Patterns of Intracranial Glioblastoma Recurrence After Aggressive Surgical Resection and Adjuvant Management: Retrospective Analysis of 43 Cases

Konishi, Yoshiyuki; Muragakı, Yoshihiro; Iseki, Hiroshi; Mitsuhashi, Norio; Okada, Yoshikazu

doi:10.2176/nmc.52.577

Cited by 53 publications

(42 citation statements)

References 54 publications

(86 reference statements)

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“…Glioblastoma (GBM), a grade IV astrocytoma, is the most common CNS tumor in adults. Despite aggressive standard therapy, consisting of surgery, radiation and adjuvant chemotherapy with the DNA alkylating drug temozolomide (Stupp et al , 2009), GBM invariably recur within months following initial diagnosis (Konishi et al , 2012) and typically become resistant to the first line therapy they have been exposed (Fan et al , 2010; Lomonaco et al , 2009). An SP with stem-like properties, the cancer stem cells, is one potential culprit for recurrence and therapy resistance in GBM (Chen et al , 2012; Schonberg et al , 2013).…”

Section: Introductionmentioning

confidence: 99%

EXPANDS: expanding ploidy and allele frequency on nested subpopulations

et al. 2013

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Motivation: Several cancer types consist of multiple genetically and phenotypically distinct subpopulations. The underlying mechanism for this intra-tumoral heterogeneity can be explained by the clonal evolution model, whereby growth advantageous mutations cause the expansion of cancer cell subclones. The recurrent phenotype of many cancers may be a consequence of these coexisting subpopulations responding unequally to therapies. Methods to computationally infer tumor evolution and subpopulation diversity are emerging and they hold the promise to improve the understanding of genetic and molecular determinants of recurrence.Results: To address cellular subpopulation dynamics within human tumors, we developed a bioinformatic method, EXPANDS. It estimates the proportion of cells harboring specific mutations in a tumor. By modeling cellular frequencies as probability distributions, EXPANDS predicts mutations that accumulate in a cell before its clonal expansion. We assessed the performance of EXPANDS on one whole genome sequenced breast cancer and performed SP analyses on 118 glioblastoma multiforme samples obtained from TCGA. Our results inform about the extent of subclonal diversity in primary glioblastoma, subpopulation dynamics during recurrence and provide a set of candidate genes mutated in the most well-adapted subpopulations. In summary, EXPANDS predicts tumor purity and subclonal composition from sequencing data.Availability and implementation: EXPANDS is available for download at http://code.google.com/p/expands (matlab version - used in this manuscript) and http://cran.r-project.org/web/packages/expands (R version).Contact: claudia.petritsch@ucsf.eduSupplementary information: Supplementary data are available at Bioinformatics online.

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Section: Introductionmentioning

confidence: 99%

EXPANDS: expanding ploidy and allele frequency on nested subpopulations

et al. 2013

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“…Recurrence often occurs as a local continuous growth within 2-3 cm of the lesion margin, at the original tumor site, through newly formed parenchymal lesions, or as unusual relapse patterns in midline tumors [47] . GBM recurrence after treatment occurs either from the bulk of the mass or within 20 mm of its boundary as detected by T1-weighted MR imaging (~97% of cases) [48] . Gadolinium-enhanced MR imaging, PET and MR spectroscopy are also used in surveillance of recurrent GBM [47] .…”

Section: Tumor Recurrencementioning

confidence: 99%

Insights into molecular therapy of glioma: current challenges and next generation blueprint

et al. 2017

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Glioma accounts for the majority of human brain tumors. With prevailing treatment regimens, the patients have poor survival rates. In spite of current development in mainstream glioma therapy, a cure for glioma appears to be out of reach. The infiltrative nature of glioma and acquired resistance substancially restrict the therapeutic options. Better elucidation of the complicated pathobiology of glioma and proteogenomic characterization might eventually open novel avenues for the design of more sophisticated and effective combination regimens. This could be accomplished by individually tailoring progressive neuroimaging techniques, terminating DNA synthesis with prodrug-activating genes, silencing gliomagenesis genes (gene therapy), targeting miRNA oncogenic activity (miRNAmRNA interaction), combining Hedgehog-Gli/Akt inhibitors with stem cell therapy, employing tumor lysates as antigen sources for efficient depletion of tumor-specific cancer stem cells by cytotoxic T lymphocytes (dendritic cell vaccination), adoptive transfer of chimeric antigen receptor-modified T cells, and combining immune checkpoint inhibitors with conventional therapeutic modalities. Thus, the present review captures the latest trends associated with the molecular mechanisms involved in glial tumorigenesis as well as the limitations of surgery, radiation and chemotherapy. In this article we also critically discuss the next generation molecular therapeutic strategies and their mechanisms for the successful treatment of glioma.

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“…Furthermore, glioblastoma multiforme cells are highly invasive, and the presence of even a small number of remaining cells makes post-surgical recurrence essentially universal within this patient population. 26 The residual cells that remain in the brain are supported by the existing vasculature and due …”

Section: Tissue Penetrationmentioning

confidence: 99%

Nanomedicine for drug targeting: strategies beyond the enhanced permeability and retention effect

Nehoff

Parayath

Domanovitch

et al. 2014

IJN

107

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The growing research interest in nanomedicine for the treatment of cancer and inflammatory-related pathologies is yielding encouraging results. Unfortunately, enthusiasm is tempered by the limited specificity of the enhanced permeability and retention effect. Factors such as lack of cellular specificity, low vascular density, and early release of active agents prior to reaching their target contribute to the limitations of the enhanced permeability and retention effect. However, improved nanomedicine designs are creating opportunities to overcome these problems. In this review, we present examples of the advances made in this field and endeavor to highlight the potential of these emerging technologies to improve targeting of nanomedicine to specific pathological cells and tissues.

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Patterns of Intracranial Glioblastoma Recurrence After Aggressive Surgical Resection and Adjuvant Management: Retrospective Analysis of 43 Cases

Cited by 53 publications

References 54 publications

EXPANDS: expanding ploidy and allele frequency on nested subpopulations

EXPANDS: expanding ploidy and allele frequency on nested subpopulations

Insights into molecular therapy of glioma: current challenges and next generation blueprint

Nanomedicine for drug targeting: strategies beyond the enhanced permeability and retention effect

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