PURPOSE OF REVIEW: Hypomethylating agents (HMAs) are the standard of care for patients with myelodysplastic syndromes (MDS). Although these agents induce responses in up to 40% of patients, most patients ultimately experience loss of response. The purpose of this review is to provide an overview of the different therapies under development for MDS after HMA therapy. RECENT FINDINGS: Recent advances in the understanding of MDS pathogenesis have led to the development of new potential therapies after HMA failure. Newer HMAs, less susceptible to in-vivo deamination, such as guadecitabine or ASTX727 have shown activity. Alterations of immune checkpoints in MDS have led to multiple clinical trials evaluating the activity of monoclonal antibodies targeting these proteins (pembrolizumab, nivolumab, ipilimumab). Different combinations and new formulations of cytotoxic agents, such as clofarabine or CPX-351, are newer options for specific subsets of patients. Finally, targeted agents inhibiting multiple kinases (rigosertib), BCL2 (venetoclax) or mutant IDH1 (ivosidenib), IDH2 (enasidenib), FLT3 (sorafenib, midostaurin) or spliceosome components (H3B-8800) are other novel options. SUMMARY: Despite the poor prognosis associated with HMA failure, clinical trials, new cytotoxic agents and allogeneic stem-cell transplantation, can offer therapeutic opportunities for these patients for whom there is no standard of care.
PURPOSE OF REVIEW: Hypomethylating agents (HMAs) are the standard of care for patients with myelodysplastic syndromes (MDS). Although these agents induce responses in up to 40% of patients, most patients ultimately experience loss of response. The purpose of this review is to provide an overview of the different therapies under development for MDS after HMA therapy. RECENT FINDINGS: Recent advances in the understanding of MDS pathogenesis have led to the development of new potential therapies after HMA failure. Newer HMAs, less susceptible to in-vivo deamination, such as guadecitabine or ASTX727 have shown activity. Alterations of immune checkpoints in MDS have led to multiple clinical trials evaluating the activity of monoclonal antibodies targeting these proteins (pembrolizumab, nivolumab, ipilimumab). Different combinations and new formulations of cytotoxic agents, such as clofarabine or CPX-351, are newer options for specific subsets of patients. Finally, targeted agents inhibiting multiple kinases (rigosertib), BCL2 (venetoclax) or mutant IDH1 (ivosidenib), IDH2 (enasidenib), FLT3 (sorafenib, midostaurin) or spliceosome components (H3B-8800) are other novel options. SUMMARY: Despite the poor prognosis associated with HMA failure, clinical trials, new cytotoxic agents and allogeneic stem-cell transplantation, can offer therapeutic opportunities for these patients for whom there is no standard of care.
Authors: Pinkal Desai; Nuria Mencia-Trinchant; Oleksandr Savenkov; Michael S Simon; Gloria Cheang; Sangmin Lee; Michael Samuel; Ellen K Ritchie; Monica L Guzman; Karla V Ballman; Gail J Roboz; Duane C Hassane Journal: Nat Med Date: 2018-07-09 Impact factor: 53.440
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Authors: Costantine Albany; Zeeshan Fazal; Ratnakar Singh; Emmanuel Bikorimana; Nabil Adra; Nasser H Hanna; Lawrence H Einhorn; Susan M Perkins; George E Sandusky; Brock C Christensen; Harold Keer; Fang Fang; Kenneth P Nephew; Michael J Spinella Journal: Cancer Med Date: 2020-11-01 Impact factor: 4.452
Authors: Nathan Radakovich; Manja Meggendorfer; Luca Malcovati; C Beau Hilton; Mikkael A Sekeres; Jacob Shreve; Yazan Rouphail; Wencke Walter; Stephan Hutter; Anna Galli; Sara Pozzi; Chiara Elena; Eric Padron; Michael R Savona; Aaron T Gerds; Sudipto Mukherjee; Yasunobu Nagata; Rami S Komrokji; Babal K Jha; Claudia Haferlach; Jaroslaw P Maciejewski; Torsten Haferlach; Aziz Nazha Journal: Blood Adv Date: 2021-11-09
Authors: Daniel Heudobler; Sebastian Klobuch; Simone Thomas; Joachim Hahn; Wolfgang Herr; Albrecht Reichle Journal: Front Pharmacol Date: 2018-11-13 Impact factor: 5.810