H. M.'s Medial Temporal Lobe Lesion: Findings from Magnetic Resonance Imaging

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Volume 17, Number 10, Issue of May 15, 1997 pp. 3964-3979
Copyright ©1997 Society for Neuroscience

H. M.'s Medial Temporal Lobe Lesion: Findings from Magnetic Resonance Imaging

Suzanne Corkin¹, David G. Amaral², R. Gilberto González³, Keith A. Johnson⁴, and Bradley T. Hyman⁵
¹ Department of Brain and Cognitive Sciences and the Clinical Research Center, Massachusetts Institute of Technology, Cambridge, Massachusetts 02139, ² Department of Psychiatry and Center for Neuroscience, University of California, Davis, Davis, California 95616, ³ Nuclear Magnetic Resonance Center and Neuroradiology Section, Massachusetts General Hospital, Harvard Medical School, Boston, Massachusetts 02114, ⁴ Departments of Neurology and Radiology, Brigham and Women's Hospital, Harvard Medical School, Boston, Massachusetts 02115, and ⁵ Department of Neurology, Massachusetts General Hospital, Harvard Medical School, Boston, Massachusetts 02114

ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
FOOTNOTES
REFERENCES

ABSTRACT

Although neuropsychological studies of the amnesic patient H. M. provide compelling evidence that normal memory function dependson the medial temporal lobe, the full extent of his surgical resectionhas not been elucidated. We conducted magnetic resonance imagingstudies to specify precisely the extent of his bilateral resectionand to document any other brain abnormalities. The MRI studiesindicated that the lesion was bilaterally symmetrical and includedthe medial temporal polar cortex, most of the amygdaloid complex,most or all of the entorhinal cortex, and approximately half ofthe rostrocaudal extent of the intraventricular portion of thehippocampal formation (dentate gyrus, hippocampus, and subicularcomplex). The collateral sulcus was visible throughout much ofthe temporal lobe, indicating that portions of the ventral perirhinalcortex, located on the banks of the sulcus, were spared; the parahippocampalcortex (areas TF and TH) was largely intact. The rostrocaudalextent of the ablation was ~5.4 cm (left) and 5.1 cm (right).The caudal 2 cm, approximately, of the hippocampus body (normallength, ~4 cm) was intact, although atrophic. The temporal stemwas intact. Outside the temporal lobes, the cerebellum demonstratedmarked atrophy, and the mammillary nuclei were shrunken. The lateraltemporal, frontal, parietal, and occipital lobe cortices appearednormal for age 66 years. The mediodorsal thalamic nuclei showedno obvious radiological changes. These findings reinforce theview that lesions of the hippocampal formation and adjacent corticalstructures can produce global and enduring amnesia and can exacerbateamnesia beyond that seen after more selective hippocampal lesions.
Key words: amnesia; medial temporal lobe; human; explicit/declarative memory; MRI; epilepsy surgery; H. M.

INTRODUCTION

At the 1953 meeting of the Harvey Cushing Society, Scoville (1954) discussed two patients (one epileptic, H. M., and the otherschizophrenic) in whom he had performed "bilateral resection ofthe entire (pyriform-amygdaloid-hippocampal) complex includingthe hippocampal gyrus extending posteriorly for a length of 8-9cm from the tips of the temporal lobes." He reported that bothpatients experienced "a very grave, recent memory loss" (p 65).Independent of Scoville's report, Milner and Penfield (1955) documenteda similar impairment in two patients after left temporal lobectomy.At autopsy, one of them had a substantial lesion in the righthippocampal formation (Penfield and Mathieson, 1974); the otherwas presumed (based on electroencephalography and the presenceof automatism) (Feindel and Penfield, 1954; Penfield and Milner,1958) to have a preoperatively unsuspected lesion in the rightmedial temporal lobe. Scoville realized his patients' importancefor the understanding of human memory mechanisms, and when helearned of Penfield and Milner's findings, he invited them toexamine his patients. The resulting paper (Scoville and Milner,1957) described the findings for nine schizophrenic patients andH. M. Based on analyses of patients with three different typesof medial temporal lobe ablations compromising various rostrocaudalamounts of the intraventricular portion of the hippocampal formation,the authors concluded that the severity of the memory impairmentwas related to the extent of resection of the hippocampus andparahippocampal gyrus bilaterally. The severe and lasting anterogradeamnesia was in sharp contrast to their preserved early memoriesand overall intelligence.

The significance of this paper (Scoville and Milner, 1957) was fourfold: (1) it informed neurosurgeons that a bilateral lesionof medial temporal lobe structures placed recent memory functionsat risk; (2) it suggested that the establishment of memory hada distinct neural substrate; memory for new experiences was disturbed,but other cognitive functions and sensory capacities were unimpaired;(3) it inaugurated 4 decades of experimental studies of H. M.(Milner et al., 1968; Corkin, 1984); and (4) it inspired animalmodels of human amnesia (Correll and Scoville, 1965). The animalmodels, together with the human studies, demonstrate that medialtemporal lobe structures are critical for establishing long-termexplicit/declarative memory (Squire, 1992).

Because previous imaging studies of H. M. did not reveal the precise extent of his temporal lobe lesion (Corkin, 1984), hypothesesconcerning the neuroanatomical substrate of his amnesia have beenbased on Scoville's surgical report. This uncertainty has promptedspeculation (Horel, 1978) that lesions in structures other thanthe hippocampal formation may explain the memory impairment. Moreover,recent studies in animal models of human amnesia have raised questionsabout which temporal lobe structures included within the ablationin H. M. contribute to normal memory function (Mishkin and Murray,1994). For example, the perirhinal cortex has been shown to bean important component of the medial temporal lobe memory systemin the monkey (Zola-Morgan et al., 1989c, 1993; Meunier et al.,1993; Suzuki et al., 1993), but it is currently unclear to whatextent this region is damaged in H. M. The present study usedmagnetic resonance imaging (MRI) to survey the structure of H.M.'s entire brain to specify the damage to particular medial temporallobe structures and to document any other brain lesions.

MATERIALS AND METHODS
Case history of the patient H. M. At the time of the imaging studies (May, 1992 and August, 1993), H. M. was 66 and 67 yearsold, respectively. He was born in Manchester, CT, in 1926. Atage 9 years, he was knocked down by a bicycle. He sustained alaceration of the left supraorbital region and was unconsciousfor ~5 min. He experienced his first minor seizure (atypical petitmal) at age 10 years and his first generalized convulsion at age16. We assume that the seizures are a consequence of his headinjury, but there also is a paternal history of epilepsy. H. M.graduated from high school at age 21, having dropped out of schoolfor several years for reasons related to his epilepsy. After highschool, he obtained a position as a motor winder but had to relinquishthat job because of the frequency and severity of his seizures.When high doses of the available anticonvulsant medications didnot provide adequate seizure control, H. M.'s family consultedDr. William Beecher Scoville at the Hartford Hospital about abrain operation to relieve his epilepsy.

Scoville offered H. M. a procedure that had been performed previously only in psychotic patients (Scoville et al, 1953). In1953, when H. M. was 27 years old, he underwent "this franklyexperimental operation" (Scoville and Milner, 1957, p 11): a bilateralmedial temporal lobe resection. At the time of operation, Scovilleestimated that the removal included 8 cm of medial temporal lobetissue, including the temporal pole, amygdaloid complex, and approximatelytwo thirds of the rostrocaudal extent of the intraventricularportion of the hippocampal formation. To our knowledge, the resectedtissue was not analyzed histologically. The operation reducedthe frequency of H. M.'s seizures, but it also had an unexpectedresult: It produced a severe anterograde amnesia (Scoville andMilner, 1957; Milner et al., 1968; Corkin, 1984) that has lastedto the present.

Neurological findings in H. M. are stable and consist of a severe amnesic syndrome, anosmia (with sparing of odor detectionand odor discrimination) (Eichenbaum et al., 1983), left ulnarneuropathy attributable to compression of the ulnar nerve at theelbow, peripheral neuropathy (glove and stocking sensory deficit),and cerebellar dysfunction (incoordination of movement and nystagmuson lateral gaze). He has bilateral tinnitus that may be centralin origin. The peripheral neuropathy and cerebellar dysfunctionprobably represent side effects of phenytoin (Dilantin), an anticonvulsantmedication (Theodore et al., 1987; Botez et al., 1988; Masur etal., 1989). Cerebellar atrophy typically is severe in chronicallytreated patients; it is related to duration of illness and tothe total amount of phenytoin ingested (Botez et al., 1988). H.M. had been taking high doses of phenytoin before his operation.He continued to take phenytoin until 1984, when Tegretol was prescribedas a substitute. As early as 1962, he showed symptoms of Dilantintoxicity. He was noted to have slight unsteadiness on tandem walkingand slight slowness in performing rapid alternating movementswith both feet (suggesting cerebellar dysfunction) and well-developedgum hypertrophy (a common side effect of phenytoin) (Grant etal., 1988; Bekele et al., 1990). His current seizure medicationsinclude Tegretol, Mysoline, and Klonopin. He had not experienceda major motor seizure in several years until August 1994, whena high fever precipitated two such seizures. Based on previouselectroencephalography (EEG) studies, he probably has petit malattacks.

An EEG performed in 1993 showed intermittent bursts of generalized spike and wave and polyspike activity, which were of maximalamplitude over the fronto-temporal regions bilaterally. The burstslasted between 1 and 4 sec and were more frequent and of longerduration with hyperventilation. The runs of spike and wave activitywere less prolonged than they had been in 1984. There was no clinicalaccompaniment to the epileptiform activity.

H. M. had psychiatric evaluations in 1982 and 1992, using the Eysenck Personality Inventory, Profile of Mood States, SymptomQuestionnaire, and Beck Depression Inventory. He has also participatedin psychiatric interviews on several occasions. The results ofthese evaluations can be summarized as follows. In self care,he is somewhat negligent and requires supervision. With respectto personality and motivation, he is socially interactive butlacks initiative. His emotions are typically blunted, but he iscapable of displaying a full range of emotions. He has no libido.His insight into his condition is excellent. He is always awarethat he has a memory impairment and does not confabulate to concealit. He has no evidence of anxiety, major depression, or psychosis.From September 1986 to February 1996, he received Mellaril forintermittent irritability, which appeared to be a reaction tothe noisy and hectic atmosphere of the nursing home where he lives.This medication was not administered during his stays at the MITClinical Research Center when he participated in research.

In 1992, 6 months before the imaging studies reported here were performed, H. M. was given the Wechsler-Bellevue Scale, FormI, and the Wechsler Memory Scale, Form II. His age-corrected scoreson the Wechsler-Bellevue were Verbal I.Q., 102.7; PerformanceI.Q., 122.8; and Full Scale I.Q., 110.4. His Memory Quotient was73. The 37 point discrepancy between the Wechsler-Bellevue andWechsler Memory Scale scores indicates a severe amnesia. In contrast,he scored in the normal range on numerous standard measures offrontal lobe, language, and visuospatial function (for details,see Corkin, 1984), reflecting the integrity of the neocortex andits subcortical connections. These scores may be depressed somewhatby the actions of antiepileptic medications, which are known toimpair cognition, particularly when multiple anticonvulsants areadministered (Vining, 1987).

MRI analysis. Before 1992, we were reluctant to perform MRI on H. M., because we feared that the procedure would heat up ormove three clips placed on the dura mater at the time of operation.Enhanced computed tomography showed that these clips were farremoved from any arteries. They were used to coagulate veins runningwithin the dura at the margin of the resection. Venous structuresthrombose within days after being clipped, and the clips are typicallysurrounded by fibrous tissue within a few years after placement.Thus, even if the clips were susceptible to a magnetic field,the effect on the surrounding brain would be minimal. After extensiveconsultation with colleagues in neurosurgery and neuroradiology,it was determined that the procedure would be safe for H. M. fortwo reasons. First, the dural clips were nonmagnetic and thereforewould not move during exposure to a magnetic field. Second, theclips would not heat up beyond the temperature that the brainreaches in a febrile state. Our sources of information were asfollows. We learned from Dr. Benjamin Whitcomb, a neurosurgeonand Scoville's former partner, that the dural clips used in H.M. and other patients were purchased from Codman and Shurtleffin Randolph, MA. A telephone call to Codman and Shurtleff revealedthat the dural clips made in 1953 were either silver or tantalum,i.e., nonmagnetic. We also consulted Dr. David Piepgras, Chairof the Task Force on Clips and Clip Appliers, a subcommittee ofthe Joint Committee on Devices and Drugs of the American Associationof Neurological Surgeons and the Congress of Neurological Surgeons.Dr. Piepgras stated that in the case of dural clips from 1953,there should be no risk of movement, deflection, or overheatingduring exposure to magnetic fields such as those encountered inMRI. Additionally, a review of more than 40 published studiesby Shellock and Curtis (1991) stated that
None of the six hemostatic vascular clips evaluated were [sic] attracted by static magnetic fields used for MR imaging, upto field strengths of 1.5 T. These hemostatic clips are made fromnonferromagnetic materials and, therefore, do not present a riskto patients during MR imaging. Patients with each of the hemostaticvascular clips listed have undergone imaging safely with a 1.5T MR imager at our institution (p 547).

With our concerns for the safety of H. M. eliminated, MRI was performed in May 1992, using a 1.5-Tesla Signa System (GeneralElectric, Milwaukee, WI) scanner at the Brigham and Women's Hospital.T1-weighted coronal images [repetition time (TR) 550; echo time(TE) 16] were acquired with a 5-mm-slice thickness and a 1 mminterval between slices [256 × 192 matrix; number of excitations(NEX) 1.0; field of view (FOV) 22]. A sagittal series of T1-weightedimages (TR 600; TE 19) was acquired with a 4 mm slice thicknessand a 1 mm gap between sections (256 × 192 matrix; NEX 1.0; FOV24). A T2-weighted series of axial images (TR 2500; TE 90) wasacquired with a 5-mm-slice thickness and no gap between slices(256 × 192 matrix; 1.0 NEX; FOV 22). In a second scanning sessionconducted in August 1993 at the Massachusetts General HospitalNuclear Magnetic Resonance Center, a three-dimensional acquisitionwith 3.2 mm slices using an SPGR/35 sequence (256 × 256; 1.0 NEX;FOV 25) was undertaken. Both scanning sessions produced similarresults as to the extent of the temporal lobe lesion. The figuresshow images from both series. Figure legends describe the imagingparameters.

RESULTS

Review of the surgical procedure
Scoville's approach to the temporal lobes was made through bilateral 3.8 cm supraorbital trephine holes; the skull defectsresulting from this approach are visible in the MRI (see Fig.2M,O). Scoville described his "medial temporal lobotomy" procedure,which had been performed in a number of schizophrenic patients,in the following way (Scoville et al., 1953):
After exposing both the tip and medial surface of the temporal lobes, a cortical incision is made just anterior to the middlecerebral vessels under the midpoint of the sphenoidal ridge soas to bisect the tips of the temporal lobes. It is necessary toretract the middle cerebral vessels both posteriorly and superiorlywith the narrow flat spatula and to remove fractionally by finesuction the entire medial tips of the temporal lobes. It is notnecessary to coagulate vessels with the exception of an occasionalsmall subpial vein on the floor of the temporal fossa. After resectingthe medial tips of the lobes, it is necessary to elevate the middlecerebral vessels even higher and remove subpially by suction thegrey and white matter situated medial to the temporal horns. Thisincludes the amygdaloid nucleus, periamygdaloid cortex and anteriorportion of the hippocampus. The resection is carried 5 cm. posteriorlyfrom the tips of the temporal lobes and 3 cm. from the tips ofthe temporal horns which lie approximately level with the 3rdnerve exit into its dural ridge. The resection includes the medialwall of the anterior 3 cm. of the temporal horns and exposes thechoroid plexus within the horns. It extends vertically down tothe floor of the temporal fossa and superiorly to the upper limitsof the lobe. Posteriorly, the resection emerges in the subpialspace approximately level with the posterior surface of the pedunclesand posterior edge of the petrous ridge. The medial landmarksfrom front backwards are the anterior clinoid, the carotid artery,the 3rd nerve and optic tracts, the peduncle and posterior cerebralartery. These structures are protected by keeping subpially thruout[sic] the fractional suction resection, but it is necessary tocontinually insert the very narrow spatula extrapially and visualizethe peduncles and optic tracts as one progresses in order to preventpenetrating the pia and damaging these structures. It is to benoted that the peduncles constitute both the medial and superiorsurface of the temporal lobes (pp 353-354).

Fig. 2. T1-weighted series of coronal sections arranged from caudal (A) to rostral (P) to show the extent of the lesion in H. M. (seetext for details). Scale bars (shown in L and P), 2 cm.
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In the paper documenting the surgical procedure used with H. M. (Scoville and Milner, 1957), Scoville first described operativeprocedures performed in 30 psychiatric patients. In one group,the resections "were limited to the uncus and underlying amygdaloidnucleus" (p 11). In a second group, larger resections were carriedback 5 cm or more from the tips of the temporal lobes and "encroached...upon the anterior hippocampus" (p 11), as described above. Ina single psychiatric case, "all tissue mesial to the temporalhorns for a distance of at least 8 cm posterior to the temporaltips was destroyed, a removal which presumably included the anteriortwo-thirds of the hippocampal complex bilaterally." (p 11). Itwas this more extensive resection that was performed in H. M."An equally radical bilateral medial temporal lobe resection wascarried out in one young man (H. M.) with a long history of majorand minor seizures... " (p 11).

The present findings update this description with precise anatomical localization of the surgical lesion. By our estimation,and consistent with previous analyses of the human hippocampalformation (Amaral and Insausti, 1990), the entire rostrocaudaldistance from the temporal pole to the caudal limit of the hippocampalformation in H. M. is ~7.0 cm. Thus, had Scoville actually removed8 cm of mesial tissue, the resection would have continued wellinto the calcarine cortex. The diagram in the Scoville and Milnerpaper pictured a resection that appeared to extend caudal to thehippocampal formation (Fig. 1, left). This illustration is atvariance with Scoville's written description (which likely representshis best estimate) depicting the resection as sparing at leastone third of the caudal hippocampus. The MRI analysis providedevidence of a smaller lesion (Fig. 1, right), which is not entirelyconsistent either with Scoville's figure or with his written description.The right side of Figure 1 provides a modification of the originalScoville illustration that is more consistent with the MRI findings.
Fig. 1. Left, Diagram showing the surgeon's estimate of H. M.'s medial temporal lobe resection (Scoville and Milner, 1957, their Fig.2, p 13). The inset at the top is a ventral view of the humanbrain showing the predicted rostrocaudal extent of the ablation.A through D are drawings of coronal sections, arranged from rostral(A) to caudal (D), showing the predicted extent of the lesion.Note that although the lesion was made bilaterally, the rightside is shown intact to illustrate structures that were removed.Right, An amended version of the original diagram indicating theextent of the ablation based on the MRI studies reported here.The rostrocaudal extent of the lesion is 5 cm rather than 8 cm,and the lesion does not extend as far laterally as initially pictured.
[View Larger Version of this Image (47K GIF file)]

MRI analysis
Terminology Before presenting the results of H. M.'s MRI analysis, it is necessary to define medial temporal lobe terminology. The rostralpole of the medial temporal lobe (Brodmann area 38) is made upof cortex that closely resembles perirhinal cortex (areas 35 and36) (Insausti et al., 1994).

The temporal polar portion of the perirhinal cortex is continuous with the ventrally situated portion of the perirhinal cortex,which lines the banks of the collateral sulcus. The perirhinalcortex extends approximately to the rostral limit of the lateralgeniculate nucleus and is replaced caudally by the parahippocampalcortex (areas TF and TH). Medially, the amygdaloid complex liescaudal to the temporal polar cortex, and the hippocampal formationis caudal to the amygdala.

The hippocampal formation is made up of four components: the dentate gyrus, hippocampus, subicular complex, and entorhinalcortex. The portion of the hippocampal formation that lies inthe floor of the lateral ventricle (the portion that we referto as the intraventricular portion) is made up of the dentategyrus, hippocampus, and subicular complex. The entorhinal cortexlies ventral to the intraventricular portion of the hippocampalformation and extends for ~1 cm anterior to the anterior limitof the lateral ventricle. Here the entorhinal cortex is mediallyand ventrally adjacent to the amygdaloid complex. In a normal,adult brain, the distance from the tip of the temporal pole tothe most caudal aspect of the hippocampal formation is ~7.5 cm.The normal extent of the intraventricular portion of the hippocampalformation is ~4 cm. (For additional details on the human hippocampalformation, see Amaral and Insausti, 1990.)
General appearance of the brain The rostrocaudal length of the brain is ~14-15 cm, and the rostrocaudal extent of the temporal lobe (from the temporal poleto the splenium of the corpus callosum) is ~7 cm. The corticalsurface generally appears normal for a 66-year-old subject and,other than the temporal lobe and cerebellar alterations describedbelow, there is no indication of diffuse cortical or subcorticalbrain pathology.
Temporal lobe findings In general, the MR images of H. M.'s resection matched Scoville's description. The only major discrepancy was in the rostrocaudalextent of the ablation. Scoville had indicated that the resectionextended ~8 cm rostrocaudally. Using a liberal criterion of includingwithin the ablation those levels with even minor damage (as inthe left hemisphere shown in Fig. 2D), the rostrocaudal extentof the ablation on the left is ~5.4 cm and on the right is ~5.1cm. The resection was evident from the rostral pole of the temporallobe (Figs. 2K,L, 4D,E) and remained medial to the lateral wallof the temporal horn of the lateral ventricle. For much of itsrostrocaudal extent, the resection extended to the ventral surfaceof the temporal lobe. However, unlike the illustration depictingthe surgical report (Fig. 1, left), the edge of the resectionhad an oblique, ventromedial orientation and thus spared muchof the cortex on both banks of the collateral sulcus (Fig. 2E-I).
Fig. 4. T2-weighted axial sections indicating the extent of the anterior temporal lobe resection bilaterally (bright signal areasin C-F). Cerebellar atrophy is obvious in A and B as increasedfluid space (bright signal) surrounding the cerebellum and withinfolial spaces. Scale bar (shown in F), 2 cm.
[View Larger Version of this Image (139K GIF file)]

The surgical resection produced a bilaterally symmetrical lesion of the medial temporal lobe. Although there were minor differencesin the extent of lesion in the two hemispheres, the resectionsof the left and right hemispheres were remarkably similar. A seriesof T1-weighted coronal images through the frontal and temporallobes illustrates the extent of the ablation (Fig. 2). SagittalT1-weighted images through the body of the hippocampus (Fig. 3)show the extent of the ablation in the rostral temporal lobe andthe amount of residual intraventricular hippocampal formation.The axial T2-weighted images (Fig. 4) also show the temporal lobelesion as well as the dramatic cerebellar atrophy.
Fig. 3. T1-weighted parasagittal sections from the left (A) and right (B) sides of H. M.'s brain. The resected portion of the anteriortemporal lobes is indicated bilaterally with an asterisk. Theremaining portion of the intraventricular portion of the hippocampalformation is indicated with an open arrow. Scale bar (right ofA), 5 cm in 1 cm increments. Approximately 2 cm of preserved hippocampalformation is visible bilaterally. Note also the substantial cerebellardegeneration obvious as enlarged folial spaces.
[View Larger Version of this Image (127K GIF file)]

The ablation damaged extensively the anterior medial temporal polar cortex bilaterally. The subcortical white matter associatedwith the most anterior portions of the superior, middle, and inferiortemporal gyri may have also been compromised by the resection(Fig. 2I,J). The ablation was extensive at levels at which theamygdaloid complex would be expected (Figs. 2G,H, 3), and mostof the amygdaloid complex is missing. Only a thin rim of dorsomediallysituated amygdaloid tissue is evident at these levels. This regionwould contain remnants of the periamygdaloid and piriform corticesand the anterior cortical nucleus. At more caudal levels (Fig.2G), the most dorsal portion of the amygdaloid complex, whichconsists in part of the central nucleus, appears to be intactbilaterally. Scoville clearly intended to spare this dorsal amygdaloidregion, because he was concerned about damaging the numerous bloodvessels that perforate the overlying substantia innominata (anteriorperforated substance). The cholinergic cell groups of the basalnucleus of Meynert are embedded in this region, and this portionof the basal forebrain appears to be spared. At levels throughthe amygdaloid complex, the lesion extended obliquely with a mediallydirected inclination to the ventral surface of the temporal lobe.The underlying rostral entorhinal cortex appeared to be completelyremoved. A key finding was that the collateral sulcus was clearlyvisible at these levels (Fig. 2E-G), and thus, the ventrocaudalperirhinal cortex (areas 35 and 36), which occupies both banksof the collateral sulcus, appears to be at least partially intactat these levels. The laterally adjacent fusiform gyrus was entirelyintact.

Just behind the amygdaloid complex in the normal brain is the uncal portion of the hippocampal formation, consisting of anintricately folded allocortex, and the subjacent entorhinal cortex.The intraventricular portion of the hippocampal formation is typicallyfirst visible in the normal brain at approximately the rostrocaudallevel at which the mammillary nuclei are apparent (Fig. 2F). InH. M., the uncal portion and this rostral portion of the bodyof the hippocampal formation was completely removed bilaterally.Virtually all of the entorhinal cortex, bilaterally, was eitherremoved or damaged extensively. Posterior portions of the intraventricularhippocampal formation, however, were spared (Fig. 2C-E). The sparedportion of the hippocampus was appreciated best in the sagittalimages (Fig. 2). Although it was difficult to estimate with certaintythe amount of residual hippocampal formation, estimates from the5-mm-thick slices and from the 3.2 mm contiguous series indicatedthat these remnants accounted for ~1.9-2.2 cm of hippocampal tissue.Because the intraventricular extent of the hippocampal formationin a normal human brain is ~4 cm in rostrocaudal extent (Amaraland Insausti, 1990), the residual hippocampal formation in H.M. thus approximated 50% of the normal intraventricular extent.It also should be noted that although the hippocampal formationwas clearly visible at these caudal levels, it appeared to besomewhat atrophic bilaterally; thus, its functional integritycannot be assured. This atrophy could be attributed to any numberof factors, including loss of neuropil after extrinsic deafferentation,loss of associational connections from rostral hippocampal levels,or even hippocampal sclerosis related to H. M.'s epilepsy. Thefimbria and fornix, as expected, appeared somewhat thin.

At the posterior levels where the hippocampal formation was clearly present (Fig. 2D,E), the parahippocampal gyrus continuedto be somewhat compromised by the ablation. Figure 2D illustratesa level through the lateral geniculate nucleus, which is at orposterior to the caudal border of the entorhinal cortex (Van Hoesen,1982). The ablation extended slightly caudal to this level onthe left, and thus may have invaded the rostral portions of theposterior parahippocampal gyrus. The lesion extended slightlyfarther caudally in the left hemisphere than in the right (Figs.2D, 4E) and ended completely before the posterior limit of thehippocampal formation bilaterally (Fig. 2C). It would appear,therefore, that areas TF and TH of the parahippocampal cortexreceived only minor damage.

Because the ablation maintained its medial position throughout its rostrocaudal extent, there appeared to be essentially noinvasion of the lateral temporal neocortex (other than at thetemporal pole). There was no evidence of injury to the optic radiations,to the visual cortex in the depths of the calcarine sulcus, orto the more lateral occipital cortices (Brodmann areas 17, 18,and 19).

In summary, the temporal lobe lesions included the medial temporal polar cortex, most of the amygdaloid complex, and all ofthe entorhinal cortex bilaterally (Figs. 5, 6). In addition, theanterior 2 cm (of a total 4 cm rostrocaudal distance), approximately,of the dentate gyrus, hippocampus, and subicular complex was removed.The posterior 2 cm, approximately, of these fields was visiblebut appeared atrophic. Because the collateral sulcus and the cortexlining its medial bank were also visible throughout much of thetemporal lobe, at least some of the ventral perirhinal cortex,which is located along the banks of this sulcus, appeared to beintact. The cortices of the posterior parahippocampal gyrus (areasTF and TH) appeared to be only slightly damaged, and only at rostrallevels of these fields. The lingual and fusiform gyri, locatedlateral to the collateral sulcus, were intact.

Fig. 5. This series of T1-weighted images is arranged from rostral (A) to caudal (F) through the temporal lobe of H. M. (shown onleft) and of a 66-year-old man who has served as a control subjectin neuropsychological studies. Sections from the control brainwere selected to match as closely as possible the levels illustratedfrom H. M.'s brain. Images from H. M. are from the more recentthree-dimensional acquisition in which 3.2 mm sections were reconstructed.The control brain illustrates the structures that are likely tohave been eliminated in H. M.'s brain at each rostrocaudal level.A, The amygdala (A) and entorhinal cortex (EC) are heavily damagedat this level. The collateral sulcus (cs) is barely visible; therefore,little of the perirhinal cortex (PR) is likely to be intact atthis level. B, This is the rostral level of the intraventricularportion of the hippocampal formation (H), which is missing bilaterallyin H. M. The entorhinal cortex is also missing at this level.Because the collateral sulcus is visible, it is possible thatsome perirhinal cortex is intact at this level. The medial mammillarynucleus is present at this level and appears to be slightly shrunkenin H. M. C, This is a rostral level through the body of the intraventricularhippocampal formation. Most of the hippocampal formation, includingthe entorhinal cortex, is missing at this level in H. M. D, Alevel through the caudal body of the hippocampus. Some tissueis visible bilaterally in the region of the hippocampus in H.M., although it is clearly shrunken compared with the normal controlsubject. This level is typically located caudal to the entorhinalcortex, which is replaced with parahippocampal cortex (areas TFand TH). E, This level is at the caudal pole of the hippocampus.There is no overt damage to the medial temporal lobe at this level.The intraventricular portion of the hippocampal formation doeslook shrunken, however, relative to the normal control subject.The fimbria (f) is visible in the normal control subject and inH. M. F, This level is caudal to the hippocampal formation andis presented primarily to illustrate the substantial atrophy ofthe cerebellum (Cer) in H. M. In the normal control subject, thecerebellar cortex extends to the limit provided by the tentoriumcerebelli. In H. M., there is a substantial fluid-filled gap betweenthe cerebellar cortex and the tentorium. Note throughout thatH. M.'s cerebral cortex demonstrates relatively little sulcalwidening and that sulcal widening is more pronounced in the cognitivelynormal control subject. Figure continues.
[View Larger Versions of these Images (171 + 153K GIF file)]

Fig. 6. Nissl-stained sections from a control brain and comparable MRI sections from H. M.'s scan at rostral (top) and caudal (bottom)levels through the hippocampal formation. H. M.'s left hemisphereis shown at the rostral level, and the right hemisphere is shownat the caudal level. The Nissl-stained sections provide informationon the normal appearance of the removed (Rostral) portion of thehippocampal formation and the preserved (Caudal) portion. CS,Collateral sulcus; EC, entorhinal cortex; H, hippocampus; LGN,lateral geniculate nucleus; MMN, medial mammillary nucleus; PHG,parahippocampal gyrus; V, ventricle.
[View Larger Version of this Image (123K GIF file)]

Brain regions outside the temporal lobes The most noticeable nontemporal lobe region of pathology was in the cerebellum (Figs. 2A, 4A, 5). There was marked and diffuseatrophy of the vermis and hemispheres, evident in Figure 4A ashigh-signal, CSF-filled subarachnoid space.

The frontal, parietal, and occipital lobe cortices had a generally normal appearance. Neocortical atrophy was slight and consistentwith H. M.'s age (Fig. 5). There was no obvious lesion in theorbital or ventromedial frontal cortex that could be attributedto the surgical elevation of these areas for visualization ofthe temporal lobes. Although regions of the dorsolateral frontalcortex located deep to the defects of the trephine holes appearedto have somewhat prominent sulcal spaces (Fig. 2M-O), it was unclearwhether this damage resulted from trauma during the neurosurgicalprocedure. The mediodorsal nucleus of the thalamus (Fig. 2D,E)demonstrated no clear alterations, but the mammillary nuclei (Figs.2F, 5) were reduced in size.

DISCUSSION
For the first time, we have been able to evaluate the neurosurgical resection in H. M., perhaps the most studied person inbehavioral neuroscience. These investigations were driven by theneed to determine precisely which medial temporal lobe regionswere included in his resection and which may be responsible forhis amnesic syndrome. It was particularly important to conductthis study at this time because experimental animal studies recentlyhave questioned the role of the hippocampus in memory function(Mishkin and Murray, 1994). This initial MRI study has confirmedand extended conclusions from Scoville's surgical report. Thefollowing discussion focuses on two issues: (1) the anatomicalsubstrates for explicit or declarative memory in humans, and (2)the correspondence between the critical neural substrates in amnesicpatients and in primate models of amnesia.

Anatomical substrates for explicit/declarative memory in humans
The anterograde amnesia in H. M. is profound (Scoville and Milner, 1957; Milner et al., 1968; Corkin, 1984) and, as a result,he has become the yardstick against which the severity of otheramnesias are judged. In fact, most other published cases of medialtemporal lobe amnesia demonstrate a less severe form of memoryimpairment. What is it about H. M.'s lesion that has caused sucha profound memory impairment? H. M.'s resection eliminated theentire medial temporal polar cortex (Filimonoff area TG, Brodmannarea 38), virtually the entire amygdaloid complex, essentiallyall of the entorhinal cortex, and at least half of the intraventricularportion of the hippocampal formation. Because the entorhinal cortexwas eliminated, the remaining caudal portion of the hippocampalformation is devoid of most of its input from sensory and high-ordercortices (Van Hoesen, 1982; Amaral et al., 1987; Insausti et al.,1987). By contrast, cholinergic innervation from the basal forebrainis probably largely intact (Alonso and Amaral, 1995). It is likelythat the memory impairments in other cases (Scoville and Milner,1957) were milder or transient, because a substantial portionof the hippocampal formation was spared.

Penfield and Milner's patient, P. B., (Penfield and Milner, 1958), provides additional evidence that partial sparing of theposterior hippocampus and sparing of the parahippocampal gyrusare not sufficient to maintain normal memory function. P. B. receiveda two-stage unilateral temporal lobe resection for the alleviationof epilepsy. In the first stage, performed on August 14, 1946,the anterior 4 cm of the left temporal (lateral) neocortex wasresected; the hippocampal formation and amygdala were left intact.In a second operation, performed on September 28, 1951, Penfieldremoved the left temporal polar cortex, amygdaloid complex, andanterior half of the hippocampal formation. After this operation,the patient became severely amnesic and was still profoundly amnesicwhen retested in 1962 (Corkin, 1965). His general intelligence,in contrast, was remarkably preserved, and he had no aphasia (Penfieldand Mathieson, 1974). This patient ultimately came to autopsy,and his brain underwent histological examination (Penfield andMathieson, 1974). The left surgical resection removed all of thecross-sectional extent of the anterior temporal lobe, i.e., itwas more extensive laterally than in H. M. As in H. M., ~22 mmof the caudal hippocampal formation remained on the left, andit had a generally normal histological appearance, except forgliosis in the alveus and fimbria. On the right, the anteriortemporal lobe and amygdala appeared normal. However, the righthippocampus was shrunken, with substantial cell loss in the pyramidalcell layer and dentate gyrus (Penfield and Mathieson, 1974). Theright-side pathology indicated epilepsy-associated hippocampalsclerosis (Margerison and Corsellis, 1966), i.e., diffuse cellloss in the hippocampus and dentate gyrus, with relatively completepreservation of the subicular complex and parahippocampal cortex(including the entorhinal cortex).

Several conclusions can be drawn from P. B.'s case. As in H. M., the preserved hippocampus on the left, even though histologicallynormal, was not sufficient to support normal memory function.Amnesia in P. B. may have occurred because the second resectionof the left anterior temporal lobe removed most, if not all, ofthe entorhinal cortex and thus eliminated much of the sensoryinformation to the residual intraventricular hippocampal formation.This case also provides evidence that a clinically significantamnesic syndrome is obtained even if the bilateral component ofthe lesion is restricted to the hippocampus proper and dentategyrus. Amnesia in P. B., however, was less severe than that inH. M. (Table 1, Fig. 6) (see also Corkin, 1965, p 347). As experimentalstudies in primates now indicate, it may be necessary for bilaterallesions to include the entorhinal and/or perirhinal cortices (asin H. M.) to obtain an amnesic syndrome as severe as that in H.M. (Meunier et al., 1993; Zola-Morgan et al., 1993).

Table 1. Relation between extent of medial temporal-lobe lesion and severity of amnesia as measured by the difference between the FullScale I.Q. (F.S. I.Q.) and the Memory Quotient (M.Q.). (Normalsubjects show no significant difference.)

Subject Lesion F.S. I.Q. M.Q. I.Q.-M.Q.

H. M. Medial temporal pole (rostral perirhinal cortex), most of amygdaloid complex, anterior 2-2.5 cm of dentate gyrus, hippocampus, and subicular complex bilaterally (age corrected) 102.7 73 37

P. B. Left anterior temporal lobectomy including left temporal pole, most of amygdaloid complex, and anterior half of hippocampal formation. Right hippocampus shrunken with diffuse cell loss in hippocampus and dentate gyrus 125 97 28

R. B. CA1 field of hippocampus bilaterally, with minimal cell loss in subiculum, CA3 field, and anterior amygdaloid area 111 91 20

A similar conclusion was reached from the analysis of patient R. B. (Zola-Morgan et al., 1986). He suffered an ischemic episodethat produced a bilaterally symmetrical lesion largely confinedto the CA1 field of the hippocampus. Although this lesion produceda clinically significant anterograde amnesia, it was milder thanthat in H. M. (Table 1). Thus, the results from P. B. and R.B. support the conclusion that a bilateral lesion of the hippocampalformation alone produces a clinically significant amnesic syndromein humans. However, if the bilateral lesion includes other medialtemporal lobe structures, such as the temporal polar cortex, perirhinalcortex, and entorhinal cortex (as in H. M.), the amnesic syndromeis much more severe than that resulting from a selective hippocampallesion. The relative importance of each of these structures inhumans for normal memory function, as well as for the precisecognitive processes to which they contribute, still needs to beascertained. By one view, each of these regions performs qualitativelysimilar functions, and the progressive severity of amnesia thatis observed with increased damage is attributable to loss of thecapacity to perform the primary function of this region (Zola-Morganet al., 1994). An alternative view is that each of these brainregions contributes differentially to memory function (Murray,1992; Gaffan, 1992a,b,c, 1994; Eacott et al., 1994; Eichenbaumet al., 1994; Meunier et al., 1996), perhaps by using differentcognitive strategies, and the progressive amnesia is attributableto the elimination of alternate means for forming memories. Becausepathology rarely invades a singular, neuroanatomical region inthe medial temporal lobe, the ultimate resolution of this issuemay rely on other methods such as functional brain imaging.

The findings from H. M., P. B., and R. B. also allow one to dismiss the "temporal stem" hypothesis of medial temporal lobeamnesia (Horel, 1978). Horel speculated that the human amnesicsyndrome was not attributable to damage of the hippocampal formation,but rather to damage of the white matter, the temporal stem, locatedimmediately dorsal to the hippocampal formation. In none of thethree patients discussed above, however, was the temporal stemdirectly damaged bilaterally, nor were most of the neocorticalregions that contribute fibers to the temporal stem damaged bilaterally.Further, because the caudal half of the hippocampus is sparedin H. M. (as it was in P. B.) and because the fornix and mammillarynuclei are also spared in H. M., the subcortical connections ofthe hippocampus do not appear to be sufficient to sustain normalmemory function. This finding would argue against Gaffan's viewthat these connections, rather than hippocampal cortical connections,are primarily responsible for the role of the hippocampal formationin memory (Gaffan, 1992c). The bulk of evidence, therefore, restson the hippocampus and associated cortical regions as the primesubstrates for medial temporal lobe amnesia.

What anatomical considerations would explain the profound amnesia in H. M.? Some of the regions removed in H. M., such asthe medial temporal polar cortex and entorhinal cortex, have notbeen studied thoroughly in the human brain. In the nonhuman primate,however, neuroanatomical and behavioral studies have convergedto indicate that these regions play a role independent of thehippocampal formation in memory function. A point of terminologicalclarification must be made. In the macaque monkey, much of whatwas previously called either Brodmann area 38 or Bonin and Baileyarea TG appears to have cytoarchitectonic and connectional similaritieswith the remainder of the perirhinal cortices (Amaral et al.,1987; Suzuki et al., 1994a,b). In the human brain as well, muchof what has been labeled area 38 has cytoarchitectonic similaritieswith the more ventrocaudally situated perirhinal cortex that liesalong the banks of the collateral sulcus. Thus, in H. M., theresection appears to have included rostral levels of the perirhinalcortex but has left intact some of the caudal portion of thisregion.

The perirhinal and parahippocampal cortices are at one end of a chain of feedforward projections from unimodal and polymodalcortical areas (Mesulam, 1982; Van Hoesen, 1982; Pandya and Yeterian,1985; Freedman et al., 1986; Tranel et al., 1988; Suzuki and Amaral,1990, 1994a; Webster et al., 1991), and, in turn, provide ~60%of the cortical input to the entorhinal cortex (Insausti et al.,1987). The entorhinal cortex then forwards this sensory informationto the hippocampal formation via the perforant path (Witter andAmaral, 1991).

Several sources of evidence indicate that the perirhinal and/or entorhinal cortices may play a critical role in human memory.First, studies of patients with unilateral anterior temporal lobectomydemonstrate that small hippocampal excisions are less damagingto memory performance than are large excisions (Milner, 1980;Milner et al., 1985). Large hippocampal removals, i.e., thosethat extend caudal to the uncus, eliminate the whole entorhinalcortex and thus interrupt cortical input to the hippocampal formation.Small hippocampal removals, in contrast, spare some of the entorhinalprojections to residual hippocampus that are apparently sufficientto support residual memory function. Second, selective amygdala-hippocampectomy,which encroaches on entorhinal and perirhinal cortex but sparesthe lateral temporal lobe neocortex (Yasargil et al., 1993), impairsmemory test performance to the same extent as does unilateralanterior temporal lobectomy with encroachment on the hippocampus(Jones-Gotman et al., 1997).

Correspondence between the critical neural substrate in amnesic patients and in primate models of amnesia
Early primate models of human medial temporal lobe amnesia emphasized the role of the hippocampal formation and amygdaloidcomplex. Specifically, monkeys with the hippocampus, amygdala,and surrounding cortex removed were impaired on several recognitionmemory tasks (Mishkin, 1978; Zola-Morgan et al., 1982; Murrayand Mishkin, 1984; Phillips and Mishkin, 1984; Saunders et al.,1984; Zola-Morgan and Squire, 1985). To determine which areaswithin the medial temporal region are critical for normal memoryperformance, recent studies have focused on the effects of smalllesions restricted to (1) the hippocampus, (2) amygdala, (3) entorhinalcortex (area 28) (Leonard et al., 1995), or (4) perirhinal cortex(areas 35 and 36) combined with parahippocampal cortex (areasTH and TF) (Zola-Morgan et al., 1989c; Suzuki et al., 1993). Theresults of these studies indicate that all of these anatomicallylinked medial temporal areas, except the amygdala, participatein recognition memory function (Murray et al., 1989; Zola-Morganet al., 1989a,b,c, 1994; Meunier et al., 1993) (but see Murray,1991). Although a significant memory impairment is seen when onlythe hippocampus, dentate gyrus, and subicular complex are includedin the lesion (the H lesion) (Clower et al., 1991; Beason-Heldet al., 1993; Alvarez et al., 1995), the memory impairment ismore severe when the caudal entorhinal and perirhinal corticesare included in the lesion (the H⁺ lesion) (Mahut et al., 1982; Zola-Morgan et al., 1989a), andeven more severe when the perirhinal cortex is also included (theH⁺⁺ lesion) (Zola-Morgan et al., 1993). Moreover, lesions restrictedto the perirhinal and parahippocampal cortices (Zola-Morgan etal., 1989c; Suzuki et al., 1993) or to the entorhinal and perirhinalcortices (Meunier et al., 1993) (sparing other medial temporallobe structures) produce memory deficits that are not only comparablein severity with those seen after bilateral medial temporal lobectomy,but also are multimodal and long-lasting (Suzuki et al., 1993).Clearly, each of the multiple areas within the medial temporallobe region, including the hippocampal formation and the perirhinalcortex, contributes to normal memory function. It is unclear,however, whether each of these regions is performing essentiallysimilar mnemonic tasks so that the deficit becomes more severewhen more of these processing regions are removed (Zola-Morganet al., 1994), or whether there are dissociations of functionwithin the medial temporal lobe region (Gaffan, 1992a,b,c, 1994;Murray, 1992; Eacott et al., 1994; Eichenbaum et al., 1994; Meunieret al., 1996) so that the memory impairment becomes more severeas more strategies for task-solution are eliminated. It will beessential to conduct parallel studies in monkeys and human amnesicsubjects to determine the precise cognitive function of each ofthese medial temporal lobe regions.

Conclusions
This MRI study has confirmed that the lesions responsible for the amnesic syndrome in H. M. are confined to the medial temporallobe. Given the severity and permanence of the anterograde amnesiain H. M., it is clear that the remaining 2 cm of posterior, intraventricularhippocampal formation, approximately, (of a total rostrocaudalextent of ~4 cm) is not sufficient to support normal memory functions.Whether this preserved tissue is functional and capable of mediatingany cognitive processes awaits the results of ongoing functionalimaging studies. The severity of the memory impairment in H. M.,compared with that in other amnesic patients with selective hippocampallesions, may be related to the inclusion of portions of his entorhinal,perirhinal, and parahippocampal cortices in the medial temporallobe removal.

FOOTNOTES

Received Jan. 28, 1997; accepted Feb. 7, 1997.

This work was supported by National Institutes of Health (NIH) Grants AG 06605 and AGNS 08117 (S.C.) and NS 16980 and MH R3741479(D.G.A.), and by the Human Frontier Science Program (D.G.A.).The MIT Clinical Research Center (CRC) is supported by NIH GrantRR00088. We are grateful to Brenda Milner for permission to studyH. M., Peter Black for helping us initiate this project, RichardB. Schwartz for performing the MRI scan at the Brigham and Women'sHospital, and Rosamund Hill and Steven W. Parker of the MassachusettsGeneral Hospital for performing the EEG. We also thank PierreGloor, Leyla deToledo-Morrell, Frank Morrell, Elisabeth A. Murray,and Larry Squire for valuable discussions. We acknowledge withthanks the special care given to H. M. by the CRC staff. We alsothank Kris Trulock for photographic assistance.

Correspondence should be addressed to Dr. Suzanne Corkin, E10-003A, MIT, Cambridge, MA 02139.

This paper is dedicated with appreciation to H. M., whose loss of memory has provided us with a wealth of information concerningthe organization of memory.

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Volume 17, Number 10, Issue of May 15, 1997 pp. 3964-3979 Copyright ©1997 Society for Neuroscience

H. M.'s Medial Temporal Lobe Lesion: Findings from Magnetic Resonance Imaging

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Volume 17, Number 10, Issue of May 15, 1997 pp. 3964-3979
Copyright ©1997 Society for Neuroscience