Publications by authors named "Jean Pierre Wery"

Engrafting the bone marrow cells of a patient with M5 acute myeloid leukemia into immunocompromised mice (AM7577) resulted in serially transferrable stable AML and eventual mortality. The disease starts in the bone marrow and then expands to peripheral areas, which is typical of M5 leukemogenesis, where high leukemic burden in blood is coincident with symptoms/mortality. The leukemic cells in the mice had myeloid morphology, phenotypes, and genotypes (including the internal tandem duplication of FMS-like tyrosine kinase receptor 3 gene [FLT3-ITD]) similar to those of the original patient.

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  • Cetuximab is an established treatment for metastatic colorectal carcinoma (mCRC) with specific KRAS mutations, but its effectiveness is being questioned, leading to the search for alternative biomarkers.
  • A study using a cetuximab mouse clinical trial dataset found that while EGFR and its ligands don't predict treatment response, a 147-gene expression signature related to the RAS pathway strongly correlates with cetuximab effectiveness.
  • The findings suggest that the RAS pathway signature could serve as a valuable predictive biomarker for colorectal cancer response to cetuximab, possibly alongside genetic mutation markers.
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The Cancer Genome Atlas (TCGA) project has generated abundant genomic data for human cancers of various histopathology types and enabled exploring cancer molecular pathology per big data approach. We developed a new algorithm based on most differentially expressed genes (DEG) per pairwise comparisons to calculate correlation coefficients to be used to quantify similarity within and between cancer types. We systematically compared TCGA cancers, demonstrating high correlation within types and low correlation between types, thus establishing molecular specificity of cancer types and an alternative diagnostic method largely equivalent to histopathology.

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Anecdote clinical observations hint that non-small cell lung cancer (NSCLC) with exon-20 insertions might respond poorly to epidermal growth factor receptor (EGFR) tyrosine kinase inhibitors (TKIs), contrasting to those with classic mutations. Lack of patient-derived experimental models has been a major hurdle for the discovery of new treatment for the diseases. We established two NSCLC-PDXs harboring two different exon-20 insertions, LU0387-adenocarcinoma (ADC) with a nine-base insertion at 2319 (H773-V774insNPH) and LU3075-squamous cell carcinoma (SCC) with a nine-base insertion at 2316 (P772-H773insDNP).

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Article Synopsis
  • Cetuximab is a treatment for metastatic colorectal cancer that typically doesn't work for patients with specific KRAS mutations, particularly at codons 12/13.
  • Recent data suggest that patients with the KRAS-G13D mutation may still benefit from cetuximab, which contradicts current treatment guidelines.
  • In a study involving 27 patient-derived xenograft models, it was found that around 30% of tumors responded to cetuximab, and the response rate for KRAS-G13D patients was similar to those without the 12/13 mutations, indicating the need for re-evaluating current patient stratification practices in cetuximab treatment.
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The HuPrime® human gastric neuroendocrine carcinoma derived xenograft model GA0087 was established in this study. GA0087 PDX model showed high gene expression of vascular endothelial growth factors (VEGF)-A and B, and high potential of lung metastasis. Circulating tumor cells (CTCs) with either large or small size, circulating tumor microemboli (CTM) and lung metastatic lesions were detected in GA0087 PDX mice.

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Article Synopsis
  • A preclinical trial found that 20% of gastric cancer patient-derived xenografts responded positively to the drug cetuximab.
  • High levels of EGFR mRNA expression and a strong immunohistochemistry score (3+) were linked to reduced tumor growth.
  • Among the responders, 50% showed EGFR amplification, indicating that certain gastric cancer subtypes with EGFR overexpression may benefit from cetuximab treatment.
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Overall benefits of EGFR-TKIs are limited because these treatments are largely only for adenocarcinoma (ADC) with EGFR activating mutation. The treatments also usually lead to development of resistances. We have established a panel of patient-derived xenografts (PDXs) from treatment naïve Asian NSCLC patients, including those containing "classic" EGFR activating mutations.

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  • The study investigates protein expression changes in melanoma to understand its progression and metastasis, focusing on potential biomarkers.
  • A total of 16 metastatic and 8 primary melanomas were analyzed using advanced proteomic techniques, identifying over 1500 proteins and highlighting 120 significant differences in protein levels.
  • The findings suggest that several differentially expressed proteins could serve as biomarkers, aiding in the understanding of tumor progression and associated biological processes.
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Platinum-based chemotherapy, such as cisplatin, is the primary treatment for ovarian cancer. However, drug resistance has become a major impediment to the successful treatment of ovarian cancer. To date, the molecular mechanisms of resistance to platinum-based chemotherapy remain unclear.

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