ABSTRACT
AIMS: The Short Course Oncology Treatment (SCOT) trial indicated that 3 months of adjuvant doublet chemotherapy was non-inferior to 6 months of treatment for patients with colorectal cancer, with considerably less toxicity. The SCOT trial results were disseminated in June 2017. The aim of this study was to understand if SCOT trial findings were implemented in Scotland. MATERIALS AND METHODS: A retrospective analysis was carried out on a dataset derived from a source population of 5.4 million people. Eligible patients were those with stage II or III colorectal cancer who received adjuvant chemotherapy. Logistic regression was applied to understand the extent of practice change to a 3-month adjuvant chemotherapy duration after the SCOT trial results were disseminated. Interrupted time series analysis was used to visualise differences in prescribing trends before and after June 2017 for the overall cohort, and by SCOT trial eligibility. RESULTS: In total, 2310 patients were included in the study; 1957 and 353 treated pre- and post-June 2017, respectively. The median treatment duration decreased from 21 weeks (interquartile range 14-24) prior to June 2017 to 12 weeks (interquartile range 12-21 weeks) after June 2017 (P < 0.001). The proportion of patients receiving over 3 months of adjuvant treatment decreased from 75% to 42% (P < 0.001). This change was most noticeable for patients who met the SCOT trial eligibility criteria, and specifically for those with low-risk stage III disease and those treated with capecitabine and oxaliplatin (CAPOX). Although practice change occurred in all locations, there were differences between regions that could be explained by pre-SCOT trial prescribing trends. DISCUSSION: A significant change in chemotherapy prescribing occurred after dissemination of the SCOT trial results. National, real-world data can be used to capture the extent of implementation of clinical trial results. In this case, implementation was aligned with clinical trial subgroup findings. This type of analysis could be conducted to evaluate the impact of other clinical trials.
Subject(s)
Colorectal Neoplasms , Fluorouracil , Antineoplastic Combined Chemotherapy Protocols/adverse effects , Capecitabine , Chemotherapy, Adjuvant/adverse effects , Colorectal Neoplasms/drug therapy , Colorectal Neoplasms/pathology , Humans , Leucovorin , Neoplasm Staging , Organoplatinum Compounds , Oxaliplatin/therapeutic use , Retrospective StudiesABSTRACT
The conversion of the plant-derived omega-3 (n-3) α-linolenic acid (ALA, 18:3n-3) to the long-chain eicosapentaenoic acid (EPA, 20:5n-3) and docosahexaenoic acid (DHA, 22:6n-3) can be increased by ALA sufficient diets compared to ALA deficient diets. Diets containing ALA above an optimal level result in no further increase in DHA levels in animals and humans. The present study evaluates means of maximizing plasma DHA accumulation by systematically varying both linoleic acid (LA, 18:2n-6) and ALA dietary level. Weanling rats were fed one of 54 diets for three weeks. The diets varied in the percentage of energy (en%) of LA (0.07-17.1 en%) and ALA (0.02-12.1 en%) by manipulating both the fat content and the balance of vegetable oils. The peak of plasma phospholipid DHA (>8% total fatty acids) was attained as a result of feeding a narrow dietary range of 1-3 en% ALA and 1-2 en% LA but was suppressed to basal levels (â¼2% total fatty acids) at dietary intakes of total polyunsaturated fatty acids (PUFA) above 3 en%. We conclude it is possible to enhance the DHA status of rats fed diets containing ALA as the only source of n-3 fatty acids but only when the level of dietary PUFA is low (<3 en%).
Subject(s)
Diet, High-Fat/adverse effects , Docosahexaenoic Acids/metabolism , Fatty Acids, Essential/metabolism , Fatty Acids, Unsaturated/administration & dosage , alpha-Linolenic Acid/metabolism , Algorithms , Animals , Diet, Fat-Restricted , Docosahexaenoic Acids/blood , Eicosapentaenoic Acid/blood , Eicosapentaenoic Acid/metabolism , Fatty Acids, Essential/blood , Fatty Acids, Essential/deficiency , Fatty Acids, Omega-6/adverse effects , Fatty Acids, Omega-6/blood , Fatty Acids, Omega-6/chemistry , Fatty Acids, Omega-6/metabolism , Fatty Acids, Unsaturated/adverse effects , Fatty Acids, Unsaturated/analysis , Fatty Acids, Unsaturated/blood , Linoleic Acid/administration & dosage , Linoleic Acid/adverse effects , Linoleic Acid/blood , Linoleic Acid/metabolism , Linseed Oil/administration & dosage , Linseed Oil/chemistry , Linseed Oil/metabolism , Male , Phospholipids/blood , Phospholipids/chemistry , Phospholipids/metabolism , Plant Oils/administration & dosage , Plant Oils/adverse effects , Plant Oils/chemistry , Plant Oils/metabolism , Rats , Rats, Wistar , Safflower Oil/administration & dosage , Safflower Oil/adverse effects , Safflower Oil/chemistry , Safflower Oil/metabolism , Sunflower Oil , Weaning , alpha-Linolenic Acid/administration & dosage , alpha-Linolenic Acid/analysis , alpha-Linolenic Acid/bloodABSTRACT
There is evidence that gastrointestinal function adapts in response to a high-fat (HF) diet. This study investigated the hypothesis that an HF diet modifies the acute effects of duodenal lipid on appetite, antropyloroduodenal pressures, plasma CCK and plasma glucagon-like peptide-1 (GLP-1) levels in humans. Twelve healthy men were studied twice in randomized, crossover fashion. The effects of a 90-min duodenal lipid infusion (6.3 kJ/min) on the above parameters were assessed immediately following 14-day periods on either an HF or a low-fat (LF) diet. After the HF diet, pyloric tonic and phasic pressures were attenuated, and the number of antropyloroduodenal pressure-wave sequences was increased when compared with the LF diet. Plasma CCK and GLP-1 levels did not differ between the two diets. Hunger was greater during the lipid infusion following the HF diet, but there was no difference in food intake. Therefore, exposure to an HF diet for 14 days attenuates the effects of duodenal lipid on antropyloroduodenal pressures and hunger without affecting food intake or plasma hormone levels.
Subject(s)
Appetite/drug effects , Diet , Dietary Fats/pharmacology , Duodenum/physiology , Gastrointestinal Motility/physiology , Hormones/blood , Adult , Cholecystokinin/blood , Dietary Fats/administration & dosage , Eating/physiology , Energy Metabolism/physiology , Glucagon/blood , Glucagon-Like Peptide 1 , Humans , Hunger/physiology , Intubation, Gastrointestinal , Male , Muscle Tonus/physiology , Peptide Fragments/blood , Protein Precursors/blood , Pylorus/physiologyABSTRACT
The ectodomains of the T cell surface glycoproteins CD4 and CD8 bind to membrane-proximal domains of MHC class II and class I molecules, respectively, while both cytoplasmic domains interact with the protein tyrosine kinase (PTK) p56lck (lck) through a shared cysteine-containing motif. Function of CD4 and CD8 requires their binding to the same MHC molecule as that recognized by the T cell antigen receptor (TCR). In vitro studies indicate that CD4-associated lck functions even in the absence of kinase activity. In vivo experiments show that, whereas helper T cell development is impaired in CD4-deficient mice, high level expression of a transgenic CD4 that cannot bind lck rescues development of this T cell subset. These studies suggest that CD4 is an adhesion molecule whose localization is regulated through protein-protein interactions of the associated PTK and whose function is to increase the stability of the TCR signalling complex by binding to the relevant MHC. The function of CD4 in development has been further studied in the context of how double positive (CD4+CD8+) thymocytes mature into either CD4+ T cells with helper function and TCR specificity for class II or into CD8+ T cells with cytotoxic function and specificity for class I. Studies using CD4-transgenic mice indicate that development of single positive T cells involves stochastic downregulation of either CD4 or CD8, coupled to activation of a cytotoxic or helper program, respectively, and subsequent selection based on the ability of the TCR and remaining co-receptor to engage the same MHC molecule.
