Holoprosencephaly - Topologic variations in a Liveborn series: A general model based upon MRI analysis

Ts Takahashi; S. Kinsman; N. Makris; E. Grant; C. Haselgrove; S. Mcinerney; D. N. Kennedy; Ta Takahashi; K. Fredrickson; S. Mori; V. S. Caviness

doi:10.1023/B:NEUR.0000029646.75645.9c

Holoprosencephaly - Topologic variations in a Liveborn series: A general model based upon MRI analysis

Ts Takahashi, S. Kinsman, N. Makris, E. Grant, C. Haselgrove, S. Mcinerney, D. N. Kennedy, Ta Takahashi, K. Fredrickson, S. Mori, V. S. Caviness

School of Medicine

Research output: Contribution to journal › Article › peer-review

9 Scopus citations

Abstract

We present an MRI-based anatomic analysis of a series of 9 human brains, representing lobar, semilobar and alobar forms of holoprosencephaly. The analysis of these variable forms of the malformation is based upon a topologic systematics established in a prior analysis of a homogeneous set of semilobar malformations. This systematics has the dual advantage that it serves both as a uniform reference for qualitative description and as a quantitative descriptive base for mathematical correlations between parameters of topology and of growth and development. Within this systematics, the prosencephalic midline is divided from caudal to rostral into diencephalic (DD - right and left, subthalamus through suprachiasmatic junction with telencephalon), telencephalic (TT - right and left, suprachiasmatic border of telencephalon midline to hippocampal commissure) and diencephalic - telencephalic (DT - right and left - hippocampal commissure through temporal limb of choroid fissure) segments. The topologic abnormality of the initial semilobar series was expressed in an orderly rostral to caudal gradient along the TT segment. In each malformation, normal midline topology began with a small posterior corpus callosum. Although the topologic anomaly in the present series invariably also involved the TT segment, this involvement was not continuous and was variably associated with anomalies of the DD in 6 and unilaterally of the DT in 1 brain. In the present as well as with the earlier series of HPE malformations but not in "normative brains," total telencephalic growth is strongly correlated with the length of the midline telencephalic segment. We propose that this system of analysis will be sensitive to the developmental stage and locus of expression of genetic and non-genetic determinants of the formal origin of HPE. For all of the present series, karyotype anlyses were normal. Mutations in the Shh and Zic2 genes were excluded in 2 cases.

Original language	English (US)
Pages (from-to)	23-35
Number of pages	13
Journal	Journal of Neurocytology
Volume	33
Issue number	1 SPEC. ISS.
DOIs	https://doi.org/10.1023/B:NEUR.0000029646.75645.9c
State	Published - Jan 2004

ASJC Scopus subject areas

Anatomy
General Neuroscience
Histology
Cell Biology

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Takahashi, T., Kinsman, S., Makris, N., Grant, E., Haselgrove, C., Mcinerney, S., Kennedy, D. N., Takahashi, T., Fredrickson, K., Mori, S., & Caviness, V. S. (2004). Holoprosencephaly - Topologic variations in a Liveborn series: A general model based upon MRI analysis. Journal of Neurocytology, 33(1 SPEC. ISS.), 23-35. https://doi.org/10.1023/B:NEUR.0000029646.75645.9c

@article{cda9112599d54f47a59e5ba019380e34,

title = "Holoprosencephaly - Topologic variations in a Liveborn series: A general model based upon MRI analysis",

abstract = "We present an MRI-based anatomic analysis of a series of 9 human brains, representing lobar, semilobar and alobar forms of holoprosencephaly. The analysis of these variable forms of the malformation is based upon a topologic systematics established in a prior analysis of a homogeneous set of semilobar malformations. This systematics has the dual advantage that it serves both as a uniform reference for qualitative description and as a quantitative descriptive base for mathematical correlations between parameters of topology and of growth and development. Within this systematics, the prosencephalic midline is divided from caudal to rostral into diencephalic (DD - right and left, subthalamus through suprachiasmatic junction with telencephalon), telencephalic (TT - right and left, suprachiasmatic border of telencephalon midline to hippocampal commissure) and diencephalic - telencephalic (DT - right and left - hippocampal commissure through temporal limb of choroid fissure) segments. The topologic abnormality of the initial semilobar series was expressed in an orderly rostral to caudal gradient along the TT segment. In each malformation, normal midline topology began with a small posterior corpus callosum. Although the topologic anomaly in the present series invariably also involved the TT segment, this involvement was not continuous and was variably associated with anomalies of the DD in 6 and unilaterally of the DT in 1 brain. In the present as well as with the earlier series of HPE malformations but not in {"}normative brains,{"} total telencephalic growth is strongly correlated with the length of the midline telencephalic segment. We propose that this system of analysis will be sensitive to the developmental stage and locus of expression of genetic and non-genetic determinants of the formal origin of HPE. For all of the present series, karyotype anlyses were normal. Mutations in the Shh and Zic2 genes were excluded in 2 cases.",

author = "Ts Takahashi and S. Kinsman and N. Makris and E. Grant and C. Haselgrove and S. Mcinerney and Kennedy, {D. N.} and Ta Takahashi and K. Fredrickson and S. Mori and Caviness, {V. S.}",

note = "Funding Information: This work was supported by grants from the Carter Foundation, NIH Grant DA 09467, by Human Brain Project Grant NS34189, by USPHS grant NS12005, and by grants from the Fairway Trust and the Giovanni Armenise Harvard Foundation for Advanced Scientific Research.",

year = "2004",

month = jan,

doi = "10.1023/B:NEUR.0000029646.75645.9c",

language = "English (US)",

volume = "33",

pages = "23--35",

journal = "Journal of Neurocytology",

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TY - JOUR

T1 - Holoprosencephaly - Topologic variations in a Liveborn series

T2 - A general model based upon MRI analysis

AU - Takahashi, Ts

AU - Kinsman, S.

AU - Makris, N.

AU - Grant, E.

AU - Haselgrove, C.

AU - Mcinerney, S.

AU - Kennedy, D. N.

AU - Takahashi, Ta

AU - Fredrickson, K.

AU - Mori, S.

AU - Caviness, V. S.

N1 - Funding Information: This work was supported by grants from the Carter Foundation, NIH Grant DA 09467, by Human Brain Project Grant NS34189, by USPHS grant NS12005, and by grants from the Fairway Trust and the Giovanni Armenise Harvard Foundation for Advanced Scientific Research.

PY - 2004/1

Y1 - 2004/1

N2 - We present an MRI-based anatomic analysis of a series of 9 human brains, representing lobar, semilobar and alobar forms of holoprosencephaly. The analysis of these variable forms of the malformation is based upon a topologic systematics established in a prior analysis of a homogeneous set of semilobar malformations. This systematics has the dual advantage that it serves both as a uniform reference for qualitative description and as a quantitative descriptive base for mathematical correlations between parameters of topology and of growth and development. Within this systematics, the prosencephalic midline is divided from caudal to rostral into diencephalic (DD - right and left, subthalamus through suprachiasmatic junction with telencephalon), telencephalic (TT - right and left, suprachiasmatic border of telencephalon midline to hippocampal commissure) and diencephalic - telencephalic (DT - right and left - hippocampal commissure through temporal limb of choroid fissure) segments. The topologic abnormality of the initial semilobar series was expressed in an orderly rostral to caudal gradient along the TT segment. In each malformation, normal midline topology began with a small posterior corpus callosum. Although the topologic anomaly in the present series invariably also involved the TT segment, this involvement was not continuous and was variably associated with anomalies of the DD in 6 and unilaterally of the DT in 1 brain. In the present as well as with the earlier series of HPE malformations but not in "normative brains," total telencephalic growth is strongly correlated with the length of the midline telencephalic segment. We propose that this system of analysis will be sensitive to the developmental stage and locus of expression of genetic and non-genetic determinants of the formal origin of HPE. For all of the present series, karyotype anlyses were normal. Mutations in the Shh and Zic2 genes were excluded in 2 cases.

AB - We present an MRI-based anatomic analysis of a series of 9 human brains, representing lobar, semilobar and alobar forms of holoprosencephaly. The analysis of these variable forms of the malformation is based upon a topologic systematics established in a prior analysis of a homogeneous set of semilobar malformations. This systematics has the dual advantage that it serves both as a uniform reference for qualitative description and as a quantitative descriptive base for mathematical correlations between parameters of topology and of growth and development. Within this systematics, the prosencephalic midline is divided from caudal to rostral into diencephalic (DD - right and left, subthalamus through suprachiasmatic junction with telencephalon), telencephalic (TT - right and left, suprachiasmatic border of telencephalon midline to hippocampal commissure) and diencephalic - telencephalic (DT - right and left - hippocampal commissure through temporal limb of choroid fissure) segments. The topologic abnormality of the initial semilobar series was expressed in an orderly rostral to caudal gradient along the TT segment. In each malformation, normal midline topology began with a small posterior corpus callosum. Although the topologic anomaly in the present series invariably also involved the TT segment, this involvement was not continuous and was variably associated with anomalies of the DD in 6 and unilaterally of the DT in 1 brain. In the present as well as with the earlier series of HPE malformations but not in "normative brains," total telencephalic growth is strongly correlated with the length of the midline telencephalic segment. We propose that this system of analysis will be sensitive to the developmental stage and locus of expression of genetic and non-genetic determinants of the formal origin of HPE. For all of the present series, karyotype anlyses were normal. Mutations in the Shh and Zic2 genes were excluded in 2 cases.

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Holoprosencephaly - Topologic variations in a Liveborn series: A general model based upon MRI analysis

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