Your search keyword '"Parisi, Melissa A."' showing total 26 results

1. The National Institutes of Health INvestigation of Co‐occurring conditions across the Lifespan to Understand Down syndromE (INCLUDE) Project: Accelerating research discoveries for people with Down syndrome across the lifespan.

Author

Bardhan, Sujata, Li, Huiqing, Tarver, Erika, Schramm, Charlene, Brown, Marishka, Garcia, Linda, Schwartz, Bryanna, Mazzucco, Anna, Natarajan, Nikila, Walsh, Elizabeth, Ryan, Laurie, Pearson, Gail, and Parisi, Melissa A.

Published

2024

2. Moving the Needle Toward Equity: What NIH Is Doing to Promote Diversity, Inclusion, and Accessibility in Research on Intellectual and Developmental Disabilities.

Author

King, Tracy M. and Parisi, Melissa A.

Subjects

DEVELOPMENTAL disabilities, INTELLECTUAL disabilities, BEHAVIORAL research, MEDICAL research, CHILDREN with developmental disabilities, PEOPLE with disabilities, NEEDLES & pins

Abstract

As a major funder of research on intellectual and developmental disabilities (IDD), NIH has a broad view of the profound impact of cultural and structural barriers on the characteristics of IDD study populations and the composition of the IDD research workforce. While long overdue, multiple efforts are currently underway across NIH aimed at addressing these barriers and increasing meaningful representation in biomedical and behavioral research. [ABSTRACT FROM AUTHOR]

Published

2023

3. When is the best time to screen and evaluate for treatable genetic disorders?: A lifespan perspective.

Author

Parisi, Melissa A., Caggana, Michele, Cohen, Jennifer L., Gold, Nina B., Morris, Jill A., Orsini, Joseph J., Urv, Tiina K., and Wasserstein, Melissa P.

Published

2023

4. Gene‐targeted therapies: Overview and implications.

Author

Brooks, P J, Urv, Tiina K., and Parisi, Melissa A.

Published

2023

5. Are we prepared to deliver gene‐targeted therapies for rare diseases?

Author

Yu, Timothy W., Kingsmore, Stephen F., Green, Robert C., MacKenzie, Tippi, Wasserstein, Melissa, Caggana, Michele, Gold, Nina B., Kennedy, Annie, Kishnani, Priya S., Might, Matthew, Brooks, Phillip J., Morris, Jill A., Parisi, Melissa A., and Urv, Tiina K.

Published

2023

6. Newborn screening research sponsored by the NIH: From diagnostic paradigms to precision therapeutics.

Author

Minear, Mollie A., Phillips, Megan N., Kau, Alice, and Parisi, Melissa A.

Published

2022

7. Growth in Joubert syndrome: Growth curves and physical measurements with correlation to genotype and hepatorenal disease in 170 individuals.

Author

Knoll, Jasmine, Altintas, Burak, Gahl, William A., Parisi, Melissa, and Gunay‐Aygun, Meral

Abstract

Joubert syndrome (JS) is a genetically heterogenous disorder of nonmotile cilia with a characteristic "molar tooth sign" on axial brain imaging. Clinical features can include developmental delay, kidney failure, liver disease, and retinal dystrophy. Prospective growth and measurement data on 170 individuals with JS were collected, including parental measurements, birth measurements, and serial measures when available. Analysis of growth parameters in the context of hepatorenal disease, genotype, and other features was performed on 100 individuals assessed at the National Institutes of Health Clinical Center. Individuals with JS had shorter stature despite normal growth velocity and were shorter than predicted for mid‐parental height. Individuals were lighter in weight, resulting in a normal body mass index (BMI). Head circumference was larger, averaging 1.9 Z‐scores above height. At birth, head circumference was proportional to length. Individuals with variants in CPLANE1 had a larger head circumference compared to other genotypes; individuals with evidence of liver disease had lower weight and BMI; and individuals with polydactyly had shorter height. Here we present growth curves and physical measurements for Joubert syndrome based on the largest collection of individuals with this disorder to aid in clinical management and diagnosis. [ABSTRACT FROM AUTHOR]

Published

2022

8. Systematic analysis of physical examination characteristics of 94 individuals with Joubert syndrome: Keys to suspecting the diagnosis.

Author

Forsyth, RaeLynn, Parisi, Melissa A., Altintas, Burak, Malicdan, May Christine, Vilboux, Thierry, Knoll, Jasmine, Brooks, Brian P., Zein, Wadih M., Gahl, William A., Toro, Camilo, and Gunay‐Aygun, Meral

Published

2022

9. Healthcare recommendations for Joubert syndrome.

Author

Bachmann‐Gagescu, Ruxandra, Dempsey, Jennifer C., Bulgheroni, Sara, Chen, Maida L., D'Arrigo, Stefano, Glass, Ian A., Heller, Theo, Héon, Elise, Hildebrandt, Friedhelm, Joshi, Nirmal, Knutzen, Dana, Kroes, Hester Y., Mack, Stephen H., Nuovo, Sara, Parisi, Melissa A., Snow, Joseph, Summers, Angela C., Symons, Jordan M., Zein, Wadih M., and Boltshauser, Eugen

Abstract

Joubert syndrome (JS) is a recessive neurodevelopmental disorder defined by a characteristic cerebellar and brainstem malformation recognizable on axial brain magnetic resonance imaging as the "Molar Tooth Sign". Although defined by the neurological features, JS is associated with clinical features affecting many other organ systems, particularly progressive involvement of the retina, kidney, and liver. JS is a rare condition; therefore, many affected individuals may not have easy access to subspecialty providers familiar with JS (e.g., geneticists, neurologists, developmental pediatricians, ophthalmologists, nephrologists, hepatologists, psychiatrists, therapists, and educators). Expert recommendations can enable practitioners of all types to provide quality care to individuals with JS and know when to refer for subspecialty care. This need will only increase as precision treatments targeting specific genetic causes of JS emerge. The goal of these recommendations is to provide a resource for general practitioners, subspecialists, and families to maximize the health of individuals with JS throughout the lifespan. [ABSTRACT FROM AUTHOR]

Published

2020

10. Note from the editors.

Author

Urv, Tiina K. and Parisi, Melissa A.

Published

2023

11. Characteristics of Liver Disease in 100 Individuals With Joubert Syndrome Prospectively Evaluated at a Single Center.

Author

Strongin, Anna, Heller, Theo, Doherty, Dan, Glass, Ian A., Parisi, Melissa A., Bryant, Joy, Choyke, Peter, Turkbey, Baris, Daryanani, Kailash, Yildirimli, Deniz, Vemulapalli, Meghana, Mullikin, Jim C., Malicdan, May C., Vilboux, Thierry, Gahl, William A., Gunay-Aygun, Meral, and NISC Comparative Sequencing Program

Published

2018

12. Joubert syndrome: neuroimaging findings in 110 patients in correlation with cognitive function and genetic cause.

Author

Poretti, Andrea, Snow, Joseph, Summers, Angela C., Tekes, Aylin, Huisman, Thierry A. G. M., Aygun, Nafi, Carson, Kathryn A., Doherty, Dan, Parisi, Melissa A., Toro, Camilo, Yildirimli, Deniz, Vemulapalli, Meghana, Mullikin, Jim C., Cullinane, Andrew R., Vilboux, Thierry, Gahl, William A., and Gunay-Aygun, Meral

Abstract

Background Joubert syndrome is a clinically and genetically heterogeneous ciliopathy. Neuroimaging findings have not been systematically evaluated in a large cohort of patients with Joubert syndrome in correlation with molecular genetic cause and cognitive function. Methods Brain MRI of 110 patients with Joubert syndrome was included in this study. A comprehensive evaluation of brain MRI studies for infratentorial and supratentorial morphological abnormalities was performed. Genetic cause was identified by whole-exome sequencing, and cognitive functions were assessed with age-appropriate neurocognitive tests in a subset of patients. Results The cerebellar hemispheres were enlarged in 18% of the patients, mimicking macrocerebellum. The posterior fossa was enlarged in 42% of the patients, resembling Dandy-Walker malformation. Abnormalities of the brainstem, such as protuberance at the ventral contour of the midbrain, were present in 66% of the patients. Abnormalities of the supratentorial brain were present in approximately one-third of the patients, most commonly malrotation of the hippocampi. Mild ventriculomegaly, which typically did not require shunting, was present in 23% of the patients. No correlation between neuroimaging findings and molecular genetic cause was apparent. A novel predictor of outcome was identified; the more severe the degree of vermis hypoplasia, the worse the neurodevelopmental outcome was. Conclusions The spectrum of neuroimaging findings in Joubert syndrome is wide. Neuroimaging does not predict the genetic cause, but may predict the neurodevelopmental outcome. A high degree of vermis hypoplasia correlates with worse neurodevelopmental outcome. This finding is important for prognostic counselling in Joubert syndrome. [ABSTRACT FROM AUTHOR]

Published

2017

13. Neuropsychological phenotypes of 76 individuals with Joubert syndrome evaluated at a single center.

Author

Summers, Angela C., Snow, Joseph, Wiggs, Edythe, Liu, Alexander G., Toro, Camilo, Poretti, Andrea, Zein, Wadih M., Brooks, Brian P., Parisi, Melissa A., Inati, Sara, Doherty, Dan, Vemulapalli, Meghana, Mullikin, Jim C., Vilboux, Thierry, Gahl, William A., and Gunay‐Aygun, Meral

Abstract

Joubert syndrome (JS) is a genetically heterogeneous ciliopathy characterized by hypo-dysplasia of the cerebellar vermis, a distinct hindbrain/midbrain malformation (molar tooth sign), and intellectual disability. We evaluated the neuropsychological profiles of 76 participants with JS in the context of molecular genetics and clinical covariates. Evaluations included neuropsychological testing, structured parental interviews, DNA sequencing, brain magnetic resonance imaging (MRI), electroencephalography (EEG), ophthalmologic examination, and assessment for renal and hepatic disease. On average, participants manifested Full Scale Intelligence Quotients (FSIQ) in the moderately to profoundly low range ( M = 64.3 ± 15.3). Of the Wechsler index scores, verbal comprehension was least affected and processing speed was most affected. Receptive language was rated as better than expressive language on the Vineland Adaptive Behavior Scales-Second Edition. Those with abnormal EEG had a significantly lower FSIQ ( n = 15; M = 50.7 ± 12.9) compared to participants with normal EEG ( n = 39; M = 64.7 ± 16.3; p = .004). Participants taking psychiatric medications manifested a lower FSIQ ( n = 20; M = 54.8 ± 13.2) than those not taking them ( n = 42; M = 65.0 ± 17.2; p = .022). These correlations were also present in the TMEM67-related JS sub-cohort ( n = 14). Based on parental assessment, psychiatric and behavioral problems were significantly more common than in the general population for all measures ( p < .004 for all). The majority (65%) of individuals with JS have some degree of intellectual disability. Abnormal EEG is associated with lower neuropsychological function. Processing speed is a weakness, while verbal comprehension and receptive language are relative strengths. These findings may guide parents, teachers, therapists, and doctors to determine appropriate therapies, accommodations, and academic goals for individuals with JS. [ABSTRACT FROM AUTHOR]

Published

2017

14. Ambiguous genitalia: What prenatal genetic testing is practical?

Author

Adam, Margaret P., Fechner, Patricia Y., Ramsdell, Linda A., Badaru, Angela, Grady, Richard E., Pagon, Roberta A., McCauley, Elizabeth, Cheng, Edith Y., Parisi, Melissa A., and Shnorhavorian, Margarett

Abstract

Concern for ambiguous genitalia or chromosome-phenotype discordance detected in a prenatal setting has increased over the last two decades. Practitioners faced with this prenatal finding have a variety of genetic tests available to them; however, it is unclear to what extent prenatal testing for disorders of sex development (DSD) is useful or practical. We undertook a retrospective review of the medical records of 140 individuals evaluated through the DSD clinic at Seattle Children's Hospital with birthdates from 01/01/1994 through 08/16/2011 to determine the rate of prenatal detection of ambiguous genitalia in individuals with DSD, what prenatal diagnostic workup was undertaken, and the postnatal outcome, including whether a postnatal genetic diagnosis was confirmed. Of all 140 subjects, 34 (24%) were identified prenatally. The most common postnatal diagnoses were penoscrotal hypospadias with transposition of the scrotum with no known genetic cause (24/140; 17%) and 21-hydroxylase deficiency (20/140; 14%). Apart from these, no single diagnosis comprised more than a few cases. Prenatal diagnostic testing varied widely, from no tests to multiple molecular tests with amniotic fluid hormone concentrations. In the absence of other fetal anomalies or growth retardation on ultrasound, prenatal karyotype with fluorescence in situ hybridization for the SRY gene is the most useful test when ambiguous genitalia is suspected. Further prenatal testing for Smith-Lemli-Opitz syndrome in 46,XY individuals and congenital adrenal hyperplasia in 46,XX individuals may be considered. However, targeted molecular testing for rare DSD conditions in the absence of a family history of DSD has a low yield. © 2012 Wiley Periodicals, Inc. [ABSTRACT FROM AUTHOR]

Published

2012

15. Genotypeephenotype correlation in CC2D2A—related Joubert syndrome reveals an association with ventriculomegaly and seizures.

Author

Bachmann-Gagescu, Ruxandra, Ishak, Gisele E., Dempsey, Jennifer C., Adkins, Jonathan, O'Day, Diana, Phelps, Ian G., Gunay-Aygun, Meral, Kline, Antonie D., Szczaluba, Krzysztof, Martorell, Loreto, Alswaid, Abdulrahman, Alrasheed, Shatha, Pai, Shashidhar, Izatt, Louise, Ronan, Anne, Parisi, Melissa A., Mefford, Heather, Glass, Ian, and Doherty, Dan

Subjects

SPASMS, POLYDACTYLY, RETINAL degeneration, KIDNEY diseases, MOLECULAR diagnosis

Abstract

Background Joubert syndrome (JS) is a ciliopathy characterised by a distinctive brain malformation (the 'molar tooth sign'), developmental delay, abnormal eye movements and abnormal breathing pattern. Retinal dystrophy, cystic kidney disease, liver fibrosis and polydactyly are variably present, resulting in significant phenotypic heterogeneity and overlap with other ciliopathies. JS is also genetically heterogeneous, resulting from mutations in 13 genes. These factors render clinical/molecular diagnosis and management challenging. CC2D2A mutations are a relatively common cause of JS and also cause Meckel syndrome. The clinical consequences of CC2D2A mutations in patients with JS have been incompletely reported. Methods Subjects with JS from 209 families were evaluated to identify mutations in CC2D2A. Clinical and imaging features in subjects with CC2D2A mutations were compared with those in subjects without CC2D2A mutations and reports in the literature. Results 10 novel CC2D2A mutations in 20 subjects were identified; a summary is provided of all published CC2D2A mutations. Subjects with CC2D2A-related JS were more likely to have ventriculomegaly (p<0.0001) and seizures (p=0.024) than subjects without CC2D2A mutations. No mutation-specific genotype—phenotype correlations could be identified, but the findings confirm the observation that mutations that cause CC2D2A-related JS are predicted to be less deleterious than mutations that cause CC2D2A-related Meckel syndrome. Missense variants in the coiled-coil and C2 domains, as well as the C-terminal region, identify these regions as important for the biological mechanisms underlying JS. Conclusions CC2D2A testing should be prioritised in patients with JS and ventriculomegaly and/or seizures. Patients with CC2D2A-related JS should be monitored for hydrocephalus and seizures. [ABSTRACT FROM AUTHOR]

Published

2012

16. Fanconi anemia-like presentation in an infant with constitutional deletion of 21q including the RUNX1 gene.

Author

Click, Eleanor S., Cox, Barbara, Olson, Susan B., Grompe, Markus, Akkari, Yassmine, Moreau, Lisa A., Shimamura, Akiko, Sternen, Darci L., Liu, Yajuan J., Leppig, Kathleen A., Matthews, Dana C., and Parisi, Melissa A.

Abstract

We describe a newborn female with a de novo interstitial deletion of chromosome 21q21.1-22.12 including the RUNX1 gene who had developmental delay, multiple congenital anomalies, tetralogy of Fallot, anemia, and chronic thromobocytopenia requiring frequent platelet transfusions from birth. Because of her physical and hematologic abnormalities, she was tested for Fanconi anemia (FA). Lymphocytes and fibroblasts from this patient demonstrated increased chromosome breakage with exposure to the clastogen mitomycin C, but not, in contrast to most FA patients, to diepoxybutane. Further testing by Western analysis and complementation testing did not show a defect in the function of known Fanconi proteins. Her constitutional deletion was later found to span 13.2 Mb by chromosome microarray analysis, encompassing the RUNX1 gene that has been implicated in thrombocytopenia and predisposition to acute myelogenous leukemia (AML) when in the haploinsufficient state. We compare her phenotype to other individuals with similar 21q deletions and thrombocytopenia, as well as those with FA. We suggest that deletion of RUNX1 or another critical gene within the deleted region may result in chromosomal instability similar to that seen in FA. © 2011 Wiley-Liss, Inc. [ABSTRACT FROM AUTHOR]

Published

2011

17. Mutation analysis of NPHP6/CEP290 in patients with Joubert syndrome and Senior—Løken syndrome.

Author

Helou, Juliana, Otto, Edgar A., Attanasio, Massimo, Allen, Susan J., Parisi, Melissa A., Glass, Ian, Utsch, Boris, Hashmi, Seema, Fazzi, Elisa, Omran, Heymut, O'Toole, John F., Sayer, John A., and Hildebrandt, Friedhelm

Subjects

RESEARCH, KIDNEY diseases, RETINAL diseases, RETINAL degeneration, EUGENICS

Abstract

Background: Nephronophthisis (NPHP) is an autosomal recessive cystic kidney disease that constitutes the most common genetic cause of renal failure in the first three decades of life. Using positional cloning, six genes (NPHP1-6) have been identified as mutated in NPHP. In Joubert syndrome (JBTS), NPHP may be associated with cerebellar vermis aplasia/hypoplasia, retinal degeneration and mental retardation. In Senior-Løken syndrome (SLSN), NPHP is associated with retinal degeneration. Recently, mutations in NPHP6/CEP290 were identified as a new cause of JBTS. Methods: Mutational analysis was performed on a worldwide cohort of 75 families with SLSN, 99 families with JBTS and 21 families with isolated nephronophthisis. Results: Six novel and six known truncating mutations, one known missense mutation and one novel 3 bp pair in-frame deletion were identified in a total of seven families with JBTS, two families with SLSN and one family with isolated NPHP. [ABSTRACT FROM AUTHOR]

Published

2007

18. Mutations in the gene encoding the basal body protein RPGRIP1L, a nephrocystin-4 interactor, cause Joubert syndrome.

Author

Arts, Heleen H., Doherty, Dan, van Beersum, Sylvia E. C., Parisi, Melissa A., Letteboer, Stef J. F., Gorden, Nicholas T., Peters, Theo A., Märker, Tina, Voesenek, Krysta, Kartono, Aileen, Ozyurek, Hamit, Farin, Federico M., Kroes, Hester Y., Wolfrum, Uwe, Brunner, Han G., Cremers, Frans P. M., Glass, Ian A., Knoers, Nine V. A. M., and Roepman, Ronald

Subjects

GENETIC mutation, GENETIC code, PROTEIN-protein interactions, BLINDNESS, HUMAN abnormalities, KIDNEY diseases, GENETIC polymorphisms

Abstract

Protein-protein interaction analyses have uncovered a ciliary and basal body protein network that, when disrupted, can result in nephronophthisis (NPHP), Leber congenital amaurosis, Senior-Løken syndrome (SLSN) or Joubert syndrome (JBTS). However, details of the molecular mechanisms underlying these disorders remain poorly understood. RPGRIP1-like protein (RPGRIP1L) is a homolog of RPGRIP1 (RPGR-interacting protein 1), a ciliary protein defective in Leber congenital amaurosis. We show that RPGRIP1L interacts with nephrocystin-4 and that mutations in the gene encoding nephrocystin-4 (NPHP4) that are known to cause SLSN disrupt this interaction. RPGRIP1L is ubiquitously expressed, and its protein product localizes to basal bodies. Therefore, we analyzed RPGRIP1L as a candidate gene for JBTS and identified loss-of-function mutations in three families with typical JBTS, including the characteristic mid-hindbrain malformation. This work identifies RPGRIP1L as a gene responsible for JBTS and establishes a central role for cilia and basal bodies in the pathophysiology of this disorder. [ABSTRACT FROM AUTHOR]

Published

2007

19. Joubert syndrome (and related disorders) (OMIM 213300).

Author

Parisi, Melissa A, Doherty, Dan, Chance, Phillip F, and Glass, Ian A

Subjects

EYE movements, ATAXIA, RETINAL degeneration, KIDNEY diseases, RESPIRATION, MAGNETIC resonance imaging

Abstract

Joubert syndrome (JS) and related disorders are characterized by the ‘molar tooth sign’ (cerebellar vermis hypoplasia and brainstem anomalies) on MRI, hypotonia, developmental delay, ataxia, irregular breathing pattern and abnormal eye movements. Combinations of additional features such as polydactyly, ocular coloboma, retinal dystrophy, renal disease, hepatic fibrosis, encephalocele, and other brain malformations define clinical sub-types. Recent identification of the NPHP1, AHI1, and CEP290 genes has started to reveal the molecular basis of JS, which may implicate the primary cilium in these disorders. Additional genes remain to be identified.European Journal of Human Genetics (2007) 15, 511–521. doi:10.1038/sj.ejhg.5201648; published online 21 March 2007 [ABSTRACT FROM AUTHOR]

Published

2007

20. A case of true hermaphroditism reveals an unusual mechanism of twinning.

Author

Souter, Vivienne, Parisi, Melissa, Nyholt, Dale, Kapur, Raj, Henders, Anjali, Opheim, Kent, Gunther, Daniel, Mitchell, Michael, Glass, Ian, and Montgomery, Grant

Subjects

TWINS, CELLS, BLOOD, FIBROBLASTS, DNA, GENES, SEXUAL dysfunction, IN situ hybridization, BIOPSY

Abstract

Traditionally twins are classified as dizygous or fraternal and monozygous or identical (Hall Twinning, 362, and 735–743). We report a rare case of 46,XX/46,XY twins: Twin A presented with ambiguous genitalia and Twin B was a phenotypically normal male. These twins demonstrate a third, previously unreported mechanism for twinning. The twins underwent initial investigation with 17-hydroxyprogesterone and testosterone levels, pelvic ultrasound and diagnostic laparoscopy. Cytogenetic analysis was performed on peripheral blood cells and skin fibroblasts. Histological examination and Fluorescence in situ hybridization studies on touch imprints were performed on gonadal biopsies. DNA analysis using more than 6,000 DNA markers was performed on skin fibroblast samples from the twins and on peripheral blood samples from both parents. Twin A was determined to be a true hermaphrodite and Twin B an apparently normal male. Both twins had a 46,XX/46,XY chromosome complement in peripheral lymphocytes, skin fibroblasts, and gonadal biopsies. The proportion of XX to XY cells varied between the twins and the tissues evaluated. Most significantly the twins shared 100% of maternal alleles and approximately 50% of paternal alleles in DNA analysis of skin fibroblasts. The twins are chimeric and share a single genetic contribution from their mother but have two genetic contributions from their father thus supporting the existence of a third, previously unreported type of twinning. [ABSTRACT FROM AUTHOR]

Published

2007

21. Variable presentation of nemaline myopathy: Novel mutation of alpha actin gene.

Author

Bouldin, Anthony A., Parisi, Melissa A., Laing, Nigel, Patterson, Kathleen, and Gospe, Sidney M.

Abstract

Nemaline myopathy is a rare disorder of varying severity and genetic etiology. We present two cases, a father and son, with a novel missense mutation in the alpha actin gene. Both have a history of early motor impairment, with the son's course being considerably more severe. This pair illustrates the clinical variability of nemaline myopathy, highlighting the possible influence of environmental and epigenetic factors. Implications for the current classification system and prognosis are discussed. Muscle Nerve, 2006 [ABSTRACT FROM AUTHOR]

Published

2007

22. Prenatal diagnosis in pregnancies at risk for Joubert syndrome by ultrasound and MRI.

Author

Doherty, Dan, Glass, Ian A., Siebert, Joseph R., Strouse, Peter J., Parisi, Melissa A., Shaw, Dennis W. W., Chance, Phillip F., Barr, Mason, and Nyberg, David

Abstract

Objectives To describe the prenatal imaging findings in fetuses at risk for Joubert syndrome (JS), review the literature and propose a protocol for prenatal diagnosis of JS using ultrasound and MRI. Methods We reviewed prenatal ultrasound and fetal MRI studies in two pregnancies at 25% recurrence risk for JS and correlated these findings with gross neuropathology in one affected fetus. Results While abnormalities such as occipital encephalocele or enlarged cisterna magna have been identified before mid-trimester, the definitive diagnosis of JS, based on core cerebellar findings, has only been possible after 17 weeks' gestation. Conclusions With longitudinal monitoring, it is possible to diagnose JS in at-risk pregnancies before 24 weeks' gestation. On the basis of our data and review of the literature, we propose a protocol for monitoring pregnancies at risk for JS, utilizing serial ultrasounds combined with fetal MRI at 20-22 weeks' gestation to maximize the accuracy of prenatal diagnosis. Copyright © 2005 John Wiley & Sons, Ltd. [ABSTRACT FROM AUTHOR]

Published

2005

23. Hox11L1 Expression by Precursors of Enteric Smooth Muscle: An Alternative Explanation for Megacecum in Hox11L1-I- Mice.

Author

Kapur, P., Clarke, Christine M., Doggett, Barbara, Taylor, Brian E., Baldessari, Audrey, Parisi, Melissa A., and Howe, Douglas G.

Subjects

SMOOTH muscle, NERVOUS system, URINARY organs, TRANSCRIPTION factors, MESSENGER RNA, NEURONS

Abstract

Previous studies have focused on expression of Hoxl ILl in enteric neurons as the explanation loi" intestinal and uiinai bladder dysniotilily observed in mice that do not have the transcription factor. However", Ho\I loll is also expressed transiently in endo-, mcso-, and ectodermai cells of the most caudal embryo during gastrulation. We sought to more fully eharaeterize the fates of these cells because they might help explain the pathogenesis of lethal pseudo-obstruction in HoxllLl-nulI mice. The Cre recombinase cDNA was introduced into the Hoxl ILl locus, and expression of the "knock-in" allele was used to activate the Rosa26R, P-galactosidase reporter gene in cells with ongoing Hoxl ILl transcription and their descendants. During gastrulation, Rosa26R activation was observed in progenitors of caudal somatic and visceral ceils, including enteric smooth muscle. Expression in enteric neural precursors appeared much later. Analysis of endogenous Hoxl 1 LI mRNA in ancuronal segments of large intestine that were grafted under the ix-nai capsule indicated that the early activation of Hox 11L1 in visceral mesoderm was transient and ceased before colonization of the large intestine by neural progenitors. Mice homozygous for the Cre allele died shortly after weaning, with cecal and proximal colonic distention but without overt anatomic defects that might represent maldevelopment of the visceral mesoderm. Our findings expand the range of possible functions of Hoxl ILl to include activation of an as yet unknown developmental program in visceral smooth muscle and allow the possibility that intestinal dysmotility in HoxllLI-null animals may not be a primary neural disorder. [ABSTRACT FROM AUTHOR]

Published

2005

24. Cerebral and Cerebellar Motor Activation Abnormalities in a Subject With Joubert Syndrome: Functional Magnetic Resonance Imaging (MRI) Study.

Author

Parisi, Melissa A., Pinter, Joseph D., Glass, Ian A., Field, Katherine, Maria, Bernard L., Chance, Phillip K, Mahurin, Roderick K., and Cramer, Steven C.

Subjects

MUSCLE hypotonia in children, ATAXIA, PYRAMIDAL tract, BRAIN, RADIOGRAPHY, BRAIN stem

Abstract

Joubert syndrome is an autosomal recessive disorder characterized by hypotonia, ataxia, developmental delay, and a distinctive hindbrain malformation involving the cerebellum and brain stem, visualized radiographically on magnetic resonance imaging (MRI) as the "molar tooth sign." In postmortem brains from subjects with Joubert syndrome, there is an apparent absence of decussation of both corticospinal and superior cerebellar tracts, although the functional significance has not been elucidated. We sought to explore the cerebral and cerebellar activation pattern elicited by finger topping in an adolescent with Joubert syndrome and in a normal control subject using functional MRI. In contrast to the typical highly lateralized activation seen in our control subject, the subject with Joubert syndrome demonstrated striking bilateral activation of the sensorimotor and cerebellar cortex. Although our functional MRI data do not indicate a clear absence of decussation, the abnormal activation pattern observed suggests altered brain functional organization in relation to anatomic differences. Malformation of the hindbrain could result in recruitment of alternative pathways, similar to what has been observed following ischémie injury to the developing or mature central nervous system. (J Child Neural 2004;19:214-218). [ABSTRACT FROM AUTHOR]

Published

2004

25. The spectrum and evolution of phenotypic findings in PTEN mutation positive cases of Bannayan-Riley-Ruvalcaba syndrome.

Author

Parisi, Melissa A., Dinulos, Mary Beth, Leppig, Kathleen A., Sybert, Virginia P., Eng, Charis, and Hudgins, Louanne

Subjects

LETTERS to the editor, TUMORS

Abstract

Presents a letter to the editor about Bannayan-Riley-Ruvalcaba syndrome.

Published

2001

26. Outcome After Surgical Repair of Junctional Epidermolysis Bullosa–Pyloric Atresia Syndrome: A Report of 3 Cases and Review of the Literature.

Author

Dank, Jan P., Kim, Susan, Parisi, Melissa A., Brown, Tod, Smith, Lynne T., Waldhausen, John, and Sybert, Virginia P.

Subjects

SYNDROMES in children, SURGERY, CHILDREN, EPIDERMOLYSIS bullosa, PYLORUS diseases

Abstract

Background: Junctional epidermolysis bullosapyloric atresia syndrome is recognized as a distinct autosomal recessive entity. Affected infants present with skin fragility and inability to feed due to intestinal obstruction. Despite successful surgical repair of the anatomical defect, the outcome is poor owing to poor feeding, malabsorption, failure to thrive, and sepsis. Observations: In 70 cases of intestinal obstruction and epidermolysis bullosa reported in the medical literature and the 3 reported here, surgical intervention was attempted 51 times. In all except 16 infants, death occurred before age 11 months (mean age, 70 days). Renal involvement and continued failure to thrive accompanied the skin disease in survivors, who ranged in age from 30 days to 16 years (mean age, 4.0 years). Conclusions: The poor prognosis of this condition must be considered when decisions are made regarding surgical correction. Attempting surgical correction may be warranted in individual circumstances, but withholding surgical intervention and providing palliative support is an acceptable alternative. [ABSTRACT FROM AUTHOR]

Published

1999