PDAM is frequently downregulated in oligodendroglial tumors and its knockdown by siRNA induces cisplatin resistance Ng Ho-Keung 吳浩強 The State Key Laboratory of Oncology in South China Department of Anatomical and Cellular Pathology The Chinese University of Hong Kong
Bigner et al., Am J Pathol, p/19q co-deletion is a genetic hallmark of oligodendroglial tumors (OTs) Frequency of 1p/19q codeletion 60-70%
Frequent 1p/19q co-deletion suggests the presence of tumor suppressor genes 1p/19q co-deletion is correlated with oligodendrogliomas with ‘classic’ histology - an adjunct marker in OT diagnosis 1p/19q co-deletion or 1p deletion alone is also associated with better survival and chemosensitivity in OT patients - first molecular marker in neuro-oncology for prognosis and chemosensitivity Investigation into the mechanism of 1p loss would provide insights into - molecular pathogenesis of OTs - mechanism underlying chemosensitivity Significance of chromosome 1p/19q co-deletion
Deletion mapping on chromosome 1p in 52 OTs 1p loss frequency : 61% Dong et al., Br J Cancer 2004
Candidate genes within the minimally deleted region on 1p36.3 ~1.2 Mb
RT-PCR analysis of candidate genes in microdissected tumors 7/12 (58%) CCDC27 LOC LOC No detectable transcripts In all samples examined / KIAA Pang et al., Brain Pathol, in press
PDAM is downregulated in OTs p= % (37 of 58) tumors showed reduced PDAM expression by >2-fold compared to normal brain, with 51% showing >10-fold decreased level
Mechanisms responsible for PDAM downregulation Allelic deletion - 24 of 37 tumors with reduced PDAM expression showed chr 1p loss (p=0.01) Epigenetic modifications
PDAM promoter is hypermethylated Reduced PDAM expression was associated with promoter hypermethylation (p=0.004)
PDAM expression is regulated by epigenetic modifications * ** * * * * * * * P<0.05
Mechanisms responsible for PDAM downregulation Of 37 cases with reduced PDAM expression: - 20 (54%) exhibited both chr 1p loss and promoter hypermethylation - 10 (27%) showed promoter hypermethylation but intact chr 1p - 3 (8%) showed 1p deletion only - 4 (11%) -- other mechanisms? Hemizygous 1p deletion and epigenetic modifications are the major mechanisms contributing to PDAM downregulation
Chr 1p loss is associated with chemosensitivity Would knockdown of PDAM render glioma cells sensitive to chemotherapeutic drugs?
Chemosensitivity assay
PDAM knockdown induces cisplatin resistance p53 WT WT Mut Mut Mut A172 U87MG
PDAM knockdown + cisplatin (DNA damage) p53 ? cisplatin resistance Why would p53-wild-type glioma cells become cisplatin- resistant when PDAM was knocked down? Cisplatin is a DNA damaging agent p53- mediated DNA damage response cell death
p53 p21 A172 U87MG Effects of PDAM knockdown and cisplatin on p53 Western blotting RT-PCR
PDAM knockdown + cisplatin (DNA damage) p53 stablization + upregulation ? cisplatin resistance DNA damage response
PDAM knockdown antagonizes apoptosis Anti-apoptosis Pro-apoptosis Cisplatin resistance A172 U87MG
BCL-xL knockdown reverses PDAM-dependent cisplatin resistance
PDAM knockdown + cisplatin (DNA damage) p53 stablization + upregulation BCL-xL upregulation + BCL2 partial derepression cisplatin resistance Anti- apoptosis PDAM may modulate apoptosis via regulation of p53-dependent anti-apoptotic genes PDAM : P53-Dependent Apoptosis Modulator
Summary A novel gene PDAM is found to be frequently downregulated, mediated through epigenetic modifications and genomic loss, in OTs. These findings suggest that PDAM plays a role in the OT development A novel mechanism for cisplatin resistance is discoverd, in which PDAM may possess the ability to modulate p53-dependent DNA damage response
The Chinese University of Hong Kong Anatomical and Cellular Pathology Ng Ho-Keung Li Ka Wai Kay Chung Yuk Fei Li Hiu Ming Yang Ling Surgery Poon Wai Sang Clinical Oncology Lui Wai Yan Vivian Grant support Research Grants Council of Hong Kong Sun Yat-sen University Neurosurgery Chen Zhong-ping Fudan University, Huashan Hospital Neurosugery Zhou Liangfu Acknowledgements
Thank you !