作者: Neftel, Cyril ; Bieback, Karen ; Kramer, Magdalena ; Wiestler, Benedikt ; Kaulfuss, Stefan ; Uhlig, Stefanie ; Burger, Michael C ; Thon, Niklas ; Friedrich, Mirco ; Alansary, Dalia ; Suvà, Mario L ; Nicolay, Brandon ; Meyer, Jochen ; Pusch, Stefan ; Preusser, Matthias ; Kilian, Michael ; Cahill, Daniel P ; Harter, Patrick N ; Weller, Michael ; Marsh, Kelly ; Habel, Antje ; Okun, Jürgen ; Breckwoldt, Michael O ; Bunse, Theresa ; Platten, Michael ; Plate, Karl H ; Dorsch, Marion ; Herold-Mende, Christel ; Sonner, Jana K ; Karcher-Bausch, Simone ; Hess-Stumpp, Holger ; Harbottle, Richard ; Steadman, Mya ; Sanghvi, Khwab ; Wick, Wolfgang ; Sahm, Felix ; Ratliff, Miriam ; Kessler, Tobias ; Turcan, Sevin ; Benner, Axel ; Al-Ali, Ruslan ; Poschet, Gernot ; von Landenberg, Anna ; von Deimling, Andreas ; Hänggi, Daniel ; Bozza, Matthias ; Eisel, Jessica ; Niemeyer, Barbara A ; Oezen, Iris ; Deumelandt, Katrin ; Bunse, Lukas ; Green, Edward ; Schrimpf, Daniel ; Zhu, Dongwei ; Berghoff, Anna S ; Nadji-Ohl, Minou

The oncometabolite (R)-2-hydroxyglutarate (R-2-HG) produced by isocitrate dehydrogenase (IDH) mutations promotes gliomagenesis via DNA and histone methylation. Here, we identify an additional activity of R-2-HG: tumor cell-derived R-2-HG is taken up by T cells where it induces a perturbation of nuclear factor of activated T cells transcriptional activity and polyamine biosynthesis, resulting in suppression of T cell activity. IDH1-mutant gliomas display reduced T cell abundance and altered calcium signaling. Antitumor immunity to experimental syngeneic IDH1-mutant tumors induced by IDH1-specific vaccine or checkpoint inhibition is improved by inhibition of the neomorphic enzymatic function of mutant IDH1. These data attribute a novel, non-tumor cell-autonomous role to an oncometabolite in shaping the tumor immune microenvironment.

Blood and lymphatic cancer : targets and therapy

<p>IDH1-mutated relapsed or refractory AML: current challenges and future prospects</p>

Review

作者: Ballesta-López, Octavio ; Montesinos, Pau ; Megías-Vericat, Juan Eduardo ; Barragán, Eva

The prognosis of patients with relapsed or refractory acute myeloid leukemia (R/R AML) is discouraging with salvage standard approaches. Mutations of isocitrate dehydrogenase 1 (IDH1 ^mut ), present in 7-14% of AML patients, have been discovered recently, opening the door to targeted agents aiming to improve the outcomes in this setting. Several oral selective IDH1 ^mut inhibitors are under investigation, ivosidenib being the first approved for R/R AML. We performed a systematic review to analyze the clinical outcomes and safety reported with IDH1 ^mut inhibitors and other agents in adult patients with IDH1 ^mut R/R AML. Ivosidenib in monotherapy achieved complete remission (CR) of 24%, overall response of 42%, and median overall survival of 9 months in R/R AML, and promising outcomes were reported with IDH305 and FT-2102. IDH1 ^mut inhibitors were generally well tolerated, but some therapy-related toxicities should be monitored, including IDH-differentiation syndrome, prolongation of the QT interval, and leukocytosis, all manageable and reversible. Also, venetoclax, CB-839, PARP inhibitors, and IDH1 peptide vaccine are being studied in IDH1^mut AML. The results of the ongoing and upcoming clinical trials will bring new evidence to establish the role of IDH1 ^mut inhibitors in therapeutic strategies of AML.

100 项与 IDH1 peptide vaccine(Deutsches Krebsforschungszentrum, Dkfz) 相关的药物交易

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