Single Cell Network Profiles in Non-M3 AML Associated with Patient Response to Standard Induction Therapy.

Abstract: 1582 Poster Board I-608 Background Traditional AML prognostic markers are based on clinical characterization (e.g. age) or static measurements of leukemia biology present at diagnosis, such as cytogenetics and isolated molecular events (e.g. presence of FLT3 ITD mutation). No validated methods currently exist to predict the disease response to standard AML induction chemotherapy for individual patients. Objectives: Single Cell Network Profiling… Show more

“…However, the sample set was unintentionally biased with samples predominantly from NR, female patients of younger age with intermediate cytogenetics ( Table S1 ). In spite of these limitations, univariate analysis of this sample set and an independent sample set (with 57 CR samples out of a total of 88 samples) from a separate institution revealed common nodes for CR and NR stratification suggesting that survival, DDR and apoptosis pathways may be relevant ways to characterize AML disease subtypes with further follow-up warranted in additional AML sample cohorts [28] .…”

“…Heat map of Jak/Stat signaling responses, where each row represents a specific readout and metric such as: p-Stat1 | Basal, IL-27 → p-Stat1 | Total. The samples have been ordered according to IL-27 → p-Stat3 | Total, since this node had the highest AUC and p-value for stratifying CRs from NRs [28] . Cytogenetic risk and FAB categories are noted for each sample.…”

“…It is more relevant for pathway measurements regulated by activity thresholds. For apoptosis assays, the percentage of cells that undergo cell death in response to an agent was measured with the amine aqua viability dye and with antibodies against cleaved PARP [28] .…”

“…In the AML study by Irish, although a subset of samples were identified in which potentiated p-Stat3/p-Stat5 signaling correlated with clinical refractoriness to chemotherapy, not all AML patients who were refractory to chemotherapy showed a potentiated p-Stat3/p-Stat5 signaling response, suggesting the role of alternate oncogenic pathways in their leukemia [5] . In a recent report, SCNP analysis of a separate cohort of AML samples taken at diagnosis was used to describe correlations between an expanded panel of intracellular signaling pathways with clinical response to induction therapy [28] .…”

Distinct Patterns of DNA Damage Response and Apoptosis Correlate with Jak/Stat and PI3Kinase Response Profiles in Human Acute Myelogenous Leukemia

“…However, the sample set was unintentionally biased with samples predominantly from NR, female patients of younger age with intermediate cytogenetics ( Table S1 ). In spite of these limitations, univariate analysis of this sample set and an independent sample set (with 57 CR samples out of a total of 88 samples) from a separate institution revealed common nodes for CR and NR stratification suggesting that survival, DDR and apoptosis pathways may be relevant ways to characterize AML disease subtypes with further follow-up warranted in additional AML sample cohorts [28] .…”

“…Heat map of Jak/Stat signaling responses, where each row represents a specific readout and metric such as: p-Stat1 | Basal, IL-27 → p-Stat1 | Total. The samples have been ordered according to IL-27 → p-Stat3 | Total, since this node had the highest AUC and p-value for stratifying CRs from NRs [28] . Cytogenetic risk and FAB categories are noted for each sample.…”

“…It is more relevant for pathway measurements regulated by activity thresholds. For apoptosis assays, the percentage of cells that undergo cell death in response to an agent was measured with the amine aqua viability dye and with antibodies against cleaved PARP [28] .…”

“…In the AML study by Irish, although a subset of samples were identified in which potentiated p-Stat3/p-Stat5 signaling correlated with clinical refractoriness to chemotherapy, not all AML patients who were refractory to chemotherapy showed a potentiated p-Stat3/p-Stat5 signaling response, suggesting the role of alternate oncogenic pathways in their leukemia [5] . In a recent report, SCNP analysis of a separate cohort of AML samples taken at diagnosis was used to describe correlations between an expanded panel of intracellular signaling pathways with clinical response to induction therapy [28] .…”

Distinct Patterns of DNA Damage Response and Apoptosis Correlate with Jak/Stat and PI3Kinase Response Profiles in Human Acute Myelogenous Leukemia