A Textbook of Clinical Pharmacology and Therapeutics

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doses are used to prepare patients with acute leukaemia or aplastic anaemia for allogeneic bone marrow transplantation. Cyclophosphamide is highly effective in treating various lymphomas, leukaemias and myeloma, but also has some use in other solid tumours. It is an effective immunosuppressant (Chapter 50). Adverse effects Adverse effects are listed in Table 48.5. Pharmacokinetics Cyclophosphamide undergoes metabolic activation in the liver via CYP2B6 and chronic use autoinduces the metabolic activation to cytotoxic alkylating metabolites, the most potent of which is the short-lived phosphoramide mustard. Absorption from the gastro-intestinal tract is excellent (essentially 100% bioavailabilty). Cyclophosphamide and its metabolites are excreted in the urine. Renal excretion of one of its metabolites, acrolein, causes the haemorrhagic cystitis that accompanies high-dose therapy. MESNA (UROPROTECTION AGENT) Use Mesna (2-mercaptoethane sulphonate) is solely used to protect the urinary tract against the urotoxic metabolites of cyclophosphamide and ifosfamide. Mesna is given by intravenous injection or by mouth. Because mesna is excreted more rapidly (t1/2 is 30 minutes) than cyclophosphamide and ifosfamide, it is important that it is given at the initiation of treatment, and that the dosing interval is no more than four hours. The mesna dose and schedule vary with the dose of cyclophosphamide or ifosfamide. Urine is monitored for volume, proteinuria and haematuria. The side effects of mesna include headache, somnolence and rarely rashes. Mechanism of action Mesna protects the uro-epithelium by reacting with acrolein in the renal tubule to form a stable, non-toxic thioether. OTHER ALKYLATING AGENTS PROCARBAZINE Uses Procarbazine, a hydrazine, is a component of combination therapy for Hodgkin’s disease and brain tumours. Procarbazine is given daily by mouth. The other agent in this class is dacarbazine. Mechanism of action Procarbazine is activated in the liver by CYP450 enzymes to reactive azoxy compounds that alkylate DNA. In addition, it methylates DNA and inhibits DNA and protein synthesis. DRUGS USED IN CANCER CHEMOTHERAPY 373 Adverse effects These include the following: • dose-related haematopoietic suppression, leukopenia and thrombocytopenia at 10–14 days after treatment; • nausea and vomiting. Pharmacokinetics Procarbazine is well absorbed. The plasma t1/2 is approximately ten minutes. Procarbazine and its metabolites penetrate the blood–brain barrier. It is converted to active metabolites in the liver (see above); these are excreted by the kidneys. Drug interactions Procarbazine blocks aldehyde dehydrogenase (for comparison see disulfiram, Chapter 53) and consequently causes flushing and tachycardia if ethanol is taken concomitantly. It is also a weak monoamine oxidase inhibitor and may precipitate a hypertensive crisis with tyramine-containing foods (Chapter 20). PLATINUM COMPOUNDS CISPLATIN Uses Cisplatin is an inorganic platinum (II) co-ordination complex in which two amine (NH3) and two chlorine ligands occupy cis positions (the trans compound is inactive). Cisplatin is markedly effective for testicular malignancies and several other solid tumours, including carcinoma of the ovary, lung, head and neck, and bladder may also respond well. Cisplatin is given intravenously in combination with other cytotoxic agents. Because of the efficacy of platinum compounds and the toxicity of cisplatin, there has been a search for less toxic analogues, yielding carboplatin and oxaliplatin. The comparative pharmacology of carboplatin and oxaliplatin is summarized in Table 48.6. Mechanism of action Platinum compound cytotoxicity results from selective inhibition of tumour DNA synthesis by the formation of intra- and inter-strand cross-links at guanine residues in the nucleic acid backbone. This unwinds and shortens the DNA helix. Adverse effects These include the following: • severe nausea and vomiting; • nephrotoxicity (especially cisplatin) which is dose-related and dose-limiting. Prehydration and fluid diuresis reduce the immediate effects, but cumulative and permanent damage still occurs; • hypomagnesaemia and hypokalaemia; • ototoxicity develops in up to 30% of patients: audiometry should be carried out before, during and after treatment;
374 CANCER CHEMOTHERAPY Table 48.6: Comparative pharmacology of some platinum compounds Drug Standard dosing regimen Side effects Pharmacokinetics Additional comments Carboplatin (CBP) i.v. dose is calculated based Like cisplatin, but less Activation slower than Anti-tumour spectrum on the desired AUC by the vomiting and cisplatin t1/2 2–3 h, 60–70% similar to that of cisplatin Calvert formula nephrotoxicity. Low excreted in the urine in potential for ototoxicity and neuropathy first 24 h Oxaliplatin i.v. administration. Mild bone marrow Biotransformed in blood. Third generation Bulky DACH carrier ligand. suppression. Little Renal and tissue platinum analogue. Activity Unlike cisplatin or carboplatin nephro- or ototoxicity, elimination. Good tissue profile differs from cisplatin. cf. cisplatin but cold-induced distribution due to DACH Ovarian, colorectal, neurosensory toxicity pancreatic cancer, and mesothelioma CDDP, cisplatin; DACH, diaminocyclohexane. • myelosuppression – usually thrombocytopenia; • nervous system effects – cerebellar syndrome, peripheral neuropathy. Pharmacokinetics Cisplatin requires the replacement of the two chloride atoms with water (‘aquation’) to become active. This process takes approximately 2.5 hours. Plasma disappearance of cisplatin is multiphasic and traces of platinum are detectable in urine months after treatment. Drug interactions Additive nephrotoxicity and ototoxicity occurs with aminoglycosides or amphotericin. ANTIMETABOLITES Antimetabolites are structural analogues of, and compete with, endogenous nucleic acid precursors. Unfortunately, the pathways blocked by antimetabolites are not specific to neoplastic cells. Thus, their selectivity for malignant cells is only partial. They act in the S-phase of the cell cycle. ANTIFOLATE ANALOGUES METHOTREXATE Uses Methotrexate is curative for choriocarcinoma, also induces remission in acute lymphocytic leukaemia and is often active in breast cancer, osteogenic sarcoma and head and neck tumours. Methotrexate is also an immunosuppressant (Chapters 26 and 50) and is used to inhibit cellular proliferation in severe psoriasis (Chapter 51). There are several different dosage schedules, several of which require co-administration of folinic acid (see Figure 48.5). Mechanism of action Folic acid is required in the synthesis of thymidylate (a pyrimidine) and of purine nucleotides and thus for DNA synthesis (Figure 48.5). Methotrexate is a very slowly reversible competitive inhibitor of dihydrofolate reductase (DHFR). The affinity of DHFR for methotrexate is 100 000 times greater than that for dihydrofolate. Thus, methotrexate prevents nucleic acid synthesis and causes cell death. Folinic acid circumvents this biosynthetic block and thus non-competitively antagonizes the effect of methotrexate. Determinants of methotrexate toxicity These consist of: • a critical extracellular concentration for each target organ; • a critical duration of exposure that varies for each organ. For bone marrow and gut, the critical plasma concentration is 2 � 10 �8 M and the time factor is approximately 42 hours. Both factors must be exceeded for toxicity to occur in these organs. The severity of toxicity is proportional to the length of time for which the critical concentration is exceeded and is independent of the amount by which it is exceeded. Folinic acid rescue bypasses the dihydrofolate reductase blockade and minimizes methotrexate toxicity. Some malignant cells are less able to take up folinic acid than normal cells, thus introducing a degree of selectivity. Rescue is commenced 24 hours after methotrexate administration and continued until the plasma methotrexate concentration falls below 5 � 10 �8 M. Monitoring of the plasma methotrexate concentrations has improved the safe use of this drug and allows identification of patients at high risk of toxicity. If a patient develops severe toxicity with protracted elevation of methotrexate concentrations, methotrexate metabolism can be rapidly increased by administering an inactivating enzyme, namely carboxypeptidase-G2 (not routinely available in the UK), when methotrexate concentrations exceed 1 � 10 �7 M.
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A Textbook of Clinical Pharmacology
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A Textbook of Clinical Pharmacology
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This fifth edition is dedicated to
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FOREWORD viii PREFACE ix ACKNOWLEDG
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PREFACE Clinical pharmacology is th
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PART I GENERAL PRINCIPLES
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● Use of drugs 3 ● Adverse effe
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and acquired factors, notably disea
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100 Effect (%) 0 0 5 10 1 10 100 (a
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Dose ratio -1 100 50 The relationsh
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● Introduction 11 ● Constant-ra
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In reality, processes of eliminatio
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lood (from which samples are taken
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● Introduction 17 ● Bioavailabi
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ROUTES OF ADMINISTRATION ORAL ROUTE
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Transdermal absorption is sufficien
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FURTHER READING Fix JA. Strategies
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and thromboxanes are CYP450 enzymes
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and lorazepam. Some patients inheri
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Orally administered drug Parenteral
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● Introduction 31 ● Glomerular
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ACTIVE TUBULAR REABSORPTION This is
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DISTRIBUTION Drug distribution is a
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Detailed recommendations on dosage
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DIGOXIN Myxoedematous patients are
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● Introduction 41 ● Role of dru
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25 20 10 Life-threatening toxicity
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● Introduction 45 ● Harmful eff
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vagina in girls in their late teens
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an anti-analgesic effect when combi
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Case history A 20-year-old female m
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METABOLISM At birth, the hepatic mi
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lifelong effects as a result of tox
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DISTRIBUTION Ageing is associated w
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DIGOXIN Digoxin toxicity is common
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FURTHER READING Dhesi JK, Allain TJ
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Factors involved in the aetiology o
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analgesic. Following its release, t
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antibiotics, such as penicillin or
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predisposes to non-immune haemolysi
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● Introduction 71 ● Useful inte
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Response Therapeutic range Toxic ra
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Table 13.1: Interactions outside th
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Table 13.5: Competitive interaction
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● Introduction: ‘personalized m
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Table 14.2: Variations in drug resp
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lipoprotein (LDL) is impaired. LDL
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Key points • Genetic differences
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• Discovery • • Screening Pre
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Too many statistical comparisons pe
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ETHICS COMMITTEES Protocols for all
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Table 16.1: Recombinant proteins/en
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duration and benefit. Adenoviral ve
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● Introduction 97 ● Garlic 97
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A case report has suggested a possi
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including hypericin and pseudohyper
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PART II THE NERVOUS SYSTEM
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● Introduction 105 ● Sleep diff
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and daytime sleeping should be disc
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Key points • Insomnia and anxiety
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Box 19.1: Dopamine theory of schizo
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The Boston Collaborative Survey ind
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Oral medication, especially in liqu
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e.g. interpersonal difficulties or
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Partial response to first-line trea
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Key points Drug treatment of depres
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Case history A 45-year-old man with
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Levodopa PRINCIPLES OF TREATMENT IN
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• pulmonary, retroperitoneal and
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CHOREA The γ-aminobutyric acid con
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Cholinergic crisis Treatment of mya
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● Introduction 133 ● Mechanisms
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absolute arbiter. The availability
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Table 22.2: Metabolic interactions
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FURTHER ANTI-EPILEPTICS Other drugs
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Case history A 24-year-old woman wh
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Assessment of migraine severity and
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● General anaesthetics 145 ● In
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is the theoretical concern of a ‘
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• Respiratory system - apnoea fol
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Competitive antagonists (vecuronium
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have also proved useful in combinat
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● Introduction 155 ● Pathophysi
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ASPIRIN (ACETYLSALICYLATE) Use Anti
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Key points Drugs for mild pain •
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increases, correlating with the hig
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• If possible, use oral medicatio
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PART III THE MUSCULOSKELETAL SYSTEM
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● Introduction: inflammation 167
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Chapter 33). All NSAIDs cause wheez
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• Stomatitis suggests the possibi
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Pharmacokinetics Allopurinol is wel
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PART IV THE CARDIOVASCULAR SYSTEM
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esponsible for the strong predilect
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Ezetimibe Fat Muscle Dietary fat In
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educed). The risk of muscle damage
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Each of these classes of drug reduc
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AT 1 receptor) produce good 24-hour
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Table 28.2: Examples of calcium-cha
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Key points Drugs used in essential
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Case history A 72-year-old woman se
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Assess risk factors Investigations:
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Persistent ST segment elevation Thr
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Mechanism of action GTN works by re
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Because of the risks of haemorrhage
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Intrinsic pathway XIIa XIa the acti
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that the pharmacodynamic response i
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used with apparent benefit in acute
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The drugs that are most effective i
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therapeutic plasma concentration ca
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● Common dysrhythmias 217 ● Gen
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BASIC LIFE SUPPORT CARDIOPULMONARY
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arrest. The electrocardiogram is li
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should be given to insertion of an
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Drug interactions Amiodarone potent
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effect when treating sinus bradycar
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Case history A 24-year-old medical
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PART V THE RESPIRATORY SYSTEM
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CHAPTER 33 THERAPY OF ASTHMA, CHRON
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STEP 5: CONTINUOUS OR FREQUENT USE
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Adenylyl cyclase Table 33.1: Compar
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Drug interactions Although synergis
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use in asthma has declined consider
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α 1-antitrypsin deficiency, neutro
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PART VI THE ALIMENTARY SYSTEM
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● Peptic ulceration 247 ● Oesop
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PEPTIC ULCERATION 249 • With rega
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Ranitidine has a similar profile of
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Vestibular stimulation ? via cerebe
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cortical centres affecting vomiting
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• in hepatocellular failure to re
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Ciprofloxacin is occasionally used
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withdrawal), small doses of benzodi
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Table 34.7: Dose-independent hepato
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● Introduction 265 ● General ph
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dinucleotide (NAD) and nicotinamide
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Table 35.1: Common trace element de
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PART VII FLUIDS AND ELECTROLYTES
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● Introduction 273 ● Volume ove
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Key points Diuretics Diuretics are
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is sometimes caused by drugs, notab
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or with potassium-sparing diuretics
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Greger R, Lang F, Sebekova, Heidlan
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PART VIII THE ENDOCRINE SYSTEM
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in prefilled injection devices (‘
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Metformin should be withdrawn and i
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FURTHER READING American Diabetes A
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deficiency. Potassium iodide (3 mg
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fertility. It is contraindicated du
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● Introduction 297 ● Vitamin D
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effective in life-threatening hyper
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Further reading Block GA, Martin KJ
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Table 40.1: Actions of cortisol and
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injection may be useful, but if don
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CHAPTER 41 REPRODUCTIVE ENDOCRINOLO
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elease by the pituitary via negativ
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Treatment with depot progestogen in
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infusion using an infusion pump to
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significant proportion of men who r
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with symptoms caused by the release
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FURTHER READING Birnbaumer M. Vasop
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PART IX SELECTIVE TOXICITY
Page 334 and 335: ● Principles of antibacterial che
Page 336 and 337: 2. transfer of resistance between o
Page 338 and 339: Pharmacokinetics Absorption of thes
Page 340 and 341: Mechanism of action Macrolides bind
Page 342 and 343: asic quinolone structure dramatical
Page 344 and 345: Case history A 70-year-old man with
Page 346 and 347: PRINCIPLES OF MANAGEMENT OF MYCOBAC
Page 348 and 349: Pharmacokinetics Absorption from th
Page 350 and 351: MYCOBACTERIUM LEPRAE INFECTION Lepr
Page 352 and 353: POLYENES AMPHOTERICIN B Uses Amphot
Page 354 and 355: therapy is adequate though more fre
Page 356 and 357: NUCLEOSIDE ANALOGUES ACICLOVIR Uses
Page 358 and 359: Table 45.3: Summary of available ac
Page 360 and 361: Uses Interferon-α when combined wi
Page 362 and 363: ● Introduction 351 ● Immunopath
Page 364 and 365: Table 46.1: Examples of combination
Page 366 and 367: NON-NUCLEOSIDE ANALOGUE REVERSE TRA
Page 368 and 369: FUSION INHIBITORS Uses Currently, e
Page 370 and 371: salvage therapy include azithromyci
Page 372 and 373: ● Malaria 361 ● Trypanosomal in
Page 374 and 375: Pharmacokinetics Chloroquine is rap
Page 376 and 377: Table 47.2: Drug therapy of non-mal
Page 378 and 379: ● Introduction 367 ● Pathophysi
Page 380 and 381: Table 48.1: Classification of commo
Page 382 and 383: Polymorph count/mm 3 (a) (b) 10 000
Page 386 and 387: Adverse effects Methotrexate Inhibi
Page 388 and 389: Table 48.7: Summary of clinical pha
Page 390 and 391: Table 48.9: Summary of the clinical
Page 392 and 393: Plasma membrane Signal transduction
Page 394 and 395: Table 48.10: Monoclonal antibodies
Page 396 and 397: INTERFERON-ALFA 2B Interferon-alfa
Page 398 and 399: PART X HAEMATOLOGY
Page 400 and 401: ● Haematinics - iron, vitamin B 1
Page 402 and 403: one marrow to produce red cells. Th
Page 404 and 405: EPO Erythroid precursors Erythrocyt
Page 406 and 407: Therapeutic principles The extent o
Page 408 and 409: PART XI IMMUNOPHARMACOLOGY
Page 410 and 411: ● Introduction 399 ● Immunity a
Page 412 and 413: Key points Antigen recognition Expr
Page 414 and 415: Table 50.1: Novel anti-proliferativ
Page 416 and 417: Key points Treatment of anaphylacti
Page 418 and 419: DRUGS THAT ENHANCE IMMUNE SYSTEM FU
Page 420 and 421: PART XII THE SKIN
Page 422 and 423: ● Introduction 411 ● Acne 411
Page 424 and 425: DERMATITIS (ECZEMA) PRINCIPLES OF T
Page 426 and 427: SPECIALISTS ONLY SPECIALISTS ONLY E
Page 428 and 429: TREATMENT OF OTHER SKIN INFECTIONS
Page 430 and 431: effect of too high a dose of UVB in
Page 432 and 433: PART XIII THE EYE
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● Introduction: ocular anatomy, p
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to cause pupillary dilatation, name
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Table 52.3: Antibacterial agents us
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Table 52.6: Common drug-induced pro
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PART XIV CLINICAL TOXICOLOGY
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Table 53.2: Central nervous system
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which provide anonymized data to th
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Peak plasma levels after smoking ci
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Key points Acute effects of alcohol
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FURTHER READING Goldman D, Oroszi G
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Table 54.2: Common indications for
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Table 54.5: Antidotes and other spe
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Commission on Human Medicines (CHM)
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Note: Page numbers in italics refer
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atrial fibrillation 217, 221 digoxi
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Cushing’s syndrome 302 cyclic ade
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5-fluorouracil 375-6 fluoxetine, mo
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children 54 diazepam 108 iron prepa
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non-steroidal anti-inflammatory dru
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puberty (male), delay 314 puerperiu
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tolerance 9, 433 benzodiazepines 10
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