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Proteasome inhibition targets the KMT2A transcriptional complex in acute lymphoblastic leukemia
by
Seth, Aman
, Twarog, Nathaniel
, Smith, Amelia M. R.
, Cho, Ji-Hoon
, Wright, William C.
, Rubnitz, Jeffrey E.
, Gruber, Tanja A.
, Fan, Yiping
, Obeng, Esther A.
, Shelat, Anang A.
, Chen, Taosheng
, Garfinkle, Elizabeth A. R.
, Pagala, Vishwajeeth R.
, Guy, R. Kiplin
, Mitchell, Sharnise
, Koss, Cary
, Jeha, Sima
, Kamens, Jennifer L.
, Hatley, Mark E.
, Xu, Beisi
, Nance, Stephanie
, Currier, Duane
, Peng, Junmin
, Cotton, Anitria
, Choi, John K.
, Ma, Jing
, Metzger, Monika L.
, Inaba, Hiroto
, Wallace, LaShanale M.
, Nallagatla, Pratima
, Kavdia, Kanisha
, Kim, Wonil
, Lam, Jeannie W.
in
45/15
/ 45/91
/ 49/47
/ 631/67/1990/283/2125
/ 631/67/2332
/ 64/60
/ 82/58
/ Acute lymphoblastic leukemia
/ Adult
/ Babies
/ Chemotherapy
/ Child
/ Depletion
/ Drug screening
/ Gene expression
/ Histone H2B
/ Histone H3
/ Histone methyltransferase
/ Histones
/ Humanities and Social Sciences
/ Humans
/ Infant
/ Infants
/ Leukemia
/ Lymphatic leukemia
/ Lysine
/ Lysine - genetics
/ Medical prognosis
/ Methylation
/ Methyltransferase
/ MLL protein
/ multidisciplinary
/ Myeloid-Lymphoid Leukemia Protein - genetics
/ N-Methyltransferase
/ Patients
/ Pediatrics
/ Precursor Cell Lymphoblastic Leukemia-Lymphoma - drug therapy
/ Precursor Cell Lymphoblastic Leukemia-Lymphoma - genetics
/ Prognosis
/ Proteasome Endopeptidase Complex - genetics
/ Proteasomes
/ Science
/ Science (multidisciplinary)
/ Transcriptome
/ Ubiquitination
2023
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Proteasome inhibition targets the KMT2A transcriptional complex in acute lymphoblastic leukemia
by
Seth, Aman
, Twarog, Nathaniel
, Smith, Amelia M. R.
, Cho, Ji-Hoon
, Wright, William C.
, Rubnitz, Jeffrey E.
, Gruber, Tanja A.
, Fan, Yiping
, Obeng, Esther A.
, Shelat, Anang A.
, Chen, Taosheng
, Garfinkle, Elizabeth A. R.
, Pagala, Vishwajeeth R.
, Guy, R. Kiplin
, Mitchell, Sharnise
, Koss, Cary
, Jeha, Sima
, Kamens, Jennifer L.
, Hatley, Mark E.
, Xu, Beisi
, Nance, Stephanie
, Currier, Duane
, Peng, Junmin
, Cotton, Anitria
, Choi, John K.
, Ma, Jing
, Metzger, Monika L.
, Inaba, Hiroto
, Wallace, LaShanale M.
, Nallagatla, Pratima
, Kavdia, Kanisha
, Kim, Wonil
, Lam, Jeannie W.
in
45/15
/ 45/91
/ 49/47
/ 631/67/1990/283/2125
/ 631/67/2332
/ 64/60
/ 82/58
/ Acute lymphoblastic leukemia
/ Adult
/ Babies
/ Chemotherapy
/ Child
/ Depletion
/ Drug screening
/ Gene expression
/ Histone H2B
/ Histone H3
/ Histone methyltransferase
/ Histones
/ Humanities and Social Sciences
/ Humans
/ Infant
/ Infants
/ Leukemia
/ Lymphatic leukemia
/ Lysine
/ Lysine - genetics
/ Medical prognosis
/ Methylation
/ Methyltransferase
/ MLL protein
/ multidisciplinary
/ Myeloid-Lymphoid Leukemia Protein - genetics
/ N-Methyltransferase
/ Patients
/ Pediatrics
/ Precursor Cell Lymphoblastic Leukemia-Lymphoma - drug therapy
/ Precursor Cell Lymphoblastic Leukemia-Lymphoma - genetics
/ Prognosis
/ Proteasome Endopeptidase Complex - genetics
/ Proteasomes
/ Science
/ Science (multidisciplinary)
/ Transcriptome
/ Ubiquitination
2023
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Do you wish to request the book?
Proteasome inhibition targets the KMT2A transcriptional complex in acute lymphoblastic leukemia
by
Seth, Aman
, Twarog, Nathaniel
, Smith, Amelia M. R.
, Cho, Ji-Hoon
, Wright, William C.
, Rubnitz, Jeffrey E.
, Gruber, Tanja A.
, Fan, Yiping
, Obeng, Esther A.
, Shelat, Anang A.
, Chen, Taosheng
, Garfinkle, Elizabeth A. R.
, Pagala, Vishwajeeth R.
, Guy, R. Kiplin
, Mitchell, Sharnise
, Koss, Cary
, Jeha, Sima
, Kamens, Jennifer L.
, Hatley, Mark E.
, Xu, Beisi
, Nance, Stephanie
, Currier, Duane
, Peng, Junmin
, Cotton, Anitria
, Choi, John K.
, Ma, Jing
, Metzger, Monika L.
, Inaba, Hiroto
, Wallace, LaShanale M.
, Nallagatla, Pratima
, Kavdia, Kanisha
, Kim, Wonil
, Lam, Jeannie W.
in
45/15
/ 45/91
/ 49/47
/ 631/67/1990/283/2125
/ 631/67/2332
/ 64/60
/ 82/58
/ Acute lymphoblastic leukemia
/ Adult
/ Babies
/ Chemotherapy
/ Child
/ Depletion
/ Drug screening
/ Gene expression
/ Histone H2B
/ Histone H3
/ Histone methyltransferase
/ Histones
/ Humanities and Social Sciences
/ Humans
/ Infant
/ Infants
/ Leukemia
/ Lymphatic leukemia
/ Lysine
/ Lysine - genetics
/ Medical prognosis
/ Methylation
/ Methyltransferase
/ MLL protein
/ multidisciplinary
/ Myeloid-Lymphoid Leukemia Protein - genetics
/ N-Methyltransferase
/ Patients
/ Pediatrics
/ Precursor Cell Lymphoblastic Leukemia-Lymphoma - drug therapy
/ Precursor Cell Lymphoblastic Leukemia-Lymphoma - genetics
/ Prognosis
/ Proteasome Endopeptidase Complex - genetics
/ Proteasomes
/ Science
/ Science (multidisciplinary)
/ Transcriptome
/ Ubiquitination
2023
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Proteasome inhibition targets the KMT2A transcriptional complex in acute lymphoblastic leukemia
Journal Article
Proteasome inhibition targets the KMT2A transcriptional complex in acute lymphoblastic leukemia
2023
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Overview
Rearrangments in Histone-lysine-N-methyltransferase 2A (KMT2Ar) are associated with pediatric, adult and therapy-induced acute leukemias. Infants with KMT2Ar acute lymphoblastic leukemia (ALL) have a poor prognosis with an event-free-survival of 38%. Herein we evaluate 1116 FDA approved compounds in primary KMT2Ar infant ALL specimens and identify a sensitivity to proteasome inhibition. Upon exposure to this class of agents, cells demonstrate a depletion of histone H2B monoubiquitination (H2Bub1) and histone H3 lysine 79 dimethylation (H3K79me2) at KMT2A target genes in addition to a downregulation of the KMT2A gene expression signature, providing evidence that it targets the KMT2A transcriptional complex and alters the epigenome. A cohort of relapsed/refractory KMT2Ar patients treated with this approach on a compassionate basis had an overall response rate of 90%. In conclusion, we report on a high throughput drug screen in primary pediatric leukemia specimens whose results translate into clinically meaningful responses. This innovative treatment approach is now being evaluated in a multi-institutional upfront trial for infants with newly diagnosed ALL.
KMT2A rearranged infant acute lymphoblastic leukemia patients have a poor prognosis. Here, the authors use high throughput drug screening on primary infant specimens to identify a clinically active chemotherapy combination.
Publisher
Nature Publishing Group UK,Nature Publishing Group,Nature Portfolio
Subject
/ 45/91
/ 49/47
/ 64/60
/ 82/58
/ Acute lymphoblastic leukemia
/ Adult
/ Babies
/ Child
/ Histones
/ Humanities and Social Sciences
/ Humans
/ Infant
/ Infants
/ Leukemia
/ Lysine
/ Myeloid-Lymphoid Leukemia Protein - genetics
/ Patients
/ Precursor Cell Lymphoblastic Leukemia-Lymphoma - drug therapy
/ Precursor Cell Lymphoblastic Leukemia-Lymphoma - genetics
/ Proteasome Endopeptidase Complex - genetics
/ Science
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