Neurodevelopmental trajectories of the human cerebral cortex (2008)

Introduction

Most maps of human cerebral cortex have partitioned it according to histological features, such as the distribution of cell bodies or myelin, and, more recently, molecular markers (von Economo and Koskinas, 1925; Ongur et al., 2003; Zilles et al., 2004). Comparisons of similar classifications among several species provide an evolutionary perspective, and such analyses have identified two broad cortical types. One type, allocortex, has a primitive three-layered form that strongly resembles its homologues in reptiles. Another type, isocortex, lacks such homologues and has a more derived structure characterized by more than three layers (typically six) and a more complex pattern of afferent and efferent projections (Kaas, 1987; Puelles, 2001; Allman et al., 2002; Striedter, 2005). Between allocortex and isocortex, areas sometimes called “transition cortex” have intermediate properties. Using structural neuroimaging of the in vivo developing brain, we explored the possibility that these different kinds of cortex show differing levels of complexity in the trajectories of their growth in childhood and adolescence.

Using computational neuroanatomy, we defined cortical thickness at over 40,000 points throughout the cerebrum in a cohort of 375 healthy children and adolescents. Cortical thickness was chosen as a metric which both captures the columnar architecture of the cortex and is sensitive to developmental change in typically developing and clinical populations (Lerch et al., 2005; O’Donnell et al., 2005; Makris et al., 2006; Shaw et al., 2006a,b; Lu et al., 2007; Sowell et al., 2007).

Most of the children in our cohort had repeated neuroanatomic imaging, and such longitudinal data can be combined with cross-sectional data to model developmental change, with the longitudinal data being particularly informative. For cortical thickness, the simplest trajectory that can be fitted to describe its change over time is a straight line. More complex growth models include distinct phases of increase and decrease in cortical thickness: a quadratic model has two such phases (typically an initial increase which reaches a peak before declining) and a cubic model has three. The complexity of growth may vary across the cerebral cortex, and we sought to explore whether this variation aligned with cytoarchitectural properties.

Derived properties of developmental curves, such as the age of reaching various points of inflection, are frequently used as developmental indices (Tanner et al., 1976; Jolicoeur et al., 1988). For cortical thickness, the age at which peak cortical thickness is reached (the point where increase gives way to decrease in cortical thickness) can be determined for cortical points with either a cubic or quadratic (but not linear) trajectory and, thus, emerges as a potentially useful index of cortical development. We therefore additionally examined the pattern of attaining peak cortical thickness across the cerebrum, to confirm and expand previous observations of a heterochronous sequence, with primary sensory areas attaining peak cortical thickness before polymodal, high-order association areas (Gogtay et al., 2004).

Materials and Methods

Participants.

Three hundred and seventy-five children and adolescents, healthy children with no personal or family history of psychiatric or neurological disorders, had a total of 764 magnetic resonance images. Each subject completed the Childhood Behavior Checklist as a screening tool and then underwent a structured diagnostic interview by a child psychiatrist to rule out any psychiatric or neurological diagnoses (Giedd et al., 1996). Handedness was determined using the PANESS (Physical and Neurological Examination for Soft Signs), and 336 (90%) were predominately right-handed, 20 (5%) predominately left-handed, and 19 (5%) ambidextrous. The mean intelligence quotient (IQ) was 115 (SD, 13) as determined from age appropriate versions of the Wechsler Intelligence Scales (Shaw et al., 2006b). Socioeconomic status (SES) was determined from the Hollingshead Scales and the mean score was 40 (SD, 19) (Hollingshead, 1975). The age range spanned from 3.5 to 33 years, and the age distribution of scans is illustrated in Figure 1. The subjects came from 292 different families; 196 (52%) were male. The age range spanned from 3.5 to 33 years. All subjects had at least one scan (mean age at initial scan, 12.3 years; SD, 5.3); 203 (54.1%) had at least two scans (mean age, 13.8; SD, 4.6); 106 (28.3%) had at least three scans (mean, 15.3; SD, 4.2); and 57 (15.2%) had four or more scans (mean 18, SD 4.5).

 

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Figure 1. 

The age distribution of the data. The age at each scan is indicated by a blue diamond. For each subject, the first scan is always the leftmost; subjects with repeated scans have a horizontal line drawn connecting the age at first scan with the age at later scans.

Neuroimaging.

T1-weighted images with contiguous 1.5 mm axial slices and 2.0 mm coronal slices were obtained using three-dimensional spoiled gradient recalled echo in the steady state on a 1.5-T General Electric (Milwaukee, WI) Signa scanner. Imaging parameters were as follows: echo time, 5 ms; repetition time, 24 ms; flip angle, 45°; acquisition matrix, 256 × 192; number of excitations, 1; and field of view, 24 cm. Head placement was standardized as described previously (Giedd et al., 1999). The same scanner was used throughout the study. The native MRI scans were registered into standardized stereotaxic space using a linear transformation and corrected for nonuniformity artifacts (Sled et al., 1998). The registered and corrected volumes were segmented into white matter, gray matter, CSF, and background using an advanced neural net classifier (Zijdenbos et al., 2002). A surface deformation algorithm was applied which first fits the white matter surface, then expands outward to find the gray matter-CSF intersection defining a known relationship between each vertex of the white matter surface and its gray matter surface counterpart; cortical thickness is defined as the distance between these linked vertices (and measured at 40,962 such vertices) (MacDonald et al., 2000). A 30-mm-bandwidth blurring kernel was applied; this size was chosen on the basis of population simulations which that this bandwidth maximized statistical power while minimizing false positives (Lerch and Evans, 2005). This kernel allows anatomical localization, as 30 mm blurring along the surface using a diffusion smoothing operator preserves cortical topologic features and represents considerably less cortex than the equivalent volumetric Gaussian blurring kernel.

The validity of this automated measure against expert manual neuroanatomical estimation of cortical thickness has been demonstrated previously for selected cortical regions in an adult population (Kabani et al., 2001) We repeated this validation study in our pediatric population in the cortical regions included in the original study (the pre and post central gyri, the superior frontal gyrus, the superior temporal gyrus, the cuneus, the superior parietal lobule and supramarginal gyrus) (Kabani et al., 2001). We also examined regions of particular interest for this study. These were the insula, the orbitofrontal cortex (measured bilaterally in its anterior, posterior, medial, and lateral divisions), and medial cortical regions (the anterior and posterior cingulate, the medial dorsal prefrontal cortex, and the parahippocampal gyrus). Twenty scans were chosen at random from the cohort (from ages 6 through 15). For each brain region the neuroanatomist (N.K.) used image analyses software (MacDonald, 1996) to mark one point or tag on the CSF and gray matter border which represents the outer surface of the cortex, and another point of the gray and white matter border which represents the inner surface of the cortex. The distance between the two tags was calculated, mimicking the algorithm used by the automated tool. For a given tag placed by the neuroanatomist on the outer cortical surface, the closest vertex on the automatically extracted cortical surface was identified and its associated cortical thickness was noted. The output of the manual and automatic methods were compared using a repeated measures ANOVA followed by paired t tests to identify regional differences. There was a significant difference for type of measurement with the automated estimates being larger (mean, 4.62; SE, 0.06) than the manual (mean, 4.41; SE, 0.04; F_(1,684) = 8.8, p = 0.02). There was a significant interaction of the type of measurement and region (F_(35,684) = 2.59, p < 0.001) which was further explored. Overall there was no significant difference between the manual and automated measures in 30 of the 36 regions, with poorer performance noted bilaterally in the precentral gyrus, and in the left postcentral gyrus, and in the middle frontal gyrus, gyrus rectus and the cuneus in the left hemisphere. Notably, only one of these regions lay in an area of particular interest for this study (the left gyrus rectus). There was no correlation between age and the difference between the automated and manual estimates (r = 0.02, p = 0.53). Thus, there was no evidence that the differences between the two metrics had any significant age related bias.

To determine developmental trajectories at each cortical point, mixed model regression analysis was chosen as it permits the inclusion of multiple measurements per person, missing data, and irregular intervals between measurements, thereby increasing statistical power (Pinheiro and Bates, 2000). Our classification of developmental trajectories was based on a step-down model selection procedure: at each cortical point we modeled cortical thickness using a mixed-effects polynomial regression model, testing for cubic, quadratic and linear age effects. If the cubic age effect was not significant at p < 0.05, it was removed and we stepped down to the quadratic model and so on. In this way, we were able to classify the development of each cortical point as being best explained by a cubic, quadratic, or linear function of age. We consider cubic models to be more complex than quadratic, which in turn are held to be more complex than linear models. A random effect for each individual was nested within a random effect for each family, thus accounting for both within-person and within-family dependence. Thus, for cortical points with a cubic model, the kth cortical thickness of the ith individual in the jth family was modeled as thickness_ijk = intercept + d_ij + β₁(age) + β2*(age)**2 + β3*(age)**3 + e_ijk, where d_ij are nested random effects modeling within-person and within family dependence, the intercept and β terms are fixed effects, and e_ijk represents the residual error. Quadratic models lacked the cubic age term, and linear models the cubic and quadratic age terms. The analyses were repeated entering SES and IQ as covariates.

The age at which peak cortical thickness was attained was calculated for cubic and quadratic models from the first order derivatives of the fitted curves.

Results

Throughout most of the lateral frontal, lateral temporal, parietal and occipital isocortex, developmental trajectories are cubic, with a period of initial childhood increase, followed by adolescent decline and then stabilization of cortical thickness in adulthood (Fig. 2). Growth characterized by increase and decrease, but lacking the phase of stabilization within the first three decades of life (a quadratic model) is present in much of the insula and anterior cingulate cortex. A linear trajectory is seen in the posterior orbitofrontal and frontal operculum, portions of the piriform cortex, the medial temporal cortex, subgenual cingulate areas, and medial occipitotemporal cortex. Graphs illustrating individual data points from representative regions with a cubic, quadratic or linear trajectory are shown in Figure 3.

 

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Figure 2. 

Complexity of developmental trajectories throughout the cerebral cortex. The brain maps show the vertices having a cubic (red), quadratic (green) or linear (blue) developmental trajectory. The graphs show the growth pattern for each of these divisions. In order there are dorsal, right lateral, left medial, left lateral, and right medial views. The corpus callosum is blacked out.

 

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Figure 3. 

Graphs showing raw cortical thickness data in blue, with the fitted trajectory superimposed in pink. a–c, The first three images show in order the mean cortical thickness and trajectory for representative regions: the superior frontal gyri, which have a cubic trajectory (a); the portion of the insula which has a quadratic trajectory, seen in green in Figure 5 (b); the portion of the orbitofrontal cortex which has a linear trajectory, seen in blue in Figure 4 (c).

We examined the complexity of developmental trajectories with respect to cortical regions of differing cytoarchitecturonic types, using histological atlases to assign cytoarchitectonic fields (Ongur et al., 2003). This analysis revealed a clear parallel between basic types of cortex and the pattern of cortical development. The orbitofrontal cortex exemplifies the correspondence between cortical types and developmental trajectories (Fig. 4). In the most anterior part of this region, a cubic trajectory characterizes the homotypical (six-layered) isocortex of the frontal pole and lateral orbitofrontal regions. In contrast, most of the cortex on the posterior orbital surface follows relatively simple quadratic and linear growth trajectories. This region has a lamination pattern typical of transitional cortex: compared with homotypical isocortex it has fewer, less well developed layers and lacks the clear concentration of nonpyramidal cells of layer 4, the internal granular layer (Brockhaus, 1940; Mesulam and Mufson, 1982; Ongur et al., 2003). In the most posterior part of this region, linear and quadratic growth characterizes the piriform cortex, a primitive allocortical area that subserves olfaction.

 

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Figure 4. 

A, Complexity of developmental trajectories throughout the orbitofrontal cortex, projected onto a standard brain template. The anterior and lateral orbitofrontal cortex has a cubic fit (red); medial and posterior orbitofrontal cortex has simpler quadratic (green) and linear (blue) trajectories. B, The trajectories are superimposed on a cytoarchitectonic map of the region by Öngür et al. (2003) to illustrate the overlap between the cytoarchitectonic fields and regional differences in trajectories. C, The trajectory of each of the divisions.

Although Figure 4 focuses on the orbitofrontal cortex, the same principles are observed generally, where a transition from isocortex to simpler forms occurs. The results for the medial frontal cortex are similar to those in the orbitofrontal cortex, with cubic growth anteriorly, especially in the homotypical cortex of the medial frontal pole- and linear or quadratic trajectories more posteriorly in regions of dysgranular or agranular architecture (Fig. 5, top). For the insula (Fig. 5, bottom), the pattern is much the same. The anterior insula, with its agranular and poorly laminated cortex, has a linear developmental trajectory. Moving posteriorly to the dysgranular and homotypical insula, there is at first a more complex quadratic fit; still more posteriorly, as the cortex becomes increasingly homotypical, the trajectory becomes cubic. Likewise in the temporal lobe, an allocortical component such as the piriform cortex shows a predominately a linear trajectory. In contrast, the lateral temporal isocortex has a cubic trajectory and transition areas such as the entorhinal and perirhinal regions have quadratic and linear trajectories (Fig. 2). These results are summarized in Table 1. There are some cortical regions where this link between cortical types and developmental trajectories does not hold, most notably in the medial occipitotemporal and the anterior superior temporal areas, both of which are isocortical regions that nonetheless have a linear and quadratic trajectory, respectively. The pattern of results held when SES and IQ were entered as covariates, either separately or together.

 

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Figure 5. 

Top, Detailed views of trajectories in the right medial prefrontal cortex, where isocortical regions have a cubic trajectory, and transitional areas have either a quadratic trajectory (e.g., the agranular and poorly laminated cortex of area 24a in the cingulate gyrus) or a linear decline in thickness (e.g., the thin and largely agranular cortex of the gyrus rectus). Bottom, The right insula shows progressively more complex trajectories moving: the posterior portion has a cubic trajectory (red), the body of the insula has a quadratic fit (green) and the anterior insula has a linear fit (blue). A similar pattern holds for the left insula.

We next determined the age at which peak cortical thickness was attained for all points with either a cubic or quadratic trajectory, using the first order derivative of the fitted curve for each point. A peak age cannot be determined for the points with a linear trajectory. The results are presented as a time-lapse dynamic sequence (supplemental Movies 1, 2, available at www.jneurosci.org as supplemental material), “stills” taken from the movies (Fig. 6), and the estimated age of peak cortical thickness for 56 brain regions (as defined by the ANIMAL segmentation tool).

 

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Figure 6. 

Age of attaining peak cortical thickness across the cerebral cortex. Peak thickness can only be estimated for regions with a cubic or quadratic trajectory and not for regions with linear change (which are indicated with a darker red shade). The changes are illustrated dynamically in supplemental Movies 1 and 2, available at www.jneurosci.org as supplemental material.

To summarize the results, within isocortex, the primary sensory and motor areas generally attain their peak cortical thickness before adjacent secondary areas, and also before other polymodal association areas. In the posterior brain, the first area to reach its peak thickness is the somatic sensory cortex (∼7 years), followed by the occipital poles, containing much of the striate primary visual area (∼7 years on the left, and ∼8 years on the right) and then the remaining parieto-occipital cortex, with polymodal regions (such as the posterior parietal cortex) reaching peak thickness later (∼9–10 years). In the frontal cortex, the primary motor cortex attains peak cortical thickness relatively early (∼9 years), followed by the supplementary motor areas (∼10 years) and most of the frontal pole (∼10 years). High-order cortical areas, such as the dorsolateral prefrontal cortex and cingulate cortex, reach peak thickness last (∼10.5 years). In the medial views, the occipital and frontal poles attain peak thickness early, and then a centripetal wave sweeps from these areas, with the medial prefrontal and cingulate cortex attaining peak thickness last. There is also a marked dorsal to ventral progression of development. Detailed results for each brain regions are given in Table 2.

Discussion

Footnotes

• Received November 30, 2007.
• Revision received February 7, 2008.
• Accepted February 26, 2008.

• This work was supported by the Intramural Research Program of the National Institutes of Health. We thank all the participants in the study and their families.

• The authors declare no competing financial interests.

• Correspondence should be addressed to Philip Shaw, Child Psychiatry Branch, Room 3N202, Building 10, Center Drive, National Institute of Mental Health, Bethesda, MD 20892. [email protected]

References

1. ↵
   1. Allman J,
   2. Hakeem A,
   3. Watson K

   (2002) Two phylogenetic specializations in the human brain. Neuroscientist 8:335–346.

   Abstract/FREE Full Text
2. ↵
   1. Brockhaus H

   (1940) Die cyto-und myleoarchitcktonik des crotex clastralis und des clastrum beim menschen. J Psychol Neurol 49:249–348.

   Search Google Scholar
3. ↵
   1. Brown SM,
   2. Hariri AR

   (2006) Neuroimaging studies of serotonin gene polymorphisms: exploring the interplay of genes, brain, and behavior. Cogn Affect Behav Neurosci 6:44–52.

   Medline
4. ↵
   1. Buckholtz JW,
   2. Meyer-Lindenberg A,
   3. Honea RA,
   4. Straub RE,
   5. Pezawas L,
   6. Egan MF,
   7. Vakkalanka R,
   8. Kolachana B,
   9. Verchinski BA,
   10. Sust S,
   11. Mattay VS,
   12. Weinberger DR,
   13. Callicott JH

   (2007) Allelic variation in RGS4 impacts functional and structural connectivity in the human brain. J Neurosci 27:1584–1593.

   Abstract/FREE Full Text
5. ↵
   1. Chelune GJ,
   2. Baer RA

   (1986) Developmental norms for the Wisconsin Card Sorting test. J Clin Exp Neuropsychol 8:219–228.

   Medline
6. ↵
   1. Chklovskii DB,
   2. Mel BW,
   3. Svoboda K

   (2004) Cortical rewiring and information storage. Nature 431:782–788.

   CrossRefMedline
7. ↵
   1. Diamond A

   (2002) in Principles of frontal lobe function, Normal development of prefrontal cortex from birth to young adulthood: cognitive functions, anatomy and biochemistry, eds Stuss DT, Knight RT (Oxford UP, New York), pp 466–503.

   Search Google Scholar
8. ↵
   1. Evans PD,
   2. Anderson JR,
   3. Vallender EJ,
   4. Choi SS,
   5. Lahn BT

   (2004a) Reconstructing the evolutionary history of microcephalin, a gene controlling human brain size. Hum Mol Genet 13:1139–1145.

   Abstract/FREE Full Text
9. ↵
   1. Evans PD,
   2. Anderson JR,
   3. Vallender EJ,
   4. Gilbert SL,
   5. Malcom CM,
   6. Dorus S,
   7. Lahn BT

   (2004b) Adaptive evolution of ASPM, a major determinant of cerebral cortical size in humans. Hum Mol Genet 13:489–494.

   Abstract/FREE Full Text
10. ↵
    1. Giedd JN,
    2. Snell JW,
    3. Lange N,
    4. Rajapakse JC,
    5. Casey BJ,
    6. Kozuch PL,
    7. Vaituzis AC,
    8. Vauss YC,
    9. Hamburger SD,
    10. Kaysen D,
    11. Rapoport JL

    (1996) Quantitative magnetic resonance imaging of human brain development: ages 4–18. Cereb Cortex 6:551–560.

    Abstract/FREE Full Text
11. ↵
    1. Giedd JN,
    2. Blumenthal J,
    3. Jeffries NO,
    4. Castellanos FX,
    5. Liu H,
    6. Zijdenbos A,
    7. Paus T,
    8. Evans AC,
    9. Rapoport JL

    (1999) Brain development during childhood and adolescence: a longitudinal MRI study. Nat Neurosci 2:861–863.

    CrossRefMedline
12. ↵
    1. Gilbert SL,
    2. Dobyns WB,
    3. Lahn BT

    (2005) Genetic links between brain development and brain evolution. Nat Rev Genet 6:581–590.

    CrossRefMedline
13. ↵
    1. Gogtay N,
    2. Giedd JN,
    3. Lusk L,
    4. Hayashi KM,
    5. Greenstein D,
    6. Vaituzis AC,
    7. Nugent TF III.,
    8. Herman DH,
    9. Clasen LS,
    10. Toga AW,
    11. Rapoport JL,
    12. Thompson PM

    (2004) Dynamic mapping of human cortical development during childhood through early adulthood. Proc Natl Acad Sci USA 101:8174–8179.

    Abstract/FREE Full Text
14. ↵
    1. Gogtay N,
    2. Nugent TF III.,
    3. Herman DH,
    4. Ordonez A,
    5. Greenstein D,
    6. Hayashi KM,
    7. Clasen L,
    8. Toga AW,
    9. Giedd JN,
    10. Rapoport JL,
    11. Thompson PM

    (2006) Dynamic mapping of normal human hippocampal development. Hippocampus 16:664–672.

    CrossRefMedline
15. ↵
    1. Harrison RV,
    2. Gordon KA,
    3. Mount RJ

    (2005) Is there a critical period for cochlear implantation in congenitally deaf children? Analyses of hearing and speech perception performance after implantation. Dev Psychobiol 46:252–261.

    CrossRefMedline
16. ↵
    1. Hensch TK

    (2004) Critical period regulation. Annu Rev Neurosci 27:549–579.

    CrossRefMedline
17. ↵
    1. Hensch TK

    (2005) Critical period plasticity in local cortical circuits. Nat Rev Neurosci 6:877–888.

    CrossRefMedline
18. ↵
    1. Hollingshead AB

    (1975) Four-factor index for social status (Yale UP, New Haven, CT).

    Search Google Scholar
19. ↵
    1. Huizinga M,
    2. Dolan CV,
    3. van der Molen MW

    (2006) Age-related change in executive function: developmental trends and a latent variable analysis. Neuropsychologia 44:2017–2036.

    CrossRefMedline
20. ↵
    1. Huttenlocher PR,
    2. Dabholkar AS

    (1997) Regional differences in synaptogenesis in human cerebral cortex. J Comp Neurol 387:167–178.

    CrossRefMedline
21. ↵
    1. Jacobs R,
    2. Harvey AS,
    3. Anderson V

    (2007) Executive function following focal frontal lobe lesions: impact of timing of lesion on outcome. Cortex 43:792–805.

    CrossRefMedline
22. ↵
    1. Jolicoeur P,
    2. Pontier J,
    3. Pernin MO,
    4. Sempe M

    (1988) A lifetime asymptotic growth curve for human height. Biometrics 44:995–1003.

    CrossRefMedline
23. ↵
    1. Kaas JH

    (1987) The organization of neocortex in mammals: implications for theories of brain function. Annu Rev Psychol 38:129–151.

    CrossRefMedline
24. ↵
    1. Kabani N,
    2. Le Goualher G,
    3. MacDonald D,
    4. Evans AC

    (2001) Measurement of cortical thickness using an automated 3-D algorithm: a validation study. NeuroImage 13:375–380.

    Medline
25. ↵
    1. Kennerley SW,
    2. Walton ME,
    3. Behrens TE,
    4. Buckley MJ,
    5. Rushworth MF

    (2006) Optimal decision making and the anterior cingulate cortex. Nat Neurosci 9:940–947.

    CrossRefMedline
26. ↵
    1. Knudsen EI

    (2004) Sensitive periods in the development of the brain and behavior. J Cogn Neurosci 16:1412–1425.

    CrossRefMedline
27. ↵
    1. Kostovic I,
    2. Rakic P

    (1990) Developmental history of the transient subplate zone in the visual and somatosensory cortex of the macaque monkey and human brain. J Comp Neurol 297:441–470.

    CrossRefMedline
28. ↵
    1. Kostovic I,
    2. Judas M,
    3. Rados M,
    4. Hrabac P

    (2002) Laminar organization of the human fetal cerebrum revealed by histochemical markers and magnetic resonance imaging. Cereb Cortex 12:536–544.

    Abstract/FREE Full Text
29. ↵
    1. Lee JK,
    2. Lee JM,
    3. Kim JS,
    4. Kim IY,
    5. Evans AC,
    6. Kim SI

    (2006) A novel quantitative cross-validation of different cortical surface reconstruction algorithms using MRI phantom. NeuroImage 31:572–584.

    CrossRefMedline
30. ↵
    1. Lenroot RK,
    2. Schmitt JE,
    3. Ordaz SJ,
    4. Wallace GL,
    5. Neale MC,
    6. Lerch JP,
    7. Kendler KS,
    8. Evans AC,
    9. Giedd JN

    (2007) Differences in genetic and environmental influences on the human cerebral cortex associated with development during childhood and adolescence. Hum Brain Mapp, in press.

    Search Google Scholar
31. ↵
    1. Lerch JP,
    2. Evans AC

    (2005) Cortical thickness analysis examined through power analysis and a population simulation. NeuroImage 24:163–173.

    CrossRefMedline
32. ↵
    1. Lerch JP,
    2. Pruessner JC,
    3. Zijdenbos A,
    4. Hampel H,
    5. Teipel SJ,
    6. Evans AC

    (2005) Focal decline of cortical thickness in Alzheimer’s disease identified by computational neuroanatomy. Cereb Cortex 15:995–1001.

    Abstract/FREE Full Text
33. ↵
    1. Levi DM

    (2005) Perceptual learning in adults with amblyopia: a reevaluation of critical periods in human vision. Dev Psychobiol 46:222–232.

    CrossRefMedline
34. ↵
    1. Lewis TL,
    2. Maurer D

    (2005) Multiple sensitive periods in human visual development: evidence from visually deprived children. Dev Psychobiol 46:163–183.

    CrossRefMedline
35. ↵
    1. Lu LH,
    2. Leonard CM,
    3. Thompson PM,
    4. Kan E,
    5. Jolley J,
    6. Welcome SE,
    7. Toga AW,
    8. Sowell ER

    (2007) Normal developmental changes in inferior frontal gray matter are associated with improvement in phonological processing: a longitudinal MRI analysis. Cereb Cortex 17:1092–1099.

    Abstract/FREE Full Text
36. ↵
    1. Luciana M,
    2. Conklin HM,
    3. Hooper CJ,
    4. Yarger RS

    (2005) The development of nonverbal working memory and executive control processes in adolescents. Child Dev 76:697–712.

    CrossRefMedline
37. ↵
    1. Luna B,
    2. Garver KE,
    3. Urban TA,
    4. Lazar NA,
    5. Sweeney JA

    (2004) Maturation of cognitive processes from late childhood to adulthood. Child Development 75:1357–1372.

    CrossRefMedline
38. ↵
    1. MacDonald D

    (1996) MNI-display (McConnell Brain Imaging Center, Montreal Neurological Institute, Montreal).

    Search Google Scholar
39. ↵
    1. MacDonald D,
    2. Kabani N,
    3. Avis D,
    4. Evans AC

    (2000) Automated 3-D extraction of inner and outer surfaces of cerebral cortex from MRI. NeuroImage 12:340–356.

    CrossRefMedline
40. ↵
    1. Makris N,
    2. Biederman J,
    3. Valera EM,
    4. Bush G,
    5. Kaiser J,
    6. Kennedy DN,
    7. Caviness VS,
    8. Faraone SV,
    9. Seidman LJ

    (2006) Cortical thinning of the attention and executive function networks in adults with attention-deficit/hyperactivity disorder. Cereb Cortex 17:1364–1375.

    CrossRefMedline
41. ↵
    1. Mataga N,
    2. Mizuguchi Y,
    3. Hensch TK

    (2004) Experience-dependent pruning of dendritic spines in visual cortex by tissue plasminogen activator. Neuron 44:1031–1041.

    CrossRefMedline
42. ↵
    1. Mesulam MM,
    2. Mufson EJ

    (1982) Insula of the old world monkey. I. Architectonics in the insulo-orbito-temporal component of the paralimbic brain. J Comp Neurol 212:1–22.

    CrossRefMedline
43. ↵
    1. Meyer-Lindenberg A,
    2. Nichols T,
    3. Callicott JH,
    4. Ding J,
    5. Kolachana B,
    6. Buckholtz J,
    7. Mattay VS,
    8. Egan M,
    9. Weinberger DR

    (2006) Impact of complex genetic variation in COMT on human brain function. Mol Psychiatry 11:867–877.

    CrossRefMedline
44. ↵
    1. Narr KL,
    2. Woods RP,
    3. Thompson PM,
    4. Szeszko P,
    5. Robinson D,
    6. Dimtcheva T,
    7. Gurbani M,
    8. Toga AW,
    9. Bilder RM

    (2006) Relationships between IQ and regional cortical gray matter thickness in healthy adults. Cereb Cortex 17:2163–2171.

    CrossRefMedline
45. ↵
    1. O’Donnell S,
    2. Noseworthy MD,
    3. Levine B,
    4. Dennis M

    (2005) Cortical thickness of the frontopolar area in typically developing children and adolescents. NeuroImage 24:948–954.

    CrossRefMedline
46. ↵
    1. Ongur D,
    2. Ferry AT,
    3. Price JL

    (2003) Architectonic subdivision of the human orbital and medial prefrontal cortex. J Comp Neurol 460:425–449.

    CrossRefMedline
47. ↵
    1. Pinheiro JC,
    2. Bates DM

    (2000) Mixed-effects models in S and S-PLUS (Springer, New York).

    Search Google Scholar
48. ↵
    1. Puelles L

    (2001) Thoughts on the development, structure and evolution of the mammalian and avian telencephalic pallium. Philos Trans R Soc Lond B Biol Sci 356:1583–1598.

    Abstract/FREE Full Text
49. ↵
    1. Rolls ET

    (2004) The functions of the orbitofrontal cortex. Brain Cogn 55:11–29.

    CrossRefMedline
50. ↵
    1. Shaw P,
    2. Lerch J,
    3. Greenstein D,
    4. Sharp W,
    5. Clasen L,
    6. Evans A,
    7. Giedd J,
    8. Castellanos FX,
    9. Rapoport J

    (2006a) Longitudinal mapping of cortical thickness and clinical outcome in children and adolescents with attention-deficit/hyperactivity disorder. Arch Gen Psychiatry 63:540–549.

    Abstract/FREE Full Text
51. ↵
    1. Shaw P,
    2. Greenstein D,
    3. Lerch J,
    4. Clasen L,
    5. Lenroot R,
    6. Gogtay N,
    7. Evans A,
    8. Rapoport J,
    9. Giedd J

    (2006b) Intellectual ability and cortical development in children and adolescents. Nature 440:676–679.

    CrossRefMedline
52. ↵
    1. Sled JG,
    2. Zijdenbos AP,
    3. Evans AC

    (1998) A nonparametric method for automatic correction of intensity nonuniformity in MRI data. IEEE Trans Med Imaging 17:87–97.

    CrossRefMedline
53. ↵
    1. Sowell ER,
    2. Thompson PM,
    3. Leonard CM,
    4. Welcome SE,
    5. Kan E,
    6. Toga AW

    (2004) Longitudinal mapping of cortical thickness and brain growth in normal children. J Neurosci 24:8223–8231.

    Abstract/FREE Full Text
54. ↵
    1. Sowell ER,
    2. Peterson BS,
    3. Kan E,
    4. Woods RP,
    5. Yoshii J,
    6. Bansal R,
    7. Xu D,
    8. Zhu H,
    9. Thompson PM,
    10. Toga AW

    (2007) Sex differences in cortical thickness mapped in 176 healthy individuals between 7 and 87 years of age. Cereb Cortex 17:1550–1560.

    Abstract/FREE Full Text
55. ↵
    1. Striedter GF

    (2005) Principles of brain evolution (Sinauer, Sunderland, MA).

    Search Google Scholar
56. ↵
    1. Sur M,
    2. Rubenstein JL

    (2005) Patterning and plasticity of the cerebral cortex. Science 310:805–810.

    Abstract/FREE Full Text
57. ↵
    1. Tanner JM,
    2. Whitehouse RH,
    3. Marubini E,
    4. Resele LF

    (1976) The adolescent growth spurt of boys and girls of the Harpenden growth study. Ann Hum Biol 3:109–126.

    CrossRefMedline
58. ↵
    1. Taylor WD,
    2. Zuchner S,
    3. Payne ME,
    4. Messer DF,
    5. Doty TJ,
    6. MacFall JR,
    7. Beyer JL,
    8. Krishnan KRR

    (2007) The COMT Val158Met polymorphism and temporal lobe morphometry in healthy adults. Psychiatry Res 155:173–177.

    CrossRefMedline
59. ↵
    1. Thompson PM,
    2. Cannon TD,
    3. Narr KL,
    4. van Erp T,
    5. Poutanen VP,
    6. Huttunen M,
    7. Lonnqvist J,
    8. Standertskjold-Nordenstam CG,
    9. Kaprio J,
    10. Khaledy M,
    11. Dail R,
    12. Zoumalan CI,
    13. Toga AW

    (2001) Genetic influences on brain structure. Nature Neuroscience 4:1253–1258.

    CrossRefMedline
60. ↵
    1. von Economo C,
    2. Koskinas GN

    (1925) Die dytoarchitektonik der hirnrinde des erwachsenen menschen (Springer, Berlin).

    Search Google Scholar
61. ↵
    1. Yakovlev PI,
    2. Lecours AR

    (1967) in Regional development of the brain in early life, The myelinogenetic cycles of regional maturation of the brain, ed Minokowski A (Blackwell Scientific, Oxford).

    Search Google Scholar
62. ↵
    1. Zijdenbos AP,
    2. Forghani R,
    3. Evans AC

    (2002) Automatic “pipeline” analysis of 3-D MRI data for clinical trials: application to multiple sclerosis. IEEE Trans Med Imaging 21:1280–1291.

    CrossRefMedline
63. ↵
    1. Zilles K,
    2. Palomero-Gallagher N,
    3. Schleicher A

    (2004) Transmitter receptors and functional anatomy of the cerebral cortex. J Anat 205:417–432.

    CrossRefMedline
64. ↵
    1. Zinkstok J,
    2. Schmitz N,
    3. van Amelsvoort T,
    4. de Win M,
    5. van den Brink W,
    6. Baas F,
    7. Linszen D

    (2006) The COMT val158met polymorphism and brain morphometry in healthy young adults. Neurosci Lett 405:34–39.

    CrossRefMedline