherapeutic agents such as VCR, CY, and AraC. In addition, lower ARID5B gene expression may be associated with MTX resistance.

Published

2020

44. Author response for 'High prevalence of <scp> MEF2D </scp> fusion in human B‐cell precursor acute lymphoblastic leukemia cell lines'

Author

Takeshi Inukai, Kumiko Goi, Nobutaka Kiyokawa, Kanji Sugita, Masahito Kawazu, Shinpei Somazu, Daisuke Harama, Hiroaki Goto, Toshihiko Imamura, Masayoshi Minegishi, Hiroyuki Mano, Koshi Akahane, Masako Abe, Shinya Kojima, Keiko Kagami, Takahiko Yasuda, Atsushi Watanabe, Hiroshi Hojo, Masafumi Abe, Shinobu Tsuzuki, Shotaro Iwamoto, Fumihiko Hayakawa, and Toshiya Inaba

Subjects

High prevalence, Cell culture, Lymphoblastic Leukemia, Cancer research, Biology, Human b cell

Published

2020

45. Specific, targetable interactions with the microenvironment influence imatinib-resistant chronic myeloid leukemia

Author

Richard A. Van Etten, Nina Rüssel, Koshi Akahane, Melanie Meister, Raquel S. Pereira, Julian Niemann, Frank Schnütgen, Maximilian Merten, Costanza Zanetti, Thomas Oellerich, Hans Michael Kvasnicka, Mike Heilemann, Daniela S. Krause, Minori Tamai, Rahul Kumar, Marina S. Dietz, Heike Pfeifer, Takeshi Inukai, Franck E. Nicolini, and Valentina R. Minciacchi

Subjects

Cancer Research, bcr-abl, Drug Resistance, Fusion Proteins, bcr-abl, Mice, hemic and lymphatic diseases, 2.1 Biological and endogenous factors, Aetiology, Chronic, Cancer, Leukemia, Kinase, Imidazoles, Integrin beta3, Myeloid leukemia, Hematology, Protein-Serine-Threonine Kinases, Pyridazines, Oncology, 5.1 Pharmaceuticals, Imatinib Mesylate, Development of treatments and therapeutic interventions, Signal transduction, Tyrosine kinase, Cancer microenvironment, Clinical Sciences, Oncology and Carcinogenesis, Immunology, Biology, Protein Serine-Threonine Kinases, Article, Rare Diseases, Leukemia, Myelogenous, Chronic, BCR-ABL Positive, medicine, Animals, Humans, ddc:610, Oncogene, Fusion Proteins, Stem Cell Research, medicine.disease, Fibronectins, Transplantation, Drug Resistance, Neoplasm, Preclinical research, Focal Adhesion Protein-Tyrosine Kinases, Cancer research, Neoplasm, BCR-ABL Positive, Myelogenous

Abstract

Therapy resistance in leukemia may be due to cancer cell-intrinsic and/or -extrinsic mechanisms. Mutations within BCR-ABL1, the oncogene giving rise to chronic myeloid leukemia (CML), lead to resistance to tyrosine kinase inhibitors (TKI), and some are associated with clinically more aggressive disease and worse outcome. Using the retroviral transduction/transplantation model of CML and human cell lines we faithfully recapitulate accelerated disease course in TKI resistance. We show in various models, that murine and human imatinib-resistant leukemia cells positive for the oncogene BCR-ABL1T315I differ from BCR-ABL1 native (BCR-ABL1) cells with regards to niche location and specific niche interactions. We implicate a pathway via integrin β3, integrin-linked kinase (ILK) and its role in deposition of the extracellular matrix (ECM) protein fibronectin as causative of these differences. We demonstrate a trend towards a reduced BCR-ABL1T315I+ tumor burden and significantly prolonged survival of mice with BCR-ABL1T315I+ CML treated with fibronectin or an ILK inhibitor in xenogeneic and syngeneic murine transplantation models, respectively. These data suggest that interactions with ECM proteins via the integrin β3/ILK-mediated signaling pathway in BCR-ABL1T315I+ cells differentially and specifically influence leukemia progression. Niche targeting via modulation of the ECM may be a feasible therapeutic approach to consider in this setting.

Published

2020

46. Degradation of Janus kinases in CRLF2-rearranged acute lymphoblastic leukemia

Author

Kathryn G. Roberts, Lisa J Alcock, Lauren Rowland, Divyabharathi Chepyala, Mark R. Litzow, Elisabeth Paietta, Jamie Jarusiewicz, Baranda S Hansen, Lei Yang, Yunchao Chang, Shondra M. Pruett-Miller, Randolph Larsen, Toshihiko Imamura, Aman Seth, Zoran Rankovic, Koshi Akahane, Dylan Maxwell, Jaeki Min, Shanshan Yu-Chen Bradford, Jun J. Yang, Marisa Actis, Chunxu Qu, Charles G. Mullighan, Stanley Nithianantham, Marcus Fischer, Anand Mayasundari, and Hiroaki Goto

Subjects

Models, Molecular, Ruxolitinib, Immunology, Plenary Paper, Context (language use), Protein degradation, Biochemistry, Mice, Inbred NOD, Cell Line, Tumor, Nitriles, Drug Discovery, medicine, Animals, Humans, Receptors, Cytokine, Protein Kinase Inhibitors, Janus Kinases, Chemistry, Gene Expression Regulation, Leukemic, Cereblon, Cell Biology, Hematology, Janus Kinase 2, Precursor Cell Lymphoblastic Leukemia-Lymphoma, medicine.disease, Leukemia, Pyrimidines, Proteolysis, Cancer research, Intercellular Signaling Peptides and Proteins, Pyrazoles, Female, Signal transduction, Janus kinase, Tyrosine kinase, medicine.drug

Abstract

CRLF2-rearranged (CRLF2r) acute lymphoblastic leukemia (ALL) accounts for more than half of Philadelphia chromosome-like (Ph-like) ALL and is associated with a poor outcome in children and adults. Overexpression of CRLF2 results in activation of Janus kinase (JAK)-STAT and parallel signaling pathways in experimental models, but existing small molecule inhibitors of JAKs show variable and limited efficacy. Here, we evaluated the efficacy of proteolysis-targeting chimeras (PROTACs) directed against JAKs. Solving the structure of type I JAK inhibitors ruxolitinib and baricitinib bound to the JAK2 tyrosine kinase domain enabled the rational design and optimization of a series of cereblon (CRBN)-directed JAK PROTACs utilizing derivatives of JAK inhibitors, linkers, and CRBN-specific molecular glues. The resulting JAK PROTACs were evaluated for target degradation, and activity was tested in a panel of leukemia/lymphoma cell lines and xenograft models of kinase-driven ALL. Multiple PROTACs were developed that degraded JAKs and potently killed CRLF2r cell lines, the most active of which also degraded the known CRBN neosubstrate GSPT1 and suppressed proliferation of CRLF2r ALL in vivo, e.g. compound 7 (SJ988497). Although dual JAK/GSPT1-degrading PROTACs were the most potent, the development and evaluation of multiple PROTACs in an extended panel of xenografts identified a potent JAK2-degrading, GSPT1-sparing PROTAC that demonstrated efficacy in the majority of kinase-driven xenografts that were otherwise unresponsive to type I JAK inhibitors, e.g. compound 8 (SJ1008030). Together, these data show the potential of JAK-directed protein degradation as a therapeutic approach in JAK-STAT–driven ALL and highlight the interplay of JAK and GSPT1 degradation activity in this context.

Published

2020

47. Tumor-intrinsic and -extrinsic determinants of response to blinatumomab in adults with B-ALL

Author

Anthony S. Stein, Charles G. Mullighan, Toshihiko Imamura, Koshi Akahane, E.K. Allen, Yaqi Zhao, Ibrahim Aldoss, Jeremy Chase Crawford, Stephen J. Forman, Guido Marcucci, Chunxu Qu, Ravi Bhatia, Zhaohui Gu, Thomas B. Alexander, Hiroaki Goto, Anthony E. Zamora, Paul G. Thomas, Kathryn G. Roberts, and Jeremy Wang

Subjects

Cytotoxicity, Immunologic, Male, Biochemistry, Antineoplastic Agents, Immunological, immune system diseases, Recurrence, T-Lymphocyte Subsets, hemic and lymphatic diseases, Antibodies, Bispecific, Protein Isoforms, RNA, Neoplasm, B-Lymphocytes, biology, hemic and immune systems, Hematology, Middle Aged, Biomarker (medicine), Blinatumomab, Female, Antibody, Single-Cell Analysis, medicine.drug, Adult, Adolescent, Immunology, Antigens, CD19, chemical and pharmacologic phenomena, CD19, Young Adult, Immune system, Antigen, Antigens, Neoplasm, Precursor B-Cell Lymphoblastic Leukemia-Lymphoma, medicine, Humans, Amino Acid Sequence, RNA, Messenger, Aged, Retrospective Studies, Salvage Therapy, Sequence Homology, Amino Acid, business.industry, Gene Expression Profiling, Cell Biology, Aneuploidy, Minimal residual disease, Gene expression profiling, Drug Resistance, Neoplasm, Mutation, biology.protein, Cancer research, business, Sequence Alignment

Abstract

Blinatumomab, a bispecific antibody that directs CD3+ T cells to CD19+ tumor cells, shows variable efficacy in B-progenitor acute lymphoblastic leukemia (B-ALL). To determine tumor-intrinsic and -extrinsic determinants of response, we studied 44 adults with relapsed or refractory B-ALL (including 2 minimal residual disease positive) treated with blinatumomab using bulk tumor and single-cell sequencing. The overall response rate in patients with hematological disease was 55%, with a high response rate in those with CRLF2-rearranged Philadelphia chromosome–like ALL (12 [75%] of 16). Pretreatment samples of responders exhibited a tumor-intrinsic transcriptomic signature of heightened immune response. Multiple mechanisms resulted in loss of CD19 expression, including CD19 mutations, CD19-mutant allele-specific expression, low CD19 RNA expression, and mutations in CD19 signaling complex member CD81. Patients with low hypodiploid ALL were prone to CD19− relapse resulting from aneuploidy-mediated loss of the nonmutated CD19 allele. Increased expression of a CD19 isoform with intraexonic splicing of exon 2, CD19 ex2part, at baseline or during therapy was associated with treatment failure. These analyses demonstrate both tumor-intrinsic and -extrinsic factors influence blinatumomab response. We show that CD19 mutations are commonly detected in CD19− relapse during blinatumomab treatment. Identification of the CD19 ex2part splice variant represents a new biomarker predictive of blinatumomab therapy failure.

Published

2020

48. Autologous Stem Cell Rescue for Graft Failure of Second Allogeneic Stem Cell Transplant After Engraftment of Primary Allogeneic Transplant

Author

Kanji Sugita, Takeshi Inukai, Keiichi Koizumi, Koshi Akahane, Hiroko Oshiro, Kumiko Goi, Kenichi Matsuda, Norikazu Harii, Shinpei Somazu, and Atsushi Watanabe

Subjects

Transplantation, Autologous Stem Cell Rescue, medicine.medical_specialty, business.industry, Surgery, Haematopoiesis, surgical procedures, operative, medicine.anatomical_structure, Cord blood, medicine, Transplantation Conditioning, Bone marrow, Stem cell, business, Etoposide, medicine.drug

Abstract

Here, we describe a case of primary graft failure with severe sepsis in a boy who experienced frequent relapses of osteosarcoma. The patient had undergone haploidentical bone marrow transplant after engraftment of unrelated cord blood transplant performed 10 months earlier. Considering his severe condition, we transfused autologous peripheral stem cells along with a single dose of etoposide (50 mg/m2). Granulocyte engraftment was confirmed on human leukocyte antigen-microsatellite analysis of bone marrow on day 14. Although the patient died due to respiratory failure, transfusion of autologous hematopoietic stem cells is a reasonable rescue option for graft failure even in patients whose background hematopoiesis is reconstituted by a first donor.

Published

2019

49. Genome-Wide CRISPR-Cas9 Screen Identifies Rationally Designed Combination Therapies Relevant for CRLF2-Rearranged Ph-like ALL

Author

Kensuke Sasaki, Takuji Yamauchi, Yuichiro Semba, Jumpei Nogami, Hiroshi Imanaga, Tatsuya Terasaki, Fumihiko Nakao, Koshi Akahane, Takeshi Inukai, Els Verhoeyen, Koichi Akashi, and Takahiro Maeda

Subjects

Immunology, Cell Biology, Hematology, Biochemistry

Abstract

Philadelphia chromosome-like acute lymphoblastic leukemia (Ph-like ALL, also known as BCR-ABL1-like ALL) is a disease entity of B-cell ALL that exhibits a gene expression profile, similar to that of Philadelphia chromosome-positive ALL. Ph-like ALL is categorized into two disease subtypes: "ABL-class"- and "CRLF2/JAK pathway"-types, both of which harbor gene alterations that constitutively activate cytokine/growth factor-related signals. Ph-like ALL with the CRLF2 rearrangement exhibits poor clinical outcomes and is the most common subtype of Ph-like ALL. Tyrosine kinase inhibitor (TKI)-based treatment regimens are effective in treating ABL-class type Ph-like ALL; however, no standard regimen has been established for the CRLF2/JAK pathway type. While multiple chemotherapeutic regimens, including Ruxolitinib monotherapy and/or its combination with chemotherapy, are being tested, their efficacy is reportedly limited. Thus, novel approaches are needed to treat CRLF2/JAK pathway type Ph-like ALL, in particular for CRLF2-rearranged (CRLF2-r) ALL. To identify molecules/pathways relevant for CRLF2-r ALL pathogenesis, we performed genome-wide CRISPR-Cas9 dropout screens in the presence or absence of Ruxolitinib using two IgH-CRLF2-r ALL lines (MUTZ5 and KOPN49) that differ in RAS mutational status. To do so, we employed a baboon envelope pseudotyped lentiviral vector system, which, for the first time, enabled highly efficient transduction of human B cell amenable for genome-wide CRSPR/Cas9 screens. While sgRNAs targeting CRLF2, IL7RA or JAK1/2 significantly affected cell fitness in both lines, those targeting STAT5A, STAT5B or STAT3 did not, suggesting that the JAK-STAT axis is largely dispensable for IgH-CRLF2-r ALL cell survival. We show that regulators of RAS signaling are critical for cell fitness and Ruxolitinib sensitivity and that CRKL and FLT3 depletion enhances Ruxolitinib sensitivity in RAS wild-type (WT) cells. Gilteritinib, a pan-tyrosine kinase inhibitor that reduces CRKL activity, effectively killed RAS WT IgH-CRLF2-r ALL cells in vitro and in vivo, either alone or combined with Ruxolitinib. We further show that combining Gilteritinib with Trametinib, a MEK1/2 inhibitor, is an effective means to target IgH-CRLF2-r ALL cells regardless of RAS mutational status. Our study delineates molecules/pathways relevant for CRLF2-r ALL pathogenesis and could suggest rationally designed combination therapies appropriate for disease subtypes. Disclosures No relevant conflicts of interest to declare.

Published

2021

50. Epigenetic Modification of Death Receptor Genes for TRAIL and TRAIL Resistance in Childhood B-Cell Precursor Acute Lymphoblastic Leukemia

Author

Takeshi Inukai, Kunio Miyake, Hideo Yagita, Atsushi Watanabe, Kumiko Goi, Koshi Akahane, and Keiko Kagami

Subjects

0301 basic medicine, medicine.medical_treatment, QH426-470, Biology, Article, Epigenesis, Genetic, TNF-Related Apoptosis-Inducing Ligand, 03 medical and health sciences, 0302 clinical medicine, Cell Line, Tumor, death receptors, Genetics, medicine, Humans, Epigenetics, Promoter Regions, Genetic, Genetics (clinical), B cell, epigenetics, Immunotherapy, Methylation, DNA Methylation, Precursor Cell Lymphoblastic Leukemia-Lymphoma, medicine.disease, Chimeric antigen receptor, B-cell precursor acute lymphoblastic leukemia, Receptors, TNF-Related Apoptosis-Inducing Ligand, Leukemia, 030104 developmental biology, medicine.anatomical_structure, Drug Resistance, Neoplasm, 030220 oncology & carcinogenesis, DNA methylation, Cancer research, CpG Islands, Blinatumomab, medicine.drug

Abstract

Immunotherapies specific for B-cell precursor acute lymphoblastic leukemia (BCP-ALL), such as anti-CD19 chimeric antigen receptor (CAR) T-cells and blinatumomab, have dramatically improved the therapeutic outcome in refractory cases. In the anti-leukemic activity of those immunotherapies, TNF-related apoptosis-inducing ligand (TRAIL) on cytotoxic T-cells plays an essential role by inducing apoptosis of the target leukemia cells through its death receptors (DR4 and DR5). Since there are CpG islands in the promoter regions, hypermethylation of the DR4 and DR5 genes may be involved in resistance of leukemia cells to immunotherapies due to TRAIL-resistance. We analyzed the DR4 and DR5 methylation status in 32 BCP-ALL cell lines by sequencing their bisulfite PCR products with a next-generation sequencer. The DR4 and DR5 methylation status was significantly associated with the gene and cell-surface expression levels and the TRAIL-sensitivities. In the clinical samples at diagnosis (459 cases in the NOPHO study), both DR4 and DR5 genes were unmethylated in the majority of cases, whereas methylated in several cases with dic(9, 20), MLL-rearrangement, and hypodiploidy, suggesting that evaluation of methylation status of the DR4 and DR5 genes might be clinically informative to predict efficacy of immunotherapy in certain cases with such unfavorable karyotypes. These observations provide an epigenetic rational for clinical efficacy of immunotherapy in the vast majority of BCP-ALL cases.

Published

2021