Plum and posner’s diagnosis of stupor and coma fourth Edition series editor sid Gilman, md, frcp
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control behavior until the delirium clears. Drugs such as lithium and valproic acid have been used as mood stabilizers, but the underlying illness appears to be self-limited, rarely lasting more than a few weeks even without specific treat- ment; controlled trials have not been done. Subacute Diencephalic Angioencephalopathy DeGirolami and colleagues described a patient with the subacute onset of a confusional state followed by progressive dementia, obtunda- tion, and diffuse myoclonus. 443
The CSF showed a progressive rise in the protein con- centration. On postmortem examination, there were extensive destructive lesions of the thal- ami bilaterally associated with a focal vasculitis of small arteries and veins (20 to 80 microns in diameter). The vascular lesions were charac- terized by thickening of all layers of the vessel wall, with occasional scattered polymorpho- nuclear leukocytes in the wall and some col- lections of mononuclear inflammatory cells in the adventitia. Giant cells were absent. The authors were unable to find similar patients reported in the literature. The disease is so rare, and its clinical signs so nonspecific, as to make it unlikely to be diagnosed in the ante- mortem state. Since the original report, several other cases have been described. 444 In most
instances, imaging revealed patchy contrast en- hancement suggesting a brain tumor. In one instance, the diagnosis was made by biopsy prior to the patient’s death and then confirmed by autopsy. 445
Varicella-Zoster Vasculitis Herpes zoster rarely causes stupor or coma. It usually presents as a cutaneous dermatomal infection, initially with itching and pain, fol- lowed by a rash and then vesicular lesions. As many as 40% of patients with uncomplicated herpes zoster have meningitis, usually asymp- tomatic and characterized only by mild CSF pleocytosis, but sometimes accompanied by fever, headache, and stiff neck. Less commonly, herpes zoster infection may cause more profound CNS problems by caus- ing a vasculitis. 446
Pathologically, this is a viral infection of the affected cerebral blood vessels, and in immunocompetent patients, this may lead to stroke. This syndrome is especially common with ophthalmic division trigeminal zoster, and typically involves the ipsilateral ca- rotid artery. In an immunocompromised pa- tient, the infectious vasculitis may be more widespread, leading to a diffuse encephalopa- thy. The diagnosis may be difficult because neurologic features are protean 446
and the dis- ease sometimes occurs months after the cuta- neous lesions have cleared. Occasionally there is no history of a zoster rash. The MRI or cerebral angiography suggests a vasculitis. Examination Multifocal, Diffuse, and Metabolic Brain Diseases Causing Delirium, Stupor, or Coma 275
of the spinal fluid looking for a varicella-zoster DNA by PCR or by examination of zoster im- munoglobulin establishes the diagnosis. This is important because even months after the rash, antiviral therapy may be effective. 446
Behc¸et’s Syndrome Behc¸et’s syndrome is an inflammatory disease of unknown cause, the vasculopathy being largely venous. The patient can present with subacutely developing neurologic symptoms and often on examination has evidence of other systemic disease including recurrent oral ul- cerations, recurrent genital ulcerations, ante- rior or posterior uveitis, and skin lesions in- cluding erythema nodosum. 447 The disorder occurs with increased frequency along the ‘‘silk road’’ extending from Japan to the Mediterra- nean where it is coupled with an HLA-B51 haplotype. It is especially prevalent in Turkey. Neurologic symptoms have been divided into three groups: (1) primary neurologic symptoms include inflammatory disease usually of the brainstem, subacute in onset and tending to remit. Ataxia, diplopia, behavioral changes, and alterations of consciousness are relatively common. The CSF may have a pleocytosis. In fact, meningoencephalitis may be the only finding in the disorder. Characteristic imag- ing signs include inflammatory lesions of the brainstem sometimes extending into the dien- cephalon, as well as periventricular subcorti- cal white matter lesions in the hemispheres. 448
Single photon emission computed tomography (SPECT) imaging discloses areas of hypopro- fusion localized in the deep basal ganglia or in the frontal temporal cortex. 447 (2) The second neurologic syndrome, characterized by cere- bral dural venous sinus thrombosis, may lead to venous infarction. When the dural venous system is involved and there is no venous in- farct, headache is the major symptom and there may be no other neurologic signs. (3) Neuro- logic symptoms may occur as a result of intra- cranial hypertension from a superior vena cava syndrome or from cerebral emboli resulting from cardiac complications. A combination of parenchymal lesions and dural venous infarc- tion should lead to a careful search for a history of genital or oral ulceration. 449
The long-term outcome is generally fairly good with the dis- ease remitting, and in some cases, burning out. Corticosteroids often successfully treat acute episodes. 447
Cerebral Autosomal Dominant Arteriopathy With Subcortical Infarcts and Leukoencephalopathy Cerebral autosomal dominant arteriopathy with subcortical infarcts and leukoencepha- lopathy (CADASIL) is an inherited vasculo- pathy resulting from mutations of the notch-3 gene. It is characterized by recurrent ischemic episodes, cognitive deficits, behavioral disor- ders, and migraine-type headaches. Encepha- lopathy and reversible coma have been re- ported in several patients. Encephalopathy usually begins with a typical migraine head- ache. The patient may go on to develop focal signs, such as visual field defects or hemipa- resis, and then become severely encephalo- pathic, lapsing into coma. 450–452
In one series, six of 70 patients with the disorder presented with an encephalopathy originally misdiag- nosed as acute encephalitis. The patients were febrile and four had convulsions. All had a history of migraine with aura and all the epi- sodes seemed to start with an otherwise typical headache. The patients showed multiple white matter abnormalities on MRI, particularly abnormalities at the anterior temporal pole as well as the external capsule and corpus callo- sum.
450 A characteristic finding is electron- dense granules in the media of arterioles. Such granules sometimes can be identified on skin biopsy. 453
MISCELLANEOUS NEURONAL AND GLIAL DISORDERS This category includes several primary CNS disorders of diverse or unknown cause that usually culminate in stupor or coma. Most pri- mary neuronal and glial disorders cause coma only after a period of profound dementia has led the physician to the appropriate diagnosis. The disorders included below occasionally pro- duce unconsciousness sufficiently early in their course that they may be confused with other conditions described in this book. As a result, a brief discussion of their clinical picture and dif- ferential diagnosis seems warranted. Although 276 Plum and Posner’s Diagnosis of Stupor and Coma some of these diseases are caused by transmis- sible agents (e.g.,Creutzfeldt-Jakob disease, pro- gressive multifocal leukoencephalopathy), they are arbitrarily categorized separately from the encephalitides and acute toxic encephalopathies because their onset is less acute and their course not so explosive. Prion Diseases Prions are infectious proteinaceous particles (membrane glycoproteins) that, when in cer- tain conformations, can cause infectivity with- out the presence of nucleic acid. 409 Human
prion diseases include the several forms of Creutzfeldt-Jacob disease (CJD) and Gerst- mann-Strau¨ssler disease, as well as fatal famil- ial insomnia. The latter group and most cases of Gerstmann-Strau¨ssler disease and some cases of CJD are due to inherited mutations in the prion protein gene. However, most cases of CJD are sporadic. Kuru, one of the first prion disorders to be described, occurred among natives of Papua, New Guinea, who reportedly ate the brains of their relatives as part of a funeral ritual. When this practice was aban- doned, the disorder disappeared. The disorder can also be transmitted from infected tissues transplanted to uninfected individuals (iatro- genic CJD) or from the ingestion of meat from cows with bovine spongiform encephalopathy (a variant of CJD that affects primarily young people and causes early psychiatric symptoms). CJD is rare, having an incidence of between 0.5 and 1.5 cases per million people per year. CJD is a subacute disorder producing widespread neuronal degeneration and spongiform patho- logic changes in the neocortex and cerebel- lum. 409
Clinically, the illness usually affects middle- aged adults. Initial symptoms roughly are di- vided into thirds. The first third complain of fatigue, anorexia, and insomnia. The second third have behavioral or cognitive changes rap- idly progressing to dementia. The final third present with focal signs, particularly visual loss, ataxia, aphasia, and motor defects. The illness progresses over a period of weeks to months with severe obtundation, stupor, and finally unresponsiveness; 90% of patients die within 1 year and many within a matter of 6 to 8 weeks of diagnosis. The motor system suffers disproportionately with diffuse paratonic rigid- ity; decorticate posturing and extensor plantar responses develop later. Early in the course, myoclonus appears in response to startle; later the myoclonus occurs spontaneously. Some suf- fer generalized convulsions. The EEG is char- acteristic, consisting of a flat, almost isoelectric background with superimposed synchronous periodic sharp waves. The CSF examination is usually normal. A protein called 14-3-3, and particularly its gamma isoform, has been re- ported to be present in CSF from many pa- tients with CJD, 454 but both false positives and false negatives occur, 455
and a reliable and re- producible version of the test is currently un- available. The MRI may be characteristic. 456
In some patients there is bilateral symmetric hyperintensity in the caudate nucleus and pu- tamen on FLAIR and diffusion-weighted im- ages. A similar appearance of lesions in the pulvinar is also diagnostic (‘‘pulvinar sign’’). 457
Additional patients may show cortical hype- rintensity on diffusion-weighted imaging, es- pecially in the parietal and occipital regions. Unilateral or asymmetric findings are common early in the course of the disease, but eventu- ally become bilateral and more extensive. The hyperintensity on diffusion-weighted imaging is accompanied by a decrease in the apparent diffusion constant, suggesting restricted water diffusion. The MRI is both more sensitive and specific than EEG. However, when taken to- gether in the appropriate clinical setting, the disorder may be diagnosed without the need for biopsy. 458 In the final stage of the disease, all spontaneous movements cease, and the pa- tients remain in coma until they die of intercur- rent infection. The appearance of subacute dementia with myoclonic twitches in a middle-aged or elderly patient without systemic disease is highly sug- gestive of the diagnosis. Although there is a tendency to mistake the early symptoms for an involutional depression, the organic nature of the disorder rapidly becomes apparent. A sim- ilar picture is produced only by severe meta- bolic diseases (e.g., hepatic encephalopathy) or CNS syphilis (general paresis). Fatal insomnia is predominantly familial but can occur in a sporadic form. 410
The onset is disrupted sleep, including loss of sleep spindles and slow-wave sleep. Dementia, myoclonus, ataxia, dysarthria, dysphagia, and pyramidal signs follow. Hypometabolism can be demon- strated by PET in thalamic and limbic areas. Multifocal, Diffuse, and Metabolic Brain Diseases Causing Delirium, Stupor, or Coma 277
Like the changes in CJD, there is severe neu- ronal loss and astrogliosis. 410 Adrenoleukodystrophy (Schilder’s Disease) Adrenoleukodystrophy (ALD; Schilder’s dis- ease) is an X-linked disease of white matter inherited as a sex-linked recessive trait that affects male children, adolescents, and rarely adults
459,460 ; it occasionally causes coma early in its course. 461
Although Schilder originally described a similar condition in three boys, the exact diagnosis in his cases has been challenged (e.g., one may have been subacute sclerosing panencephalitis) and this eponym is now rarely used. The illness comes in two forms. The first, called pure adrenal myeloneuropathy, affects myelin in the spinal cord and, to a lesser de- gree, peripheral nerves. It also causes adrenal insufficiency in some patients. There may be abnormalities on MRS in the brain, but cere- bral symptoms do not occur. A mild version of this form is also occasionally seen in female carriers (heterozygotes) of the disease. The second form is a rapidly progressive inflam- matory myelinopathy beginning in the poste- rior hemisphere that probably results from an immune response to the very-long-chain fatty acids that accumulate in the disease. MR find- ings of demyelination in parietal and occipital areas, and the relatively acute onset, may sug- gest multiple sclerosis, but the presence of very- long-chain fatty acids in the serum establishes the diagnosis. Many patients have biochemical evidence of adrenocortical failure even in the absence of clinically apparent insufficiency. CSF protein is usually elevated and the gamma globulin is sometimes elevated. The EEG is usually slow, with focal slow and sharp abnormalities. Marchiafava-Bignami Disease Marchiafava-Bignami disease is a rare disorder of the white matter that was originally believed to affect predominantly Italian males who were heavy drinkers of red wine. It is now recog- nized, however, that the disease has no demo- graphic restriction and affects chronic alcoho- lics no matter what form of alcohol they take; most of the victims are males. 462
The essential lesion is demyelination of the corpus callosum with extension of the demyelination into the ad- jacent hemispheres. Axons may either be pre- served or destroyed, and there are an abun- dance of fatty macrophages without evidence of inflammation in the lesion. Presumably, the ultimate cause is a deficiency of some critical nutrient. About 40% of patients present with the acute onset of stupor or coma, and only half of these have prodromal cognitive or behavioral symp- toms. 462
The other 60% present with cognitive and gait dysfunction. Comatose patients may be rigid, with increased reflexes and extensor plantar responses. The diagnosis is established by MRI, with hyperintensity on FLAIR in the corpus callosum, sometimes involving only the splenium. Multiple cortical or subcortical le- sions are sometimes present as well. 463,464 About 20% of comatose patients die; the rest recover, often with residual neurologic de- fects.
462 The disease may be related to central pontine myelinolysis, which is described in Chapter 4 and which may also involve the cor- pus callosum. Gliomatosis Cerebri Gliomatosis cerebri implies diffuse infiltration of the brain by neoplastic glial cells. The term is used if three or more lobes of the brain are involved. Histologically, the tumor can be as- trocytic or oligodendroglial and can be low or high grade. 465 Gliomatosis cerebri produces symptoms that begin insidiously and progress slowly with clinical illnesses lasting from less than a month to as long as a decade or more. Mental and personality symptoms predominate with memory loss, lethargy, slowed thinking, and confusion gradually leading into sleepiness, stu- por, and often prolonged coma. Hemiparesis is fairly common, but rapidly evolving focal neu- rologic defects are rare. Less than half the pa- tients have seizures, but focal or generalized sei- zures may be the presenting complaint. About one-quarter of the patients show signs of direct brainstem involvement. Indirect evidence of increased ICP has marked the course of many cases because continued tumor growth produces simple enlargement of the brain or a narrowing of CSF fluid drainage pathways. The MR scan 278
Plum and Posner’s Diagnosis of Stupor and Coma shows either multiple or diffuse areas of high intensity on FLAIR images involving largely the white matter, but the cortex and often basal ganglia and brainstem as well. Even in the ab- sence of substantial signal abnormality, small ventricles suggest increased brain mass. Abnor- malities on the MRI are often much more dra- matic than the patient’s clinical symptoms. The hyperintense areas may or may not enhance de- pending on the grade of the lesion. Cerebral bi- opsy is necessary to make a definitive diagnosis. The following case description typifies the course and findings. Patient 5–27 A 61-year-old woman insidiously became disin- terested in her surroundings and slow in thought during the early spring of 1978. By June, she was lethargic, forgetful, apathetically incontinent, and could no longer walk unassisted. In another hospital, a ventricular shunt was placed without changing her symptoms. She gradually became mentally unresponsive and was admitted to New York Hospital in September 1978. On examination she was awake but psychologically unresponsive, reacting only to noxious stimuli with an extensor (decerebrate) response. The pupils were 2 mm in diameter, equal, and fixed to light. She had roving eye movements with a gaze preference to the right. Oculocephalic responses were full and conjugate, but caloric irrigation with cold water in the right ear produced irregular upbeat nystagmus, while irrigation in the left ear evoked irregular nystagmus to the right. She had a spastic left hemiparesis and a flaccid right hemiparesis with bilateral extensor plantar responses. Numerous laboratory tests, including examina- tion of the CSF, CT scan, and arteriogram, were either normal or nonspecifically altered. A brain biopsy taken from the grossly normal-appearing right frontal lobe gave the appearance of a diffuse gemistocytic astrocytoma with considerable vari- ation in the degree of malignant change, as well as areas of normal-looking neurons and astrocytes. The patient died in a nursing home soon afterward. Comment: The insidious onset of changes in cognition and arousal accompanied by signs of fractional damage to the midbrain (fixed pupils), pontine vestibular complex (abnormal calorics), and corticospinal systems placed the lesion dif- fusely in the brainstem and perhaps the dien- cephalon. The CT scan and other tests showed no discrete mass lesions and led to a cerebral biopsy as one of the few possible ways of making a firm diagnosis. Progressive Multifocal Leukoencephalopathy Progressive multifocal leukoencephalopathy (PML)
466 (Figure 5–12) is a subacute demye- linating disorder produced when a strain of pa- povavirus (the JC virus) infects the nervous system. The disorder occurs in patients who are immunosuppressed from AIDS, lymphoma, or- gan transplants, or various forms of chemother- apy. An outbreak occurred in patients treated with natalizumab, a selective adhesion molecule inhibitor that has been used to treat multiple sclerosis and inflammatory bowel disease. 467
The drug was removed from the market, but has been reintroduced with appropriate safety warnings. PML has rarely been reported in in- dividuals whose immune system appears intact. The neurologic symptoms are implied by the name of the disorder, a progressive asymmetric disorder of white matter with hemiparesis, vi- sual impairment, sensory abnormalities, and ataxia. Headaches and seizures are rare. The course is usually progressive over several months, terminating in coma. Rarely, there may be edema associated with the demyelinating plaques, leading to hemispheral swelling and transtentorial herniation. Patients may have focal cognitive disorders if the areas of leukoenceph- alopathy affect areas of association cortex, but do not have impairment of consciousness until late in the course. The CSF is usually normal, Yüklə 9,02 Mb. Dostları ilə paylaş:
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