Article
Oncology
Timothy P. Hughes, Nelma Cristina D. Clementino, Mikhail Fominykh, Jeffrey H. Lipton, Anna G. Turkina, Elena Beatriz Moiraghi, Franck E. Nicolini, Naoto Takahashi, Tomasz Sacha, Dong-Wook Kim, Rafik Fellague-Chebra, Ranjan Tiwari, Catherine Bouard, Francois-Xavier Mahon
Summary: The ENESTop study demonstrated the durability and safety of treatment-free remission (TFR) in chronic myeloid leukemia patients who achieved sustained deep molecular response with nilotinib. Overall adverse event rates decreased over 5 years of TFR, but there was a cumulative increase in cardiovascular events with longer nilotinib exposure when reinitiating treatment.
Article
Oncology
Yin Wang, Wen-Jun Weng, Dun-Hua Zhou, Jian-Pei Fang, Srishti Mishra, Li Chai, Lu-Hong Xu
Summary: WT1 mutations are associated with poor prognosis in pediatric AML, especially when co-occurring with FLT3/ITD mutations. Hematopoietic stem cell transplantation may improve the prognosis of patients with WT1 mutations.
FRONTIERS IN ONCOLOGY
(2021)
Article
Multidisciplinary Sciences
Feng-Ting Dao, Jun Wang, Lu Yang, Ya-Zhen Qin
Summary: The study identified 64 immune-related differentially expressed genes (DEGs) associated with mutations in AML and developed an immune prognostic model (IPM) composed of PYCARD and PEAR1 genes, which independently predicted lower 2-year overall survival rates in AML patients. The IPM was validated in different databases and found to be associated with specific immune cell proportions and expression of checkpoint molecules in the AML cohort. The IPM derived from poor prognosis mutations in AML provides new biomarkers for patient stratification and personalized immunotherapy.
SCIENTIFIC REPORTS
(2021)
Review
Oncology
Claire Andrews, Vinod Pullarkat, Christian Recher
Summary: CPX-351, a dual-drug liposomal encapsulation of daunorubicin and cytarabine, has been approved for treating newly diagnosed therapy-related AML or AML with myelodysplasia-related changes. In clinical trials, CPX-351 significantly improved overall survival in high-risk or secondary AML patients aged 60-75 years. FLT3 gene mutations are found in approximately 30% of newly diagnosed AML patients and may have a negative impact. CPX-351 combined with FLT3 inhibitors shows promise as a treatment option for FLT3 mutation-positive AML patients.
FRONTIERS IN ONCOLOGY
(2023)
Article
Chemistry, Medicinal
Yuqi Jiang, Jie Xu, Kairui Yue, Chao Huang, Mengting Qin, Dongyu Chi, Qixin Yu, Yue Zhu, Xiaohan Hou, Tongqiang Xu, Min Li, C. James Chou, Xiaoyang Li
Summary: The study focused on modifying HDAC inhibitors to deactivate the Michael reaction in order to improve their potency. Compound 11h showed significant improvements in both HDAC inhibitory activity and cell-based antitumor assay, demonstrating potential for clinical application and efficacy against AML.
JOURNAL OF MEDICINAL CHEMISTRY
(2022)
Article
Oncology
Bryann Pardieu, Justine Pasanisi, Frank Ling, Reinaldo Dal Bello, Justine Penneroux, Angela Su, Romane Joudinaud, Laureen Chat, Hsin Chieh Wu, Matthieu Duchmann, Gaetano Sodaro, Clementine Chauvel, Florence A. Castelli, Loic Vasseur, Kim Pacchiardi, Yannis Belloucif, Marie-Charlotte Laiguillon, Eshwar Meduri, Camille Vaganay, Gabriela Alexe, Jeannig Berrou, Chaima Benaksas, Antoine Forget, Thorsten Braun, Claude Gardin, Emmanuel Raffoux, Emmanuelle Clappier, Lionel Ades, Hugues de The, Francois Fenaille, Brian J. Huntly, Kimberly Stegmaier, Herve Dombret, Nina Fenouille, Camille Lobry, Alexandre Puissant, Raphael Itzykson
Summary: By analyzing multiple AML datasets, we identified SLC7A11 as a potential gene that is essential for AML cell survival. Inhibition of SLC7A11 using genetic and chemical methods reduced the viability and clonogenic capacity of AML cell lines. Sulfasalazine, a drug with xCT inhibitory activity, showed anti-leukemic effects against primary AML samples in vitro. Inhibition of xCT affected multiple metabolic pathways, leading to depletion of glutathione pools and oxidative stress-induced cell death in leukemic cells.
Article
Medicine, General & Internal
Eric J. Duncavage, Molly C. Schroeder, Michele O'Laughlin, Roxanne Wilson, Sandra MacMillan, Andrew Bohannon, Scott Kruchowski, John Garza, Feiyu Du, Andrew E. O. Hughes, Josh Robinson, Emma Hughes, Sharon E. Heath, Jack D. Baty, Julie Neidich, Matthew J. Christopher, Meagan A. Jacoby, Geoffrey L. Uy, Robert S. Fulton, Christopher A. Miller, Jacqueline E. Payton, Daniel C. Link, Matthew J. Walter, Peter Westervelt, John F. DiPersio, Timothy J. Ley, David H. Spencer
Summary: This study showed that whole-genome sequencing provided rapid and accurate genomic profiling in patients with AML or MDS, with a greater diagnostic yield than conventional cytogenetic analysis, and more efficient risk stratification based on standard risk categories.
NEW ENGLAND JOURNAL OF MEDICINE
(2021)
Review
Oncology
Jorge Cortes, Fabian Lang
Summary: CML is driven by the BCR-ABL1 fusion protein, making the ATP binding site of ABL1 an optimal target for TKIs. Despite improvements in prognosis, patients often fail treatment and require new therapeutic options.
JOURNAL OF HEMATOLOGY & ONCOLOGY
(2021)
Article
Biochemistry & Molecular Biology
Abeer M. Al-Subaie, Balu Kamaraj
Summary: FLT3 gene mutations are common in AML cases, with mutations at the D835 residue affecting the protein's conformation and interaction with AML inhibitors. These structural changes may contribute to relapse and resistance to AML treatment, highlighting the importance of understanding FLT3 effects at the molecular level for personalized therapeutic strategies.
INTERNATIONAL JOURNAL OF MOLECULAR SCIENCES
(2021)
Review
Oncology
Rodrick Babakhanlou, Courtney DiNardo, Gautam Borthakur
Summary: Advances in the treatment of acute myeloid leukemia (AML) have been limited, but understanding the pathophysiology of the disease has led to new treatment options. Mutations in the isocitrate dehydrogenase (IDH) genes are common in AML and targeting these mutations has opened up new avenues of therapy. This review focuses on the function of IDHs, the effects of IDH2 mutations in AML, and treatment options.
LEUKEMIA & LYMPHOMA
(2023)
Review
Biochemistry & Molecular Biology
Daniela Damiani, Mario Tiribelli
Summary: The prognosis of acute myeloid leukemia (AML) is poor due to tumor cell immune escape, which weakens T-cells. Inhibiting immune checkpoints (ICs) through immune checkpoint inhibitors (ICIs) has emerged as a promising therapeutic strategy for AML. However, the results of clinical trials testing ICIs, alone or in combination with other treatments, in AML are conflicting.
Review
Oncology
Robert D. Schwab, Selina M. Luger
Summary: When considering second-line tyrosine kinase inhibitor therapy for patients with chronic myeloid leukemia, different options should be personalized based on clinical factors including treatment failure reason, patient's age and comorbidities, and BCR-ABL1 mutational profile analysis in case of inadequate response. However, there is a lack of head-to-head trial data to guide the choice of tyrosine kinase inhibitor in specific clinical settings. Each patient's treatment plan should be individualized to achieve optimal response and tolerability.
CURRENT TREATMENT OPTIONS IN ONCOLOGY
(2023)
Article
Hematology
Peng Li, Sara Brown, Margaret Williams, Thomas White, Wei Xie, Wei Cui, Deniz Peker, Li Lei, Christian A. Kunder, Huan-You Wang, Sarah S. Murray, Jennie Vagher, Tibor Kovacsovics, Jay L. Patel
Summary: The study revealed significant differences between patients with HM carrying DDX41 CV and those with VUS, including older age, male predominance, frequent co-occurrence of somatic DDX41 variants, and lower somatic mutation burden in CV patients. These findings underscore the distinct clinical entity defined by germline DDX41 variants and emphasize the need for gene-specific diagnostic and clinical management guidelines.
Review
Hematology
Hideki Makishima, Teresa V. Bowman, Lucy A. Godley
Summary: Deleterious germ line DDX41 variants are rare genetic changes that increase the risk for myeloid neoplasms and lymphoid malignancies. These variants can be inherited and are common in certain populations. They affect cellular processes related to RNA and DNA, leading to inflammation and promoting tumor development.
Article
Multidisciplinary Sciences
Golnaz Ensieh Kazemi-Sefat, Mohammad Keramatipour, Mohammad Vaezi, Seyed Mohsen Razavi, Kaveh Kavousi, Amin Talebi, Shahrbanoo Rostami, Marjan Yaghmaei, Bahram Chahardouli, Saeed Talebi, Kazem Mousavizadeh
Summary: This study identified important genetic variants in patients with myeloid blast crisis chronic myeloid leukemia (CML) using integrated genomic sequencing. These variants affect genes involved in leukemia stem cell proliferation, self-renewal, and differentiation. RNA sequencing was used to confirm these variants. This approach provides insights into the pathophysiology of CML and may aid in its management.
SCIENTIFIC REPORTS
(2022)
Article
Hematology
Caner Saygin, Gregory Roloff, Christopher N. Hahn, Rakchha Chhetri, Saar Gill, Hany Elmariah, Chetasi Talati, Emma Nunley, Guimin Gao, Aelin Kim, Michael Bishop, Satyajit Kosuri, Soma Das, Deepak Singhal, Parvathy Venugopal, Claire C. Homan, Anna Brown, Hamish S. Scott, Devendra Hiwase, Lucy A. Godley
Summary: There is growing recognition that pathogenic germ line variants play a role in the development of hematopoietic cancers. Patients with myeloid malignancies and deleterious germ line DDX41 variants have a higher incidence of severe acute GVHD. The use of posttransplant cyclophosphamide can reduce the risk of severe acute GVHD in these patients.
Review
Hematology
Claire C. Homan, Hamish S. Scott, Anna L. Brown
Summary: Hereditary platelet disorders (HPDs) are a diverse group of blood disorders with variable clinical impact. Genetic causes for these disorders are numerous, and multigene panels are being used to uncover missing heritability more efficiently. Some of these disorders also increase the risk of developing hematological malignancy (HM), and each disorder has distinct penetrance of HM and associated somatic alterations. Integrating these advances into routine clinical practice and optimizing management and surveillance of patients and carriers are the current challenges.
Letter
Hematology
Devendra Hiwase, Christopher Hahn, Elizabeth Ngoc Hoa Tran, Rakchha Chhetri, Anmol Baranwal, Aref Al-Kali, Kirsty Sharplin, Dariusz Ladon, Rachel Hollins, Patricia Greipp, Monika Kutyna, Hassan Alkhateeb, Talha Badar, Paul Wang, David M. Ross, Deepak Singhal, Naranie Shanmuganathan, Peter Bardy, Ashanka Beligaswatte, David Yeung, Mark R. Litzow, Abhishek Mangaonkar, Pratyush Giri, Cindy Lee, Angie Yong, Noemi Horvath, Nimit Singhal, Raghu Gowda, William Hogan, Naseema Gangat, Mrinal Patnaik, Kebede Begna, Ing S. Tiong, Andrew Wei, Sharad Kumar, Anna Brown, Hamish Scott, Daniel Thomas, Chung H. Kok, Ayalew Tefferi, Mithun Vinod Shah
Correction
Genetics & Heredity
Pleuntje J. van der Sluijs, Marieke Joosten, Caroline Alby, Tania Attie-Bitach, Kelly Gilmore, Christele Dubourg, Melanie Fradin, Tianyun Wang, Evangeline C. Kurtz-Nelson, Kaitlyn P. Ahlers, Peer Arts, Christopher P. Barnett, Myla Ashfaq, Anwar Baban, Myrthe van den Born, Sarah Borrie, Tiffany Busa, Alicia Byrne, Miriam Carriero, Claudia Cesario, Karen Chong, Anna Maria Cueto-Gonzalez, Jennifer C. Dempsey, Karin E. M. Diderich, Dan Doherty, Stense Farholt, Erica H. Gerkes, Svetlana Gorokhova, Lutgarde C. P. Govaerts, Pernille A. Gregersen, Scott E. Hickey, Mathilde Lefebvre, Francesca Mari, Jelena Martinovic, Hope Northrup, Melanie O'Leary, Kareesma Parbhoo, Sophie Patrier, Bernt Popp, Fernando Santos-Simarro, Corinna Stoltenburg, Christel Thauvin-Robinet, Elisabeth Thompson, Anneke T. Vulto-van Silfhout, Farah R. Zahir, Hamish S. Scott, Rachel K. Earl, Evan E. Eichler, Neeta L. Vora, Yael Wilnai, Jessica L. Giordano, Ronald J. Wapner, Jill A. Rosenfeld, Monique C. Haak, Gijs W. E. Santen
GENETICS IN MEDICINE
(2023)
Article
Hematology
Yazad D. Irani, Chung H. Kok, Jade Clarson, Naranie Shanmuganathan, Susan Branford, David T. Yeung, David M. Ross, Timothy P. Hughes, Agnes S. M. Yong
Summary: Dysregulation of immune-checkpoint receptors at diagnosis of chronic myeloid leukemia (CML) has been reported, but their role in maintaining remission after tyrosine kinase inhibitor (TKI) cessation is unclear. This study evaluated the expression of immune checkpoint receptors on T-cell subsets, regulatory T cells (T-regs), and natural killer (NK) cells in CML patients at the time of TKI cessation. The findings suggest that TIM-3 blockade may potentially improve immune response and target leukemic stem cells, providing a promising therapeutic strategy for preventing relapse after discontinuation of TKI in CML patients.
Article
Hematology
Naranie Shanmuganathan, Carol Wadham, NurHezrin Shahrin, Jinghua Feng, Daniel Thomson, Paul Wang, Verity Saunders, Chung Hoow Kok, Rob M. King, Rosalie R. Kenyon, Ming Lin, Ilaria S. Pagani, David M. Ross, Agnes S. M. Yong, Andrew P. Grigg, Anthony K. Mills, Anthony P. Schwarer, Jodi Braley, Haley Altamura, David T. Yeung, Hamish S. Scott, Andreas W. Schreiber, Timothy P. Hughes, Susan Branford
Summary: The presence of additional genetic abnormalities in chronic myeloid leukemia patients at diagnosis is associated with treatment failure and poorer response rates, despite proactive treatment intervention strategies. Incorporating genomic risk assessment into the treatment of CML is necessary.
Article
Endocrinology & Metabolism
Dominyka Batkovskyte, Fiona McKenzie, Fulya Taylan, Pelin Ozlem Simsek-Kiper, Sarah M. Nikkel, Hirofumi Ohashi, Roger E. Stevenson, Thuong Ha, Denise P. Cavalcanti, Hiroyuki Miyahara, Steven A. Skinner, Miguel A. Aguirre, Zuehal Akcoeren, Gulen Eda Utine, Tillie Chiu, Kenji Shimizu, Anna Hammarsjoe, Koray Boduroglu, Hannah W. Moore, Raymond J. Louie, Peer Arts, Allie N. Merrihew, Milena Babic, Matilda R. Jackson, Nikos Papadogiannakis, Anna Lindstrand, Ann Nordgren, Christopher P. Barnett, Hamish S. Scott, Andrei S. Chagin, Gen Nishimura, Giedre Grigelioniene
Summary: Lethal short-limb skeletal dysplasia Al-Gazali type is a rare disorder with unknown genetic etiology. A study involving nine patients with clinical features consistent with this disorder identified disease-causing variants in ADAMTSL2, shedding light on the genetic cause and highlighting the importance of analyzing the pseudogene region. This study enhances our understanding of Al-Gazali skeletal dysplasia and its association with ADAMTSL2-related disorders.
JOURNAL OF BONE AND MINERAL RESEARCH
(2023)
Article
Biochemistry & Molecular Biology
Sebastian Lunke, Sophie. E. E. Bouffler, Chirag. V. V. Patel, Sarah. A. A. Sandaradura, Meredith Wilson, Jason Pinner, Matthew. F. F. Hunter, Christopher. P. P. Barnett, Mathew Wallis, Benjamin Kamien, Tiong. Y. Y. Tan, Mary-Louise Freckmann, Belinda Chong, Dean Phelan, David Francis, Karin. S. S. Kassahn, Thuong Ha, Song Gao, Peer Arts, Matilda. R. S. R. Jackson, Hamish. S. S. Scott, Stefanie Eggers, Simone Rowley, Kirsten Boggs, Ana Rakonjac, Gemma. R. R. Brett, Michelle. G. G. de Silva, Amanda Springer, Michelle Ward, Kirsty Stallard, Cas Simons, Thomas Conway, Andreas Halman, Nicole. J. J. Van Bergen, Tim Sikora, Liana. N. N. Semcesen, David. A. A. Stroud, Alison. G. G. Compton, David. R. R. Thorburn, Katrina. M. M. Bell, Simon Sadedin, Kathryn. N. N. North, John Christodoulou, Zornitza Stark
Summary: A report from the Australian Acute Care Genomics programme demonstrates the clinical utility of integrating rapid whole-genome sequencing and multi-omic analyses in diagnosing and treating critically ill infants and children with rare diseases. Over a span of 2 years, the program provided whole-genome sequencing to 290 families and achieved a diagnostic yield of 54%. The results highlight the potential of incorporating multi-omic approaches into mainstream diagnostic practice for rare disease genomic testing.
Article
Clinical Neurology
Roula Ghaoui, Thuong T. Ha, Jennifer Kerkhof, Haley McConkey, Song Gao, Milena Babic, Rob King, Gianina Ravenscroft, Barbara Koszyca, Sophia Otto, Nigel G. Laing, Hamish Scott, Bekim Sadikovic, Karin S. Kassahn
Summary: This study reports a patient with a pathogenic variant in the DNMT3A gene who presented to the neuromuscular clinic with congenital myopathy, rhabdomyolysis, severe myalgias, and chest pain, along with phenotypic features associated with TBRS. Muscle biopsy showed minor myopathic features, and cardiac investigations revealed mildly impaired bi-ventricular systolic function. The study highlights the phenotypic overlap in patients with syndromic disorders presenting to neuromuscular clinics and the limitations of gene panels in establishing a molecular diagnosis.
NEUROMUSCULAR DISORDERS
(2023)
Article
Oncology
Mithun Vinod Shah, Elizabeth Ngoc Hoa Tran, Syed Shah, Rakchha Chhetri, Anmol Baranwal, Dariusz Ladon, Carl Shultz, Aref Al-Kali, Anna L. Brown, Dong Chen, Hamish S. Scott, Patricia Greipp, Daniel Thomas, Hassan B. Alkhateeb, Deepak Singhal, Naseema Gangat, Sharad Kumar, Mrinal M. Patnaik, Christopher N. Hahn, Chung Hoow Kok, Ayalew Tefferi, Devendra K. Hiwase
Summary: Revised diagnostic criteria for myeloid neoplasms recommended major changes regarding TP53(mut) MN, but these changes have not been specifically examined in therapy-related myeloid neoplasm (t-MN). In this study, TP53(mut) was analyzed in 488 t-MN patients and significant findings were observed. TP53(mut) t-MN with a variant allele frequency (VAF) >= 10% had distinct clinical and biological characteristics and significantly shorter survival compared to TP53(wt) cases.
BLOOD CANCER JOURNAL
(2023)
Article
Hematology
Yazad D. Irani, Amy Hughes, Chung H. Kok, Jade Clarson, David T. Yeung, David M. Ross, Susan Branford, Timothy P. Hughes, Agnes S. M. Yong
Summary: The combination of interferon and TKIs is being investigated to improve DMR and TFR rates in CP-CML patients, but the immunobiology of this combination is poorly understood. This study assessed the immunological changes in CML patients treated with nilotinib and interferon-alpha. The results showed that nilotinib+IFN temporarily reduced NK cell counts and mature NK cells, but did not affect NK cell function. IFN also increased CTL responses to LAAs and had no effect on regulatory T cells or myeloid-derived suppressor cells. The addition of IFN to nilotinib increased NK-activating receptors and CTLs responding to LAAs, and resulted in transient immune modulation.
BRITISH JOURNAL OF HAEMATOLOGY
(2023)
Correction
Biochemistry & Molecular Biology
Alicia B. Byrne, Peer Arts, Thuong T. Ha, Karin S. Kassahn, Lynn S. Paris, Anne O'Donnell-Luria, Milena Babic, Mahalia S. B. Frank, Jinghua Feng, Paul Wang, David M. Lawrence, Leila Eshraghi, Luis Arriola, John Toubia, Hung Nguyen, George McGillivray, Jason Pinner, Fiona McKenzie, Rebecca Morrow, Jill Lipsett, Nick Manton, T. Yee Khong, Lynette Moore, Jan E. Liebelt, Andreas W. Schreiber, Sarah L. King-Smith, Tristan S. E. Hardy, Matilda R. Jackson, Christopher P. Barnett, Hamish S. Scott, Broad Inst Ctr Mendelian Genomics, Genomic Autopsy Study Res Network
Article
Multidisciplinary Sciences
Zijing Zhou, Xiaonuo Ma, Yiechang Lin, Delfine Cheng, Navid Bavi, Genevieve A. Secker, Jinyuan Vero Li, Vaibhao Janbandhu, Drew L. Sutton, Hamish S. Scott, Mingxi Yao, Richard P. Harvey, Natasha L. Harvey, Ben Corry, Yixiao Zhang, Charles D. Cox
Summary: In this study, the researchers identified MDFIC and MDFI as interacting partners of the PIEZO1/2 channels. These proteins bind to the PIEZO1/2 channels and regulate their inactivation. The researchers also determined the interaction site of MDFIC in the PIEZO1 pore module using cryogenic electron microscopy, providing insights into the gating kinetics of endogenous Piezo channels and potential mechanisms involved in human lymphatic vascular disease.
Article
Oncology
Chung H. Kok, Verity A. Saunders, Phuong Dang, Naranie Shanmuganathan, Deborah White, Susan Branford, David Yeung, Timothy P. Hughes
Summary: Variability in the molecular response to frontline tyrosine kinase inhibitor therapy in chronic myeloid leukemia may be influenced by the level of kinase inhibition. A study found that patients with low levels of kinase inhibition had higher rates of early molecular response failure and lower rates of major molecular response and MR4.5 at 36 months compared to patients with high levels of inhibition. Patients with large spleens and low kinase inhibition had significantly inferior outcomes in terms of early molecular response failure, blast crisis, and event-free survival. Further studies are needed to investigate interventions in this subgroup.
BLOOD CANCER JOURNAL
(2023)
Article
Biotechnology & Applied Microbiology
Patricia J. Sullivan, Velimir Gayevskiy, Ryan L. Davis, Marie Wong, Chelsea Mayoh, Amali Mallawaarachchi, Yvonne Hort, Mark J. McCabe, Sarah Beecroft, Matilda R. Jackson, Peer Arts, Andrew Dubowsky, Nigel Laing, Marcel E. Dinger, Hamish S. Scott, Emily Oates, Mark Pinese, Mark J. Cowley
Summary: Introme is a tool that uses machine learning to comprehensively evaluate the likelihood of a variant impacting splicing by integrating predictions from multiple splice detection tools, additional splicing rules, and gene architecture features. Through extensive benchmarking, Introme outperformed other tools in detecting clinically significant splice variants.
