Sérgio Kaiser scite author profile

Background: The expression of carcino-embryonic antigen by colorectal cancer is an example of oncogenic activation of embryonic gene expression. Hypothesizing that oncogenesis-recapitulatingontogenesis may represent a broad programmatic commitment, we compared gene expression patterns of human colorectal cancers (CRCs) and mouse colon tumor models to those of mouse colon development embryonic days 13.5-18.5.

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IV Diretriz Brasileira sobre Dislipidemias e Prevenção da Aterosclerose: Departamento de Aterosclerose da Sociedade Brasileira de Cardiologia

Spósito¹,

Caramelli²,

Fonseca³

et al. 2007

Arq. Bras. Cardiol.

393

138

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Large-Scale Molecular Comparison of Human Schwann Cells to Malignant Peripheral Nerve Sheath Tumor Cell Lines and Tissues

Miller¹,

Rangwala²,

Williams³

et al. 2006

186

198

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Malignant peripheral nerve sheath tumors (MPNST) are highly invasive soft tissue sarcomas that arise within the peripheral nerve and frequently metastasize. To identify molecular events contributing to malignant transformation in peripheral nerve, we compared eight cell lines derived from MPNSTs and seven normal human Schwann cell samples. We found that MPNST lines are heterogeneous in their in vitro growth rates and exhibit diverse alterations in expression of pRb, p53, p14Arf , and p16INK4a proteins. All MPNST cell lines express the epidermal growth factor receptor and lack S100B protein. Global gene expression profiling using Affymetrix oligonucleotide microarrays identified a 159-gene molecular signature distinguishing MPNST cell lines from normal Schwann cells, which was validated in Affymetrix microarray data generated from 45 primary MPNSTs. Expression of Schwann cell differentiation markers (SOX10, CNP, PMP22, and NGFR) was downregulated in MPNSTs whereas neural crest stem cell markers, SOX9 and TWIST1, were overexpressed in MPNSTs. Previous studies have implicated TWIST1 in apoptosis inhibition, resistance to chemotherapy, and metastasis. Reducing TWIST1 expression in MPNST cells using small interfering RNA did not affect apoptosis or chemoresistance but inhibited cell chemotaxis. Our results highlight the use of gene expression profiling in identifying genes and molecular pathways that are potential biomarkers and/or therapeutic targets for treatment of MPNST and support the use of the MPNST cell lines as a primary analytic tool. (Cancer Res 2006; 66(5): 2584-91)

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Intravenous anti–IL-13 mAb QAX576 for the treatment of eosinophilic esophagitis

Rothenberg

Wen

Greenberg

et al. 2015

Journal of Allergy and Clinical Immunology

262

182

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Updated Cardiovascular Prevention Guideline of the Brazilian Society of Cardiology - 2019

Précoma¹,

Oliveira²,

Simão³

et al. 2019

130

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Integrative genomic analyses of neurofibromatosis tumours identify SOX9 as a biomarker and survival gene

et al. 2009

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Understanding the biological pathways critical for common neurofibromatosis type 1 (NF1) peripheral nerve tumours is essential, as there is a lack of tumour biomarkers, prognostic factors and therapeutics. We used gene expression profiling to define transcriptional changes between primary normal Schwann cells (n = 10), NF1-derived primary benign neurofibroma Schwann cells (NFSCs) (n = 22), malignant peripheral nerve sheath tumour (MPNST) cell lines (n = 13), benign neurofibromas (NF) (n = 26) and MPNST (n = 6). Dermal and plexiform NFs were indistinguishable. A prominent theme in the analysis was aberrant differentiation. NFs repressed gene programs normally active in Schwann cell precursors and immature Schwann cells. MPNST signatures strongly differed; genes up-regulated in sarcomas were significantly enriched for genes activated in neural crest cells. We validated the differential expression of 82 genes including the neural crest transcription factor SOX9 and SOX9 predicted targets. SOX9 immunoreactivity was robust in NF and MPSNT tissue sections and targeting SOX9 – strongly expressed in NF1-related tumours – caused MPNST cell death. SOX9 is a biomarker of NF and MPNST, and possibly a therapeutic target in NF1.

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Capítulo 1 - Conceituação, Epidemiologia e Prevenção Primária

Malachias¹,

Souza²,

Plavnik³

et al. 2016

106

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Sérgio Kaiser

Diretrizes Brasileiras de Hipertensão Arterial – 2020

Transcriptional recapitulation and subversion of embryonic colon development by mouse colon tumor models and human colon cancer

IV Diretriz Brasileira sobre Dislipidemias e Prevenção da Aterosclerose: Departamento de Aterosclerose da Sociedade Brasileira de Cardiologia

Large-Scale Molecular Comparison of Human Schwann Cells to Malignant Peripheral Nerve Sheath Tumor Cell Lines and Tissues

Intravenous anti–IL-13 mAb QAX576 for the treatment of eosinophilic esophagitis

Updated Cardiovascular Prevention Guideline of the Brazilian Society of Cardiology - 2019

Integrative genomic analyses of neurofibromatosis tumours identify SOX9 as a biomarker and survival gene

Capítulo 1 - Conceituação, Epidemiologia e Prevenção Primária

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