Lecture 9.2 - Control of Metabolism - Exercise and Pregnancy PDF
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Aston University
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This lecture covers the control of metabolism during exercise and pregnancy. It explains the various metabolic processes involved and how the body adapts in both situations. The different fuel sources and energy requirements are highlighted.
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Exercise: ◦Humans are well adapted to exercise ◦Many physiological and biochemical processes specifically configured ◦What is needed: ‣ Ability to rapidly alter metabolic processes ‣ Consider different 'fuel mixes' to optimise O2 availability and how rapidly ener...
Exercise: ◦Humans are well adapted to exercise ◦Many physiological and biochemical processes specifically configured ◦What is needed: ‣ Ability to rapidly alter metabolic processes ‣ Consider different 'fuel mixes' to optimise O2 availability and how rapidly energy transformation is needed to generate the required amount of power Need to...: ◦Meet the acute oxygen (heart rate and respiratory rate) and metabolic fuel needs of muscles ◦Dispose of carbon dioxide and other waste products of metabolism (e.g. lactate and protons) ◦Minimise disturbances to other physiological systems Whole system response: ◦Exercise involves changes in: ‣ Musculo-skeletal system ‣ Cardiovascular system ‣ Respiratory system ‣ Temperature system ‣ Urinary system ‣ Metabolism Metabolic response to exercise: ◦Need to mobilise stored fuels ‣ At a rate to match increased activity ◦Need to preserve blood glucose levels to protect the brain ◦Magnitude and nature of response depends on: ‣ Type of exercise (muscles used) ‣ Intensity and duration of exercise ‣ Physical condition and nutritional state of individual Energy requirements of exercise: ◦Resting metabolic rate ~4 kJ/min-1 ◦100m sprint ‣ 200 kJ/min-1 ‣ 30kJ total ◦1500m race ‣ 140 kJ/min-1 ‣ 500kJ total ◦Marathon 42km ‣ 800 kJ/min-1 ‣ 10,000 kJ total Where does the energy come from?: ◦ATP required for muscle contraction ‣ Very short term stores ATP and creatine phosphate Lasts about 5 seconds ‣ ATP must rapidly be recreated by: Oxidative phosphorylation (aerobic) Anaerobic pathways (not challenging waste product of H+) ‣ Must draw on stores Fuel stores: ◦In the circulation: ‣ Glucose (12g - about 2.5 minutes of marathon) ‣ Fatty acids (4g - about 1.5 minutes of a marathon) ◦In tissue stores: ‣ Glycogen: 400-600g - about 60 min marathon (muscle) not available for release as no glucose 6- phosphatase in muscle 100-150g - in liver, supports circulating glucose as glucose 6-phosphatase is available ‣ Triacylglycerols 15kg - about 48 hour marathon Running 100m: ◦Very short, high intensity exercise ◦Cannot deliver extra oxygen to muscles in time ◦Once high energy phosphate stores used, must create ATP anaerobically ‣ Inefficient ‣ Incomplete metabolism of glucose ◦Produces lactate (lactic acid) which includes H+ ◦Cannot deliver extra glucose to muscle cells fast enough (from circulation) ◦Need muscle store of glycogen ◦Helps to spare blood glucose (needed for tissues which are unable to store glucose as glycogen e.g. brain) Muscle glycogen: ◦Available even when blood flow limited ◦No need to cross cell membranes ◦Produces glucose-6-phosphate without using ATP ◦Can be mobilised rapidly ◦Released glucose 6-P can be metabolised anaerobically ◦Lactate can be released into circulation for gluconeogenesis in liver via Cori cycle Running 1500m: ◦Moderately high intensity which is maintained over period 3-6 minutes ◦Can deliver some extra oxygen to muscles ◦Still 40% anaerobic metabolism ◦Aerobic metabolism can use fatty acids as well as glucose Fuels in exercise: Fatty acids as fuel: ◦High capacity, but: ‣ Slow release from adipose tissue ‣ Limited carrying capacity in blood ‣ Capacity limited uptake across mitochondrial membrane (carnitine shuttle) ‣ Requires more oxygen per mole ATP produced ‣ Only metabolised under anaerobic conditions Aerobic and anaerobic metabolism in exercise: ◦0-30 sec - 95% anaerobic ◦2-4 mins - 40-50% anaerobic ◦> 20 min - 95% aerobic Phases of response: ◦Initial sprint ‣ Muscle ATP and creatine phosphate ◦Long middle phase ‣ Aerobic metabolism of glucose from glycogen and fatty acids ◦Finishing sprint ‣ Anaerobic metabolism of glucose from glycogen ◦This pattern of varying creatine phosphate/anaerobic/aerobic can cycle in intermittent sports e.g. football, hockey etc. Mobilising reserves: ◦Need insulin for glucose to enter muscle (GLUT4) - although exercise may help this (increasing insulin sensitivity) ◦Glucagon stimulates glycogenolysis in liver (glycogen phosphorylase phosphorylation) ‣ Helps to maintain blood glucose ◦Adrenaline stimulates glycogenolysis in muscle (glycogen phosphorylase phosphorylation) Running a marathon: ◦Lower intensity, long duration ◦95% (at least) aerobic ◦Use of fuel molecules and stores ‣ Muscle glycogen ‣ Liver glycogen ‣ Fatty acids ◦Muscle glycogen depleted in a few minutes ◦Utilisation of glucose from liver glycogen peaks at about 1 hour ‣ Declines steadily thereafter ◦Utilisation of fatty acids rises steadily from 20-30 minutes into exercise Mobilising reserves: ◦Over a marathon: ‣ Insulin levels fall slowly (but are not stopped completely) ‣ Glucagon levels rise ‣ Adrenaline and growth hormone rise rapidly Growth hormone mobilises fatty acids (lipolysis) ‣ Cortisol rises slowly Mobilises fats Stimulates gluconeogenesis if exercise very prolonged (phosphoenolpyruvate carboxylkinase (PEPCK) and fructose 1,6 bisphosphatase) Benefits of exercise: ◦Better balance of lean tissue and fat ◦Lower blood lipids ◦Lower blood pressure ◦Improve glucose tolerance ◦Improve muscle sensitivity to insulin ◦Reduced risk of mortality, especially cardiovascular over 5 years ◦No significant effect on weight, but can aid weight maintenance Training: ◦Regular exercise produces improved exercise capacity ‣ Can lead to adaptations e.g. muscle hypertrophy ‣ Can lead to bone remodelling ◦But most aspects rapidly reversible Response to training: ◦Cardiovascular fitness ‣ Lower heart rate for a given output ◦Skeletal muscle ‣ More and bigger fibres ‣ More capillaries ‣ More myoglobin to store oxygen ‣ Better fatty acid oxidation capacity ‣ Increased glucose transport capacity ‣ Increased glycogen storage Adaptations to pregnancy: ◦Growth of foetus requires lots of: ‣ Energy ‣ Raw materials ◦Must be supplied from maternal circulation ◦Via placental exchange Placental transfer: ◦For most substances occurs by diffusion ‣ Sometimes facilitated by carrier proteins ◦Diffusion occurs down concentration gradients ◦For molecules to move into foetal blood they are usually at higher concentration in maternal than foetal blood (there is some active transport) ◦Requires reorganisation of maternal metabolism Maternal adaptations: ◦Adjust maternal blood concentrations of nutrients ◦Modify nutrient stores to cope with demands ‣ Highest in late pregnancy and during lactation ◦Affects especially fat stores ◦Increased plasma volume ◦Change in basal metabolic rate, initially increases then slows into 2nd and 3rd trimester Maternal stores: ◦Maternal weight gain 8-10kg ◦About 3kg of which is energy stores ‣ Very variable ◦Stores accumulated mostly in first 20 weeks ◦Under influence of reproductive hormones ‣ Largely from the placenta ‣ Small contribution from ovaries up to 12 weeks The aggressive parasite: ◦The foetus is adapted via the placenta to take over maternal metabolism and ensure its own survival ◦The placenta supersedes the hypothalamus-pituitary axis (HPA) Building stores - the first 20 weeks of gestation: ◦Stimulus to appetite ◦Store more fat and more glycogen ◦Due to increased action of insulin on storage tissues and decreased action of insulin on tissues which use energy ‣ More insulin ‣ But also more anti-insulins Insulin secretion in pregnancy: ◦Reproductive steroids (oestrogens and progesterone) ‣ Increase sensitivity of beta-cell to blood glucose ‣ Increase appetite, therefore more glucose ingested Specific effect on calorific foods - to support growth Beta cell response to pregnancy: ◦Hyperplasia (more cells) ◦Hypertrophy (bigger cells) ◦Increased insulin synthesis ◦Increases secretion ‣ Basal ‣ Stimulated Anti-insulins in pregnancy: ◦Ovary, then placenta secretes huge amounts of: ‣ Oestrogen (oestriol) ‣ Progesterone ‣ Human placental lactogen (hPL) ◦These are all anti-insulins in action ‣ Make muscle resistant to insulin Blood glucose in pregnancy: ◦Blood glucose levels higher on average ‣ Especially after meals ‣ Despite higher insulin levels ◦Elevated blood glucose ‣ Increases glucose gradient across placenta ‣ Drives glucose into storage tissues Adipose tissue Gestational diabetes: ◦Control of maternal metabolism in presence of ‣ Extra demand ‣ Insulin resistance ◦Depends on increased insulin secretion ◦If beta-cells do not respond normally ◦Blood glucose seriously elevated ◦Gestational diabetes ◦Affects 3-10% of pregnancies Consequences of gestational diabetes: ◦Maternal effects of hyperglycaemia ◦Excess foetal growth ‣ Macrosomia ‣ Fat baby with lots of liver and muscle glycogen ‣ Difficult delivery (shoulder dystocia) ◦Screening for gestational diabetes after 24 weeks (NICE 24-28 weeks based on risk: BMI > 30kgm-2, previous macrosomia, ethnicity, family history previous history GDM) ‣ Fasting glucose > 5.6 mmol/L or 2 hours > 7.8 mmol/L ‣ Not by HbA1c as altered haemoglobin metabolism in pregnancy, oral glucose challenge (typically in UK 75g OGTT) Testing gestational diabetes: ◦With care: ‣ Diet - dietitian led can include manage weight gain, portion control, controlled carbohydrate intake ‣ Appropriate physical activity ◦Self monitoring of glucose ◦Often use insulin short term although metformin may also be used ◦Normally corrects after delivery ◦Increased lifetime risk of developing type 2 diabetes
