Search CORE

2 research outputs found

Alternative lengthening of telomeres in childhood neuroblastoma from genome to proteome

Author: Ambros P.
Brors B.
Feuerbach L.
Fischer M.
Gartlgruber M.
Hartlieb S.A.
Henrich K.O.
Hero B.
Herrmann C.
Ishaque N.
Jones D.T.W.
Kiesel K.
Koster J.
Nadler-Holly M.
Okonechnikov K.
Park Y.G.
Pfaff E.
Pfister S.M.
Rippe K.
Rosswog C.
Savelyeva L.
Selbach M.
Sieverling L.
Taschner-Mandl S.
Toprak U.H.
Volckmann Ri.
Wecht E.M.
Westermann F.
Witt O.
Ziehm M.
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 24/02/2021
Field of study

Telomere maintenance by telomerase activation or alternative lengthening of telomeres (ALT) is a major determinant of poor outcome in neuroblastoma. Here, we screen for ALT in primary and relapsed neuroblastomas (n = 760) and characterize its features using multi-omics profiling. ALT-positive tumors are molecularly distinct from other neuroblastoma subtypes and enriched in a population-based clinical sequencing study cohort for relapsed cases. They display reduced ATRX/DAXX complex abundance, due to either ATRX mutations (55%) or low protein expression. The heterochromatic histone mark H3K9me3 recognized by ATRX is enriched at the telomeres of ALT-positive tumors. Notably, we find a high frequency of telomeric repeat loci with a neuroblastoma ALT-specific hotspot on chr1q42.2 and loss of the adjacent chromosomal segment forming a neo-telomere. ALT-positive neuroblastomas proliferate slowly, which is reflected by a protracted clinical course of disease. Nevertheless, children with an ALT-positive neuroblastoma have dismal outcome

MDC Repository

MYCN mediates cysteine addiction and sensitizes neuroblastoma to ferroptosis

Author: Alborzinia H.
Amit I.
Bell E.
Brückner L.M.
Burhenne J.
Büttner M.
Fischer M.
Flórez A.F.
Garbowicz K.
Gartlgruber M.
Henrich K.O.
Herrmann C.
Höfer T.
Ishaque N.
Klein C.
Kreth J.
Kreth S.
Llamazares-Prada M.
Meier J.
Nadler-Holly M.
Nicke B.
Odoni D.I.
Paul F.
Poschet G.
Reiling J.H.
Schlesner M.
Selbach M.
Shaikhkarami M.
Shao C.
Stainczyk S.A.
Stresemann C.
Trumpp A.
Wecht E.M.
Westermann F.
Wölfl S.
Würth R.
Yildiz U.
Zeisberger P.
Ziehm M.
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 28/04/2022
Field of study

Aberrant expression of MYC transcription factor family members predicts poor clinical outcome in many human cancers. Oncogenic MYC profoundly alters metabolism and mediates an antioxidant response to maintain redox balance. Here we show that MYCN induces massive lipid peroxidation on depletion of cysteine, the rate-limiting amino acid for glutathione (GSH) biosynthesis, and sensitizes cells to ferroptosis, an oxidative, non-apoptotic and iron-dependent type of cell death. The high cysteine demand of MYCN-amplified childhood neuroblastoma is met by uptake and transsulfuration. When uptake is limited, cysteine usage for protein synthesis is maintained at the expense of GSH triggering ferroptosis and potentially contributing to spontaneous tumor regression in low-risk neuroblastomas. Pharmacological inhibition of both cystine uptake and transsulfuration combined with GPX4 inactivation resulted in tumor remission in an orthotopic MYCN-amplified neuroblastoma model. These findings provide a proof of concept of combining multiple ferroptosis targets as a promising therapeutic strategy for aggressive MYCN-amplified tumors

MDC Repository