In this study the effect of different fibre types was investigated on the acceptance of foods (in a short-term study) and on the nutrients' digestibility by using 10 adult, castrated cats. Peanut hull (PH, source of lignin), dried sugar beet pulp (SBP, source of hemicelluloses and pectin) and alfalfa meal (ALF, source of cellulose) were mixed to a poultry meat based cat food in 10% on dry matter (DM) basis. The average DM intake did only slightly differ according to the type of fibre added. Supplementation of basal food by dried SBP did not influence the digestibility of DM and crude protein (CP) significantly. Using ALF as a fibre source decreased the digestibility of DM (85.8% vs. 78.6%) and CP (93.8% vs. 92.0%) significantly. More severe decline could be observed in the digestibility of DM (85.8% vs. 63.4%) and CP (93.8% vs. 83.7%) when using PH as a fibre source. Fibre sources also influenced the stool DM content significantly. While application of PH increased the DM content of the faeces (45.0% vs. 49.6%), the use of dried sugar beet or ALF reduced the faecal DM content (45.0% vs. 24.1% and 39.0%, respectively). According to these results the less digestible fibre source (PH) increased the DM content of the faeces while by improving the digestibility of the fibre sources the DM content of the faeces decreased. It can be concluded, that not only the absolute fibre content of the food but also the type of fibre must be taken into account when evaluating its possible role as a component of weight loss products.
Background: Additional chromosome abnormalities (ACAs), mutations of the BCR-ABL tyrosine kinase domain (TKD) and BCR-ABL splice variants may cause resistance to first- and second-generation tyrosine kinase inhibitors (TKIs) in chronic myelogenous leukemia (CML) and Philadelphia-positive (Ph+) acute lymphoid leukemia (ALL). Methods: Karyotyping and BCR-ABL TKD mutation screening were performed in 71 imatinib-resistant CML patients and 6 Ph+ ALL patients. A total of 56 out of these 77 patients received second-generation TKI. Results: ACAs were present in 30 of 65 imatinib-resistant patients (46%). In 27 of 74 imatinib-resistant patients (36%), 15 different BCR-ABL TKD mutations were detected. Mutations were found in 25% of chronic-phase patients (12/47), 33% of accelerated-phase patients (5/15), 71% of blast crisis CML patients (5/7) and 100% of ALL patients. In nilotinib-resistant patients, Y253H, T315I and F359I/V mutations were detected; in dasatinib-resistant patients, L248M, E279K and T315I mutations were detected. T315I was found more frequently in patients on dasatinib than on imatinib therapy. The presence of ACAs predicted shorter survival during first- and second-generation TKI therapy, while TKD mutations only influenced survival during second-generation TKI therapy. Conclusion: For patients with TKI resistance, mutation and ACA screening may play a role in identifying patients with poorer prognosis.
A large number of soybean components have diverse biological activities. These include hormonal, immunological, bacteriological and digestive effects. The presently known allergens are listed. The divergence between chemical evaluation and biological value is highlighted. The following components are discussed: Kunitz inhibitor, Bowman-Birk inhibitor, saponins, soyacystatin, phytoestrogens (daidzein, glycitein, genistein), Maillard products, soybean hydrophobic protein, soy allergens, lecithin allergens, raffinose, stachyose, 2-pentyl pyridine. The studies describing the effects of the isolated components are reviewed.
Background: The germline telomerase reverse transcriptase (TERT) rs2736100_C variant was identified as a susceptibility factor for a variety of solid tumors and recently for myeloproliferative neoplasms (MPN).Methods: LightCycler melting curve analysis was applied to detect risk alleles of TERT rs2736100_C and Janus kinase 2 (JAK2) rs12343867_C tagging 46/1 haplotype in 584 BCR-ABL1-negative MPN, 308 acute, and 86 chronic myeloid leukemia (AML and CML) patients and 400 healthy individuals.Results: TERT rs2736100_C showed an increased allele frequency in BCR-ABL1-negative MPN patients compared with controls (62.7%AE2.8% vs. 48.8%AE3.5%, P < 0.0001) regardless of molecular background or disease type, but not in CML or AML. Combined TERT and JAK2 hetero-or homozygosity conferred even higher risk for classic MPN. Common complications (throm-
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