Anatomical Evidence of Multimodal Integration in Primate Striate Cortex

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The Journal of Neuroscience, July 1, 2002, 22(13):5749-5759

Anatomical Evidence of Multimodal Integration in Primate Striate Cortex
Arnaud Falchier, Simon Clavagnier, Pascal Barone, and Henry Kennedy
Institut National de la Santé et de la Recherche Médicale U371, Cerveau et Vision, 69675 Bron Cedex, France

  ABSTRACT

TOP
ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

The primary visual cortex (area 17 or V1) is not thought to receive input from nonvisual extrastriate cortical areas. However,this has yet to be shown to be the case using sensitive tracersin the part of area 17 subserving the peripheral visual field.Here we show using retrograde tracers that peripheral area 17subserving the visual field at an eccentricity of 10-20° receivesprojections from the core and parabelt areas of the auditory cortexas well as from the polysensory area of the temporal lobe (STP).The relative strength of these projections was calculated foreach injection by computing the proportions of retrogradely labeledneurons located in the auditory and STP areas with respect tonumber of labeled neurons constituting the established projectionfrom the superior temporal sulci (STS) motion complex (middletemporal area, medial superior temporal, fundus of the superiortemporal area). In peripheral area V1 the projection from auditorycortex corresponds to 9.5% of that of the STS motion complex andSTP to 35% of that from the STS motion complex. Compared to peripheralarea 17, central and paracentral area 17 showed considerably weakerinputs from auditory cortex (0.2-0.8%) but slightly more fromSTP cortex (3.5-6.1%). The present results show that the connectivityof area 17 is eccentricity dependent. Direct projections fromauditory and STP cortex to peripheral area 17 have important consequencesfor higher visual functions of area 17, including multimodal integrationat early stages of the visual corticalpathway.

Key words: area 17; area V1; auditory cortex; polysensory integration; retinotopy; visual pathways; anatomy; monkey

  INTRODUCTION

TOP
ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

Multimodal integration of sensory inputs has been shown to occur at different midbrain and cortical levels (Stein and Meredith,1993). The known anatomy of the visual cortex predicts that integrationof visual and nonvisual stimuli will occur at late stages of corticalprocessing (Hikosaka et al., 1988; Calvert et al., 2001). Previousanatomical and single-unit recording studies point to multisensoryintegration in polysensory areas located in temporal, parietal,and frontal cortex (Goldman-Rakic, 1988). However there is recentelectrophysiological and brain imaging evidence that visual, auditory,and somatosensory integration occurs at early stages of the visualcortical pathways (Giard and Peronnet, 1999; Macaluso et al.,2000), for example around the lingual gyrus where area 17 is located.Findings in favor of early polysensory integration are intriguingbecause anatomical studies in the monkey have failed to detectafferent connections to primary visual cortex from areas processingmodalities other thanvision.

The reported absence of multisensory input to area 17 is also surprising in view of the consequences of early deprivation.Congenital blindness leads to early visual cortical areas in thedorsal stream responding to nonvisual stimuli, including tactile(Sadato et al., 1996; Buchel et al., 1998; Cohen et al., 1999)and auditory (Weeks et al., 2000) stimuli. It is thought thatthese nonvisual responses are being relayed back to early visualcortical stages via back projections from the parietal cortex(Pons, 1996). Alternatively, nonvisual information may have accessto visual areas through developmental changes in the centrifugalpathways (Angelucci et al., 1998).

Area V1 receives projections from ~12 areas that have all been described as belonging to the visual cortex (Maunsell and VanEssen, 1983; Felleman and Van Essen, 1991). More recently, somewhatweak projections have been described from distant areas in theventral (temporal occipital area, temporal area) (Distler et al.,1993) and dorsal visual pathways [medial superior temporal (MST)and lateral intraparietal area (LIP)] (Boussaoud et al., 1990;Felleman and Van Essen, 1991; Rockland et al., 1994; Barone etal., 2000). However, these distant areas contain neurons thatrespond principally to visual stimuli and oculomotor activity,except for LIP where auditory related activity has been reported(Linden et al., 1999).

Evidence in favor of multimodal integration at early visual stages has led us to question the accepted wisdom concerning thenature of back-projections to area V1 (Jones and Powell, 1970;Macaluso et al., 2000). The vast majority of studies on the connectivityof area V1 have been centered on the operculum, where the representationof the central 0-8° is located. Of the few studies that have includeddata on the connectivity of the peripheral representation of areaV1, that of Shipp and Zeki (1989) revealed a quantitative differenceconcerning the back projection of the middle temporal area (MT).Their study showed that MT projections to the calcarine cortexgave a stronger labeling in layer 1 than did the MT projectionsto layer I in central area V1. In the present study we have specificallyaddressed the question of the effects of the representation ofthe visual field on connectivity of area 17 using retrograde tracerscoupled with quantification oflabeling.

  MATERIALS AND METHODS

TOP
ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

Injections of tracers. Thirteen retrograde tracing experiments were performed on nine cynomolgus monkeys (Macaca fascicularis;Table 1). After premedication with atropine (1.25 mg, i.m.) anddexamethasone (4 mg, i.m.), monkeys were prepared for surgeryunder ketamine hydrochloride (20 mg/kg, i.m.) and chlorpromazine(2 mg/kg, i.m.). Anesthesia was continued with halothane in N₂Oand O₂ (70:30). Heart rate was monitored, and artificial respirationwas adjusted to maintain the end-tidal CO₂ at 4.5-6%. The rectaltemperature was maintained at 37°C. Single injections of retrogradefluorescent tracers fast blue (FsB) and diamidino-yellow (DY)were made by means of Hamilton syringes that were in some casesequipped with glass pipettes (40-80 µm diameter). Injections weremade at a shallow angle to the cortical surface and the tracerwas injected while the needle or pipette was withdrawn from thecortex to form longitudinal injections sites (2-3 mm) primarilyrestricted to the cortical gray matter. The smallest injectionwas the DY injection in M85RH (0.05 µl). In the other single injections,0.2-0.3 µl of tracer were delivered. In one case (BB270) multipleinjections were made and a total of 2 µl of DY was delivered.Side-by-side FsB and DY injections were separated by 3 mm.


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Table 1. Numbers of labeled neurons in auditory, STP, and STS complex

In the present study we explored the connectivity at four different ranges of eccentricity with reference to published mapsof the representation of visual space in area 17 (Daniel and Whitteridge,1961; Gattass et al., 1981; Van Essen et al., 1984). Injectionsaimed at the foveal representation of area 17 and were made laterallyon the operculum of the occipital lobe, 2/5 mm from the V1-V2border (Fig. 1) These central area 17 injections were in cortexsubserving 0-2° in the lower visual field. Injections aimed atthe paracentral representation of area 17 were located at themedial limit of the operculum (Fig. 2). These paracentral area17 injections were in cortex subserving 6-8° in the lower visualfield. The description of the location of injection sites in peripheralarea 17 uses the anatomical terminology of Daniel and Whitteridge(1961) and Van Essen et al. (1984). The calcarine cortex viewedparasagitally has a mushroom configuration with a head and a stem.Injections aimed at the peripheral representation were made inthe head and stem of the calcarine sulcus by means of verticalpenetrations using stereotaxic coordinates (Fig. 3). Two differenteccentricities can be distinguished in peripheral area 17 injections.M76LH was located in the dorsal leaf of the calcarine cortex (Danieland Whitteridge, 1961). According to the published map of area17, this injection (M76LH) was in cortex subserving 10-12° eccentricity(Van Essen et al., 1984). The other two peripheral injections(M81RH and M88LH) were located further ventrally near the junctionof the dorsal leaf with the calcarine stem and were in cortexsubserving 15-20° (Van Essen et al., 1984). The auditory cortexof the caudal part of the parabelt was injected on the superiortemporal gyrus (STG) between the lateral and superior temporalsulci. FsB injection into area STP [temporal parieto-occipitalassociated area intermediate/temporal parieto-occipital associatedarea caudal (TPOi/TPOc)] did not involve STG and area MST.

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Figure 1. Injection sites in area 17 subserving the central visual field. A, Lateral view of the monkey brain showing the level of the injection sites in horizontal sections. B, Representative horizontal section showing location of central injection sites. C, Photomicrograph of DY injection site. D, Lateral view of the brain showing the visual representation of area V1 and location of central injection sites (Gattass et al., 1981). D, Bottom, Injection sites with respect to the visual field. E, Central injection sites, two sections per injection. Uptake zone is shown in black. Gray, Dense intrinsic labeling of area V1. Numbers refer to section number. Thin lines, White matter-gray matter boundary. Dotted lines, layer 4. Arrowheads, Area V1/V2 border. Cases M85RH FsB, DY, Only one injection site of a pair is shown. IOS, Inferior occipital sulcus; LS, lunate sulcus; CaS, calcarine sulcus; IPS, intraparietal sulcus; CeS, central sulcus; OTS, occipitotemporal sulcus; STS, superior temporal sulcus; LaS, lateral sulcus; AS, arcuate sulcus; PS, principal sulcus; POS, posterior occipital sulcus.

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Figure 2. Injection sites in area 17 subserving the paracentral visual field. A, Dorsal and lateral view of the monkey brain showing the level of the injection sites in parasagittal and horizontal sections. B, Injection sites on dorsal part of the operculum. Inset shows representative parasagittal section showing location of injection sites in M75LH and M75RH. C, Injection site on the posterior part of the operculum. Inset shows representative horizontal section showing location of injection site in M87RH. D, Lateral view of the brain showing visual representation of area V1 and location of paracentral injection sites (taken from Gattass et al., 1981). Bottom, Injection site with respect to the visual field. Conventions and abbreviations as in Figure 1.

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Figure 3. Injection sites in area 17 subserving the peripheral visual field. A, Lateral view of the monkey brain showing the level of the injection sites in horizontal sections. B, Photomicrograph of fast blue injection site. C, Two horizontal sections illustrating the two levels in A. D, Lateral view of the brain showing visual representation of area V1 and location of peripheral injection sites (taken from Gattass et al., 1981). Below, injection sites with respect to the visual field. E, Injection sites in the calcarine sulcus. Conventions and abbreviations as in Figure 1.

Histological procedures. After 11-13 d survival, animals were deeply anesthetized before being perfused with 200 ml of 0.9%saline, 1 ml of 4-8% paraformaldehyde-0.05% glutaraldehyde inphosphate buffer (0.1 M), pH 7.4, and 10-30% sucrose in phosphatebuffer (0.1 M), pH 7.4. All the procedures used follow the Nationaland European regulations concerning animal experiments (EC guidelines86/609/EC) and have been approved by the authorized national andveterinary agencies. Brains were removed, blocked, and 40-µm-thicksections were cut on a freezing microtome. One section in threewas mounted in saline onto gelatinized slides. Sections at regularintervals were reacted for cytochrome oxidase and acetylcholinesterase(AChE) activity (Barone et al., 2000), SMI-32 (Hof et al., 1996),parvalbumin (Kosaki et al., 1997), and Cat-301 (DeYoe et al.,1990). Sections were observed in UV light with oil-immersion objectivesusing a Leitz fluorescent microscope equipped with a D-filterset (355-425 nm). A computer-assisted program (Biocom) coupledto the microscope stage was used to trace out sections and torecord the position of labeled neurons. After observation, sectionswere counterstained with cresyl violet and projected on to chartsof labeled neurons to relate the position of labeled neurons toestablished histologicalborders.

Location of cortical areas. Immunohistochemical and myelin staining criteria made it possible to localize labeled neuronsin MT, MST, FST [superior temporal sulci (STS) complex], STP,and auditory areas (Morel et al., 1993; Cusick, 1997). MT is locatedin the posterior bank of STS and characterized by strong immunolabelingof layers 2/3 neurons with Cat-301 (DeYoe et al., 1990) and parvalbuminreactivity in layer 3 and 4. We characterized the limit betweenareas located in the medial bank of STS (MST, FST) and area STPlocated along the anterior bank of the superior temporal sulcus(Bruce et al., 1981) using SMI-32 immunohistochemistry and myelinstaining. SMI-32 reactivity distinguished MST and STP in layers3 and 5 (Cusick, 1997). In addition, myelin staining was darkerin top layers of STP compared with MST. The border of area STPwith the parabelt was distinguished using myelin staining (Morelet al., 1993). This shows that the parabelt extends across theSTG on to the upper bank of the STS, as shown in Figure 4C (Hackettet al., 1998). The auditory area A1 located in the posterior bankof lateral sulcus is distinguished using AChE and cytochrome oxidasereactivity (Morel et al., 1993; Hackett et al., 2001) and by thepresence of a strong parvalbumin staining in layers 2-4 (Kosakiet al., 1997).

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Figure 4. Labeling in auditory cortex after peripheral injections. A, Lateral view of the brain and horizontal section showing levels of sections in B and C. B, AChE labeling; arrows indicate limits of core and belt of the auditory cortex in the lateral sulcus. C, Individual sections showing labeling in auditory cortex. D, Density profiles. Numbers of neurons per section counted between the arrowheads indicated in C. Conventions and abbreviations as in Figure 1.

Analysis. For each cortical area and in each animal, numbers of neurons were computed at regular intervals and using highsampling frequencies in all structures containing labeled neurons.The regional extent of the area that contains labeled neuronsis the projection zone (Figs. 4, 5). Density profiles (numbersof neurons per section) provide a one-dimensional reconstructionof the projection zone. The zero on the horizontal axis of thedensity profiles shown in Figures 4 and 5 correspond to the lastsection before the projection zone. Density profiles show thenumber of neurons falling off from a peak in the center of theprojection zone to minimal values in the periphery (Batardièreet al., 1998). Visual inspection of the density profiles makesit possible to ensure that optimal sampling frequencies are usedfor different cortical areas. Hence, the relative proportion ofneurons in the areas of interest are calculated for maximal samplingfrequencies (1:1) from the actual frequency used (Table 1), whichvaries according to the dimension and density of labeling in individualareas.

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Figure 5. Labeling in STP after peripheral injections. A, Individual sections showing labeling in multisensory cortex. Arrowheads show limits within which neurons were counted in STP and in the STS complex. B, SMI-32 labeling; the arrow indicates the limit between area STP and the STS complex. C, Density profiles. Numbers of neurons per section in STP counted between the arrowheads indicated in A. Conventions and abbreviations as in Figure 1.

  RESULTS

TOP
ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

Three groups of injections of FsB and DY were made in area 17 subserving the central (0-2°), paracentral (6-8°), and the peripheral(10-20°) visual field (Van Essen et al., 1984). The central andparacentral injections on the operculum were made parallel tothe area 17 border (see Materials and Methods). The tracers FsBand DY have highly restricted uptake zones (Kennedy and Bullier,1985). In all cases, except for the multiple injections in BB270,injection sites were reconstructed, and the uptake zones weredetermined. All uptake zones were limited to area17.

Injections of area 17 subserving the central visual field had uptake zones, which were all restricted to the cortical graymatter and were located between 1.75 and 4 mm of the V1-V2 border(Fig. 1). The smallest injection (M85RH DY) was centered on layer4. The uptake zones of M85RH FsB and M85LH injections involvedall six cortical layers. In M81LH the uptake zone failed to involvethe bottom part of layer 6 (Fig. 1).

The paracentral injections were located on the operculum adjacent to the interhemispheric fissure. The two single paracentralinjections (M75LH and M75RH) were located dorsally between 5 and8 mm of the V1-V2 border. M75LH showed minor involvement of thewhite matter. In M75RH however, there was extensive involvementof the underlying white matter (Fig. 2). However, there was anabsence of labeled neurons in the calcarine, and there was a singlelocus of labeling in area V2 and the lateral geniculate nucleus.These observations show that uptake and transport of the dye wasrestricted to the injection of the cortical gray matter of area17 on the operculum. The third single paracentral injection (M87RH)was posterior on the operculum, and reconstruction of the uptakezone showed that it involved all cortical layers. The fourth paracentralinjection (BB270RH) was made by multipleinjections.

The reconstructions of the uptake zones of injections in area 17 subserving the peripheral visual field showed that all injectionsites had uptake zones limited to the cortical gray matter (Fig.3). Cases M81RH and M88LH involved all cortical layers. The uptakezone of the M76LH injection did not go right to the bottom oflayer 6 (Fig. 3).

Injections in peripheral area 17 consistently labeled neurons in the infragranular layers of auditory cortex, which couldbe identified by means of AChE staining (Fig. 4). Labeled neuronsin the auditory cortex were primarily located on adjacent sections,showing that labeling originates from a relatively circumscribedregion of cortex extending 5-8 mm dorsoventrally and which canbe broadly related to known subdivisions of the auditory cortex(Hackett et al., 1998) (Fig. 4B). These comprise the auditorycore and belt cortex, which coincide with the AChE dense regionon the posterior bank of the lateral sulcus (LaS). The auditoryparabelt coincides with lighter AChE staining and occupies theSTG at the lateral margin of the core and belt regions (Hackettet al., 1998). The levels of histological sections correspondingto dorsal and ventral limits of the auditory projection zone areshown on a lateral view of the brain (Fig. 4). This shows thatthe zone of labeled cells overlaps with only the more dorsal partof the AChE-dense region. Approximately one-third of the labeledcells was located inside the AChE-dense region, in the regionof the core, caudal lateral belt, and the middle lateral beltcomponents (Hackett et al., 1998). In our material we were notable to distinguish between the core, caudal lateral belt, andmiddle lateral belt components. The remaining two-thirds of labeledneurons were on the superior temporal gyrus where the caudal auditoryparabelt is located (Fig. 4) (Hackett et al., 1998). Hence, themain site of labeled neurons was the caudal parabelt, which ispart of the dorsal auditory stream (Rauschecker and Tian, 2000).After injections in the central and paracentral representationof area 17, only occasional scattered labeled neurons are foundin this region (Fig. 6) (Table 1).

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Figure 6. Quantitative analysis of labeling in auditory cortex and area STP. Histogram of the mean (±SE) proportion of labeled neurons in auditory cortex and area STP. Percentages refer to the number of neurons observed in the posterior bank of STS (STS complex) (Table 1).

Injections in peripheral area 17 labeled neurons in the STP, which is localized in the anterior bank of the superior temporalsulcus (Cusick et al., 1995). Labeled neurons were located inthe infragranular layers, and density profiles revealed labelingover ~10 mm in the dorsoventral direction with peak levels oflabeling located over 3-8 mm, suggesting relatively compact projectionzones (Fig. 5). Labeled neurons in STP are located in the posteriorpart of the anterior bank of STS, a region corresponding to TPOi/TPOc,which is interconnected to the dorsal visual stream (Cusick, 1997).

To estimate the relative strength of the projections from STP and auditory cortex to area 17, we pooled the results to formtwo groups for the central and paracentral injections. For theperipheral injections we have separated M76LH, which is locatedin cortex subserving 10-12° from M81RH and M88LH, which are incortex subserving 15-20° (see Materials and Methods) (Table 1).For each of these four groups we have proceeded to compute thefraction of neurons located in STP and auditory cortex (Fig. 6).This was done by counting the total number of neurons in STP andauditory cortex and expressing these numbers as fractions of thetotal number of neurons counted in the STS motion complex. Thismakes it possible to compare the strength of the projection atdifferent eccentricities and helps overcome variations in thesize of the effective uptake in different injections as revealedby the density plots. This is illustrated in M85LH in centralarea V1 in which the density profile shows a peak count in STPof 30 neurons per section, which is comparable to the peak countsin the two peripheral injections M76LH and M88LH (Fig. 5). However,the tracer uptake and transport in the central injection has beenmore effective in the central injection and leads to larger numbersof labeled STS complex neurons so that it returns a weaker strengthof projection from STP of 4.8% compared with 24.6 and 21% forthe two peripheral injections (Table 1). It could be objectedthat the changes we observe with eccentricity are attributableto changes in the numbers of labeled neurons in the STS complexrather than to changes in the auditory cortex and STP. To controlfor this we have calculated the percentage of neurons in eachstructure with respect to the total number of labeled neuronsin the cortex. This confirmed that eccentricity influenced numbersof neurons in STP and auditory cortex and not in the STScomplex.

In the present study we distinguish the auditory parabelt on the supratemporal gyrus from a combined area A1 and the auditorybelt area in the lateral sulcus. At all eccentricities the parabeltcontained approximately two-thirds of the labeled auditory neurons.The relative proportions of labeled neurons in auditory cortexin both central and paracentral injections is very low (0.2-0.5%)and shows a sharp increase to reach 9.5% after peripheral injections(Fig. 6). Injections in central area 17 gave relative STP projectionsof 3.5%, which showed a moderate increase in the paracentral injectionsto reach 6.1%. Again there was a sharp increase in the relativestrength of the STP projection, which reached 35.3% of the numberof neurons in the STS motion complex after peripheral injections.These central or periphery differences are not caused by individualvariability because in one case (M81; Table 1) a simultaneousinjection in the central and peripheral representation of area17 leads to a similar large eccentricity difference (inputs fromthe combined auditory and STP areas, peripheral representation:44.9%, central representation: 3.6%).

We examined whether the projections from STP and auditory cortex are reciprocal. The two cases where the auditory cortex (STG)and area STP received injections of retrograde tracer failed toreveal labeled neurons in area 17, suggesting that the projectionsfrom auditory and STP cortex to area 17 areunidirectional.

  DISCUSSION

TOP
ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

There have been only a limited number of studies investigating how the connectivity of a cortical area is influenced by representationof the visual field, and these have mostly concentrated on theinterconnections between extrastriate visual areas (Baizer etal., 1991; Stepniewska and Kaas, 1996; Galletti et al., 2001;Lyon and Kaas, 2002). Relatively few studies have addressed thedifferences in the connectivity of area 17 subserving the centraland peripheral visual field (Martinez-Millan and Hollander, 1975;Shipp and Zeki, 1989). One striking difference between centraland peripheral area 17 is evidence of a direct connection of peripheral17 with the prostriata (Sousa et al., 1991; Rosa et al., 1993).These findings are complementary to ours, suggesting that peripheralarea 17 is directly influenced by nonvisualinputs.

Technical considerations: reliability of the visual field representation of the injections sites

Area 17 has a fine grain representation of the visual field, and a number of studies have established highly reliable mapsof visual space representation in the primary visual area (Danieland Whitteridge, 1961; Gattass et al., 1981; Van Essen et al.,1984). In the present study we have been able to use these mapsto locate injection sites in cortical regions representing central,paracentral, and peripheral visual fields. The three injectionsites in cortex subserving the peripheral visual field would notappear to concern the same representation, and an injection at10-12° can tentatively be distinguished from two injections at15-20° (see Materials and Methods). However, although the distinctionbetween central, paracentral, and peripheral is sufficiently strongto not be influenced by interanimal variability, the distinctionbetween the injection sites at 10-12° and 15-20° must be consideredas a tentative in the absence of visual fieldmapping.

Influence of eccentricity on connectivity of area 17 with STP and area A1

The present results show that peripheral but not central area 17 receives projections from auditory cortex. Similar resultsare found for STP, although STP projections at 3.5% are non-negligible.Figure 6 suggests that the density of the auditory and STP projectionto area 17 increases progressively with eccentricity. Althoughthe absence of precise mapping of visual space before injectionin the present study makes this an unproven point, we need tokeep in mind the possibility that the density of auditory andSTP projections to eccentricities >20° may be more important thanthat revealed in the presentstudy.

Interspecies comparison

Although sparse projections from auditory cortex to area 18 in rodents and cat have been reported (Miller and Vogt, 1984;Innocenti et al., 1988), projections to area 17 are thought tobe absent in these species (Dehay et al., 1988; Sanderson et al.,1991; Montero, 1993). Whereas we cannot exclude the possibilitythat some of the above studies might have missed an auditory projectionto peripheral area 17, at least one specifically addressed thispossibility and found no such projection (Montero, 1993). Theseinterspecies comparisons suggest that the projection of auditorycortex to peripheral area 17 might be a primate feature. Homologiesof STP in nonprimates are difficult to identify. One candidateis the anterior ectosylvian sulcus in cat which has not been foundto have a projection to either area 17 or 18 (Symonds and Rosenquist,1984).

Role of auditory-STP projections to area 17 in polysensory integration

STP may play an important role in polysensory integration (Bruce et al., 1981; Baylis et al., 1987; Hikosaka et al., 1988).First, more than half of visual neurons also respond to auditoryand/or somatosensory stimuli. Second, lesion experiments aimedat area STP lead to auditory or somatosensory neglect (Luh etal., 1986; Watson et al., 1994), suggesting that area STP is involvedin cross-modal attentional mechanisms. All of this argues fora nonvisual modulation of peripheral V1 through the direct projectionfrom areaSTP.

The auditory system is organized in parallel streams and the caudal auditory parabelt area, which contains approximately two-thirdsof the labeled neurons in the auditory cortices in the presentstudy, is part of the dorsal auditory pathway specialized in spatialinformation processing, including sound source localization (Romanskiet al., 1999; Kaas and Hackett, 2000; Rauschecker and Tian, 2000;Recanzone et al., 2000b; Tian et al., 2001). Auditory cortex playsan important role in sound localization (Clarey et al., 1992),and receptive fields are large and extend behind the pinna axis(Barone et al., 1996). Similarly auditory receptive fields inSTP are large and expand in the peripheral visual field (Hikosakaet al., 1988). Hence, there is a possibility of congruence inthe spatial properties of the auditory receptive fields of A1/STPand the visual representation of area 17 to which these areasproject. However, we did not find a tight clustering of labeledneurons in the lateral sulcus, in agreement with the lack of aprecise spatial map of auditory space in the auditory cortex (Clareyet al., 1994; Recanzone et al., 2000b). Nor did we find clusteringof labeled neurons in STP in line with the absence of retinotopicorder in this area (Bruce et al., 1981; Hikosaka et al., 1988).

Polysensory integration could serve to enhance perceptual capacities (Stein and Meredith, 1993) so that the addition of anauditory signal to a visual stimulus might lead to improved detection.This could serve to reduce behavioral orientation response timeto visual stimuli (Goldring et al., 1996; Giard and Peronnet,1999; McDonald et al., 2000). This is relevant to our findingsbecause the short latencies to auditory stimulus in A1 and STP(Bruce et al., 1981; Recanzone et al., 2000a,b) suggest that therecould be temporal congruence in activation of A1/STP and area17. This could mean that the projections from STP and auditorycortex to area 17 could participate in a foveation mechanism towarda peripheral sound source, which would be compatible with thegreater prevalence of these projections to the peripheral representationof area 17 (Heffner and Heffner, 1992).

Corticocortical feedforward projections going from lower to higher hierarchical levels are thought to elaborate receptivefield response (Vanduffel et al., 1997). The projections fromSTP and auditory cortex to area 17 form part of the feedback pathwaysto area 17. Feedback projections are involved in more global levelsof analysis and implicate area 17 in higher visual functions (Leeet al., 1998; Pascual-Leone and Walsh, 2001; Super et al., 2001;Tolias et al., 2001). Feedback pathways have also been implicatedin visual imagery (Miyashita, 1995), and cross-modal activitycould be associated with the mental image of the stimuli and hasbeen implicated in the activation of the calcarine cortex in humans(Klein et al., 2000). Cross-modal-related activity has been foundin neurons of association temporal areas (Gibson and Maunsell,1997) and in the primary somatosensory area of the monkey (Zhouand Fuster, 2000). Similarly, in humans performing a tactile objectrecognition task, a specific activity has been observed in thevisual cortex of the calcarine in the absence of visual information(Deibert et al., 1999).

Auditory-STP projections to area 17 and functional reorganization after early deprivation

Polysensory integration could play an important role in the functional reorganization of the cortex after sensory deprivationand may depend on cortical pathways such as the auditory-STP projectionto peripheral area 17 (Pons, 1996). Patients suffering from earlyblindness have early visual areas, including primary visual cortexresponsive to tactile (Sadato et al., 1996; Cohen et al., 1997;Buchel et al., 1998) and auditory (Weeks et al., 2000) stimuli.This could improve the capacity of the blind to localize soundin peripheral auditory space (Roder et al., 1999). A recent PETstudy in deaf adults suggests that cross-modal plasticity underliesrecovery of language comprehension after cochlear implantation(Giraud et al., 2001). These authors suggest that the activationof visual cortex is similar to the recruitment of auditory cortexduring lipreading (Calvert et al., 1997). One can make the hypothesisthat cross-modal cooperation could compensate for suboptimal stimulationby processing complementary input from another sensory modality.Hence, anatomical, electrophysiological, and brain imaging studiessupport a model of cross-modal integration within a distributednetwork of cortical areas in which the primary visual area couldparticipate in the initial integration of sensory information(Stein, 1998; Calvert et al., 2000).

  FOOTNOTES

Received Feb. 20, 2002; revised April 15, 2002; accepted April 15, 2002.

This work was supported by the Human Frontier Science Program Grant RG0133/2000-B and the European Community, FP5 Qualityof Life Grant QLG3-1999-01064. Simon Clavagnier was supportedby the Fédération des Aveugles and handicapés visuels de France.We thank L. Renaud for technical assistance. P. Giroud made importantcontributions to the computerized dataanalysis.

Correspondence should be addressed to Henry Kennedy, Institut National de la Santé et de la Recherche Médicale U371, 18avenue du Doyen Lépine, 69675 BRON cedex France. E-mail: kennedy{at}lyon151.inserm.fr.

P. Barone's present address: Centre de recherche cerveau et cognition, Centre National de la Recherche Scientifique UMR5549,Université Paul Sabatier, 31062 Toulouse cedex 4, France

  REFERENCES

TOP
ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

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