Publications by authors named "Jitka Stancikova"

Background: Auer rods (AuRs) are prominent intracellular structures found almost exclusively in myeloid cell malignancies, such as acute myeloid leukemia (AML), chronic and juvenile myelomonocytic leukemia and myelodysplastic syndrome. Extremely rare AuRs have been reported in patients with acute lymphoblastic leukemia (ALL) or among ambiguous lineage leukemia patients with a dominantly lymphoblastic immunophenotype.

Procedure: We report diagnostic and follow-up data of an international cohort of 11 children suffering from leukemias with AuRs and with significant presence of T and myeloid markers, majority of whom categorized as early T-cell precursor (ETP, n = 7); or T-ALL (ETP status unknown, n = 2), ALAL (acute leukemia of ambiguous lineage, n = 1), and AML reclassified from ALAL (n = 1).

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Detailed knowledge of human B-cell development is crucial for the proper interpretation of inborn errors of immunity and malignant diseases. It is of interest to understand the kinetics of protein expression changes during development, but also to properly interpret the major and possibly alternative developmental trajectories. We have investigated human samples from healthy individuals with the aim of describing all B-cell developmental trajectories.

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  • Defective signaling of the FAS molecule, linked to autoimmune lymphoproliferative syndrome (ALPS), leads to hypergammaglobulinemia and fewer conventional memory B cells due to disrupted B cell differentiation.
  • Analysis of ALPS patients revealed low memory B cell numbers, fewer germinal center B cells, and an expanded extrafollicular B cell response, indicating a shift in B cell fate.
  • The study proposes that abnormal non-apoptotic FAS signaling affects the mTOR pathway and gene expression, contributing to the altered B cell responses observed in ALPS.
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Commensal microbiota contribute to gut homeostasis by inducing transcription of mucosal genes. Analysis of the impact of various microbiota on intestinal tissue provides an important insight into the function of this organ. We used cDNA microarrays to determine the gene expression signature of mucosa isolated from the small intestine and colon of germ-free (GF) mice and animals monoassociated with two strains.

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  • A study of 233 children with ambiguous lineage leukemia (ALAL) aimed to define treatment strategies, as previous definitions had lacked clear therapy recommendations.
  • Results showed that acute lymphoblastic leukemia (ALL)-type treatments led to a significantly higher five-year event-free survival (EFS) rate (80%) compared to acute myeloid leukemia (AML)-type treatments (36%) and combined types (50%).
  • The findings recommend using ALL-type treatment for most pediatric ALAL patients, particularly those with CD19 leukemia, while AML-type treatment is advised for a minority, and transplantation shows no overall benefit except for certain poorly responding patients.
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The regulation and stem cell origin of normal and neoplastic gastric glands are uncertain. Here, we show that Mist1 expression marks quiescent stem cells in the gastric corpus isthmus. Mist1(+) stem cells serve as a cell-of-origin for intestinal-type cancer with the combination of Kras and Apc mutation and for diffuse-type cancer with the loss of E-cadherin.

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Unlabelled: Hypermethylated in cancer 1 (HIC1) represents a prototypic tumor suppressor gene frequently inactivated by DNA methylation in many types of solid tumors. The gene encodes a sequence-specific transcriptional repressor controlling expression of several genes involved in cell cycle or stress control. In this study, a Hic1 allele was conditionally deleted, using a Cre/loxP system, to identify genes influenced by the loss of Hic1.

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Background: In previous study we showed that caspase-2 plays the role of an apical caspase in cell death induction by taxanes in breast cancer cells. This study deals with the role of other caspases. We tested breast cancer cell lines SK-BR-3 (functional caspase-3) and MCF-7 (nonfunctional caspase-3).

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  • * This study used transgenic mice to show that Nkd1 mRNA is mainly found in the intestines and liver, with elevated levels in tumors compared to healthy tissue.
  • * Analysis of human cancer samples confirmed that NKD1 is a strong marker for neoplastic growth and is linked to specific liver cancer subtypes associated with dysfunctional Wnt signaling.
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  • The Wnt signaling pathway is essential for embryonic development and adult tissue maintenance, but its abnormal activation is linked to several cancers, including those of the gastrointestinal and breast tissues.
  • This study discovered that monensin, an antibiotic, effectively inhibits Wnt signaling in various cell types and animal models, including zebrafish and Xenopus embryos.
  • Monensin also reduced β-catenin levels in colorectal cancer cells, leading to decreased expression of genes that promote cell growth and tumor progression in mice, suggesting its potential as an anticancer treatment for Wnt-related neoplasia.
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Background & Aims: The Wnt signaling pathway is required for maintenance of the intestinal epithelia; blocking this pathway reduces the proliferative capacity of the intestinal stem cells. However, aberrant Wnt signaling leads to intestinal cancer. We investigated the roles of the Wnt pathway in homeostasis of the intestinal epithelium and during malignant transformation in human cells and mice.

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