Frontal Lobe Syndromes: Background
Frontal Lobe Syndromes: Background
Frontal Lobe Syndromes: Background
OVERVIEW
Background
The frontal lobe is the largest lobe in the brain, yet it is often not specifically evaluated in routine
neurologic examinations. This may in part be due to the attention to detail and rigorous testing
strategies required to probe frontal lobe functions. As successful completion of any cognitive task
considered a frontal lobe function requires multiple brain regions both within and outside the frontal
lobe, some authors prefer the term frontal systems disease. In any case, dysfunctions of the frontal
lobe can give rise to relatively specific clinical syndromes. When a patient's history suggests frontal
lobe dysfunction, detailed neurobehavioral evaluation is necessary.
Traditional classification systems divide the frontal lobes into the precentral cortex (the strip
immediately anterior to the central or Sylvian fissure) and prefrontal cortex (extending from the
frontal poles to the precentral cortex and includes the frontal operculum), which is broken into:
orbitofrontal cortex (including the orbitobasal or ventromedial and the inferior mesial regions),
ventrolateral prefrontal cortex, dorsolateral prefrontal cortex, medial prefrontal cortex (containing
the anterior cingulate gyrus, and prelimbic and infralimbic cortices), and the caudal prefrontal cortex
(which includes the frontal eye fields). Each of these areas has widespread connectivity.
Given the unique connectivity between the frontal regions and deeper brain structures, lesions of
these areas or their connections generate relatively distinctive clinical behaviors.
The dorsolateral frontal cortex is concerned with planning, strategy formation, and executive
function. Patients with dorsolateral frontal lesions tend to have apathy, personality changes,
abulia, and lack of ability to plan or to sequence actions or tasks. These patients have poor
working memory for verbal information (if the left hemisphere is predominantly affected) or
spatial information (if the right hemisphere bears the lesion brunt).
The frontal operculum contains the center for expression of language. Patients with left frontal
operculum lesions may demonstrate Broca aphasia and defective verb retrieval, whereas
patients with exclusively right opercular lesions tend to develop expressive aprosodia.
The orbitofrontal cortex is concerned with response inhibition. Patients with orbitofrontal
lesions tend to have difficulty with disinhibition, emotional lability, and memory disorders.
Patients with such acquired sociopathy, or pseudopsychopathic disorder, are said to have an
orbital personality. Personality changes from orbital damage include impulsiveness, puerility,
a jocular attitude, sexual disinhibition, and complete lack of concern for others.
Patients with lesions affecting the cingulate cortex typically develop akinetic mutism.
Patients with inferior mesial (basal forebrain) lesions tend to manifest anterograde and
Patients with inferior mesial (basal forebrain) lesions tend to manifest anterograde and
retrograde amnesia and confabulation.
Broca aphasia from a lesion in areas 44 and 45 on the left hemisphere leads to nonfluent speech,
agrammatism, paraphasias, anomia, and poor repetition. Lesions anterior, superior, and deep to
(but sparing) the Broca area produce abnormal syntax and grammar but repetition and automatic
language are preserved. This disorder is known as transcortical motor aphasia (also called
commissural dysphasia) and uninhibited echolalia is common. Memory disturbances only develop
with lesion extension into the septal nucleus of the basal forebrain. Appreciation of verbal humor is
most impaired in right frontal polar pathology.
Axial brain MRI of a patient with progressive tremorless parkinsonism and frontal-predominant dementia (Mini Mental
State Examination = 23/30; Frontal Assessment Battery = 10/18; abnormal clock drawing task and additional
constructional impairment) with moderate ideomotor apraxia. The MRI demonstrates predominantly frontal (A) and anterior
temporal atrophy (B) suggestive of frontotemporal dementia.