Single-Cell Multiomics Reveals Increased Plasticity, Resistant Populations and Stem-Cell-like Blasts in KMT2A-Rearranged Leukemia

Chen, Changya; Yu, Wenbao; Alikarami, Fatemeh; Qiu, Qi; Chen, Chia‐Hui; Flournoy, Jennifer; Gao, Peng; Li, Fang; Hu, Yuxuan; Zhu, Qin; Wang, Kai; Libbrecht, Clara; Felmeister, Alex; Rozich, Isaiah; Ding, Yangyang; Hunger, Stephen P.; Wu, Hao; Brown, Patrick; Guest, Erin; Barrett, David M.; Bernt, Kathrin M.; Tan, Kai

doi:10.1182/blood-2021-146102

Cited by 10 publications

(22 citation statements)

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“…Deregulation of these genes initiates the development of leukemia through inhibition of proper hematopoietic development [13,14]. The KMT2Ar fusion genes with their breakpoints code for their related proteins and are regarded as poor factors for both B-ALL and acute myeloid leukemia (AML) [13][14][15].…”

Section: Discussionmentioning

confidence: 99%

Poor treatment responses were related to poor outcomes in pediatric B cell acute lymphoblastic leukemia with KMT2A rearrangements

Wen¹,

Zhou

Shen

et al. 2022

BMC Cancer

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Background The KMT2A gene, formerly named the MLL gene, is rearranged (KMT2Ar) in 70–75% of infants, 5–6% of children and 10–15% of adult patients with B cell acute lymphoblastic leukemia (B-ALL). The outcome after chemotherapy of pediatric cases remains poor, and only a few studies have investigated the clinical and laboratory features, treatment response and prognosis in Chinese populations. Methods A total of 48 B-ALL children with KMT2Ar were enrolled in the study, and clinical and laboratory data were collected and analyzed by age group. The relationship between prognosis and traditional risk factors and treatment response was investigated for these patients who received chemotherapy. Results The 48 enrolled patients included 28 males and 20 females; 18 (37.50%) or 30 (62.50%) patients were an age of < 12 m (infant B-ALL) or of > 12 m at onset. An initial WBC count of 300 × 109/L was detected in 7 (14.58%) patients; testicular leukemia (TL) or central nervous system involvement was found in 5 (10.41%) or 3 (6.25%) patients, respectively. Statistical differences were not found in the age groups of sex or initial WBC count, whereas TL was more common in the infant group (P < 0.05). 11q23 was detected in 18 patients; KMT2Ar was detected in 46 (95.83%) or 45 (93.75%) patients by FISH or multiplex RT–PCR technology, respectively; RNA-seq data were obtained for 18 patients, and 3 patients with uncommon KMT2Ar were identified. KMT2A-AFF1, KMT2A-MLLT3 and KMT2A-MLLT1 were the most common transcripts. Statistical differences were not found in treatment response by age groups, including dexamethasone induction, bone marrow (BM) smear status and minimal residual disease (MRD) level at different time points (TP), treatment-related mortality (TRM), or complete remission (CR) rate (P > 0.05); MRD levels monitored by FCM or PCR were unequal at the same TP. Four patients died of treatment, and TRM was 8.33%; 40 patients achieved CR, and the CR rate for the cohort was 83.33%. Seven patients quit, 15 patients relapsed, and the 5 yr cumulative relapse rate was 59.16 ± 9.16%; the 5 yr prospective EFS (pEFS) for patients who were included or excluded from the TRM group was 36.86 ± 8.48% or 40.84 ± 9.16%, respectively. Multivariate analysis for prognosis and hazard ratio was performed for 37 patients without TRM and revealed that an initial WBC count of > 300 × 109/L and a positive level of FCM-MRD were strongly related to a poor outcome for B-ALL patients with KMT2Ar (P < 0.05).

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Section: Discussionmentioning

confidence: 99%

Poor treatment responses were related to poor outcomes in pediatric B cell acute lymphoblastic leukemia with KMT2A rearrangements

Wen¹,

Zhou

Shen

et al. 2022

BMC Cancer

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“…ALL cases, 70-80% of ALL in infants, 15-20% of childhood AML and 50% of infant AML cases. MLL-r leukemia has long been suspected to originate from an uncommitted precursor (14). MLL-r results in the fusion of the N-terminus of MLL with the C-terminus of a partner.…”

Section: Discussionmentioning

confidence: 99%

Neonatal congenital leukemia caused by several missense mutations and AFF1‑KMT2A fusion: A case report

2022

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Neonatal leukemia, a congenital form of leukemia, is a rare and fatal disease occurring in the neonatal period. Its etiology and pathogenesis have remained to be fully elucidated and the clinical manifestations differ due to age variability. Acute myeloid leukemia (AML) occurring after birth indicates genetic abnormalities and possibly intrauterine exposure to radiation, drugs or other toxins. The present report described the case of a premature neonate without phenotypic signs of Down syndrome, but with an elevated white blood cell count, mainly pertaining to the monocytes of peripheral blood. At 31 weeks of gestation, delivery by Caesarean section was performed due to fetal distress; however, the infant died three days after birth. Further laboratory examination indicated pediatric myeloid leukemia. The present case report described a case of fetal AML. According to the results of peripheral blood smear and targeted-panel sequencing, 5 missense mutations with clinical significance and a novel AFF1-KMT2A fusion gene were detected, which may be the main causes of AML and death.

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“…So, we used methylation level of GCH sites (1× depth) to define open chromatin regions (NDRs). Because of the sparse nature of single-cell genomic data, we aggregated all cells at the same stage from ICSI/ROSI-derived embryos to define NDRs as previously described ( 13 , 23 , 68 ). As reported in our previous study ( 14 ), we used a sliding window with 100-bp length at 20-bp step size to calculate the significance of difference (chi-square test, P ≤ 10 −15 ) of GCH methylation level compared to the whole genome level.…”

Section: Methodsmentioning

confidence: 99%

“…For differential methylation analysis between ROSI and ICSI embryos, we aggregated all single-cell data at each stage ( 13 , 23 , 68 ). That meant that we defined the DNA methylation level of each WCG site by the mean level of that in all single cells derived by ICSI or ROSI at the same stage, which could circumvent the variance of genomic coverage among cells to a certain extent.…”

Section: Methodsmentioning

confidence: 99%

Single-cell multiomics sequencing reveals the reprogramming defects in embryos generated by round spermatid injection

et al. 2022

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Round spermatid injection (ROSI) technique holds great promise for clinical treatment of a proportion of infertile men. However, the compromised developmental potential of ROSI embryos largely limits the clinical application, and the mechanisms are not fully understood. Here, we describe the transcriptome, chromatin accessibility, and DNA methylation landscapes of mouse ROSI embryos derived from early-stage round spermatids using a single-cell multiomics sequencing approach. By interrogating these data, we identify the reprogramming defects in ROSI embryos at the pronuclear stages, which are mainly associated with the misexpression of a cohort of minor zygotic genome activation genes. We screen a small compound, A366, that can significantly increase the developmental potential of ROSI embryos, in which A366 can partially overcome the reprogramming defects by amending the epigenetic and transcriptomic states. Collectively, our study uncovers the reprogramming defects in ROSI embryos for understanding the mechanisms underlying compromised developmental potential and offers an avenue for ROSI technique optimization.

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Single-Cell Multiomics Reveals Increased Plasticity, Resistant Populations and Stem-Cell-like Blasts in KMT2A-Rearranged Leukemia

Cited by 10 publications

References 0 publications

Poor treatment responses were related to poor outcomes in pediatric B cell acute lymphoblastic leukemia with KMT2A rearrangements

Poor treatment responses were related to poor outcomes in pediatric B cell acute lymphoblastic leukemia with KMT2A rearrangements

Neonatal congenital leukemia caused by several missense mutations and AFF1‑KMT2A fusion: A case report

Single-cell multiomics sequencing reveals the reprogramming defects in embryos generated by round spermatid injection

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