Book contents
- Frontmatter
- Dedication
- Contents
- List of contributors
- Editor's preface
- PART I INTRODUCTION AND GENERAL PRINCIPLES
- 1 Pathophysiology of nervous system diseases
- 2 Genetics of common neurological disorders
- 3 Repeat expansion and neurological disease
- 4 Cell birth and cell death in the central nervous system
- 5 Neuroprotection in cerebral ischemia
- 6 Promoting recovery of neurological function
- 7 Measurement of neurological outcomes
- 8 Principles of clinical neuro-epidemiology
- 9 Principles of therapeutics
- 10 Windows on the working brain: functional imaging
- 11 Windows on the working brain: magnetic resonance spectroscopy
- 12 Windows on the working brain: evoked potentials, magnetencephalography and depth recording
- PART II DISORDERS OF HIGHER FUNCTION
- PART III DISORDERS OF MOTOR CONTROL
- PART IV DISORDERS OF THE SPECIAL SENSES
- PART V DISORDERS OF SPINE AND SPINAL CORD
- PART VI DISORDERS OF BODY FUNCTION
- PART VII HEADACHE AND PAIN
- PART VIII NEUROMUSCULAR DISORDERS
- PART IX EPILEPSY
- PART X CEREBROVASCULAR DISORDERS
- PART XI NEOPLASTIC DISORDERS
- PART XII AUTOIMMUNE DISORDERS
- PART XIII DISORDERS OF MYELIN
- PART XIV INFECTIONS
- PART XV TRAUMA AND TOXIC DISORDERS
- PART XVI DEGENERATIVE DISORDERS
- PART XVII NEUROLOGICAL MANIFESTATIONS OF SYSTEMIC CONDITIONS
- Complete two-volume index
- Plate Section
2 - Genetics of common neurological disorders
from PART I - INTRODUCTION AND GENERAL PRINCIPLES
Published online by Cambridge University Press: 05 August 2016
- Frontmatter
- Dedication
- Contents
- List of contributors
- Editor's preface
- PART I INTRODUCTION AND GENERAL PRINCIPLES
- 1 Pathophysiology of nervous system diseases
- 2 Genetics of common neurological disorders
- 3 Repeat expansion and neurological disease
- 4 Cell birth and cell death in the central nervous system
- 5 Neuroprotection in cerebral ischemia
- 6 Promoting recovery of neurological function
- 7 Measurement of neurological outcomes
- 8 Principles of clinical neuro-epidemiology
- 9 Principles of therapeutics
- 10 Windows on the working brain: functional imaging
- 11 Windows on the working brain: magnetic resonance spectroscopy
- 12 Windows on the working brain: evoked potentials, magnetencephalography and depth recording
- PART II DISORDERS OF HIGHER FUNCTION
- PART III DISORDERS OF MOTOR CONTROL
- PART IV DISORDERS OF THE SPECIAL SENSES
- PART V DISORDERS OF SPINE AND SPINAL CORD
- PART VI DISORDERS OF BODY FUNCTION
- PART VII HEADACHE AND PAIN
- PART VIII NEUROMUSCULAR DISORDERS
- PART IX EPILEPSY
- PART X CEREBROVASCULAR DISORDERS
- PART XI NEOPLASTIC DISORDERS
- PART XII AUTOIMMUNE DISORDERS
- PART XIII DISORDERS OF MYELIN
- PART XIV INFECTIONS
- PART XV TRAUMA AND TOXIC DISORDERS
- PART XVI DEGENERATIVE DISORDERS
- PART XVII NEUROLOGICAL MANIFESTATIONS OF SYSTEMIC CONDITIONS
- Complete two-volume index
- Plate Section
Summary
There is growing appreciation of the influence of genetic constitution on predisposition to disease, even that not usually considered ‘genetic’. Approximately 40% of the estimated 30000 human genes are expressed in the nervous system, the majority of these exclusively (Hurko, 1997; International Human Genome Sequencing Consortium, 2001; Sutcliffe, 1988; Venter et al., 2001). Neurological and psychiatric health might thus be especially susceptible to genetic influence. Furthermore, the nervous system can be uniquely vulnerable to mutations in genes expressed ubiquitously, as with huntingtin (Trottier et al., 1995), and to primary metabolic derangements in non-neural tissue, as with hepatic porphyrias (Strand et al., 1970) or diabetes mellitus. A disproportionate number of single gene disorders manifest as neurological or psychiatric dysfunction (Hurko, 2001).
Many of the successes of human molecular genetics have come from study of neurological disease. Neurological patients suffering from monogenic disorders have thus far only benefited from improved diagnosis. Identification of pathogenic genes has provided powerful reagents, transgenic animals, lessons from homologues in lower organisms and other insights into pathophysiology. These will hasten the development of effective therapies. However, most of these benefits, both realized and anticipated, have been confined to monogenic disorders. Such single gene, or Mendelian, disorders are rare.
Complexity in single gene disorders
Furthermore, even in monogenic disorders the relationship to clinical phenotype is not always straightforward (Estivill 1996). A given phenotype can result from mutation of any of a number of genes. Genetic heterogeneity exists in early-onset Alzheimer's disease (Dartigues & Letenneur, Furthermore, even in monogenic disorders the relationship to clinical phenotype is not always straightforward (Estivill 1996). A given phenotype can result from mutation of any of a number of genes. Genetic heterogeneity exists in early-onset Alzheimer's disease (Dartigues & Letenneur, 2000), autosomal dominant spinocerebellar atrophies (Durr & Brice, 2000), limb-girdle muscular dystrophies (Beckmann, 1999; Bushby, 1999; Kissel & Mendell, 1999) and X-linked mental retardation (Toniolo & D'Adamo, 2000), among others.
Allelic heterogeneity
Different mutations within a single gene also contribute complexity. Frame-shift mutations abolish activity of dystrophin, causing Duchenne muscular dystrophy (DMD); mutations that do not shift reading frame compromise function only partially, resulting in milder Becker dystrophy or just subclinical elevation of serum creatine kinase (England et al., 1990; Matsuo et al., 1990).
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- Diseases of the Nervous SystemClinical Neuroscience and Therapeutic Principles, pp. 14 - 31Publisher: Cambridge University PressPrint publication year: 2002