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7. Dysregulation of the chromatin environment leads to differential alternative splicing as a mechanism of disease in a human model of autism spectrum disorder

Author

Leung, Calvin S, primary, Rosenzweig, Shoshana J, additional, Yoon, Brian, additional, Marinelli, Nicholas A, additional, Hollingsworth, Ethan W, additional, Maguire, Abbie M, additional, Cowen, Mara H, additional, Schmidt, Michael, additional, Imitola, Jaime, additional, Gamsiz Uzun, Ece D, additional, and Lizarraga, Sofia B, additional

Published
2023
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8. Clinical features of patients with MTAP-deleted bladder cancer

Author

De Souza, Andre L, Mega, Anthony E, Douglass, John, Olszewski, Adam J, Gamsiz Uzun, Ece D, Uzun, Alper, Chou, Charissa, Duan, Fenghai, Wang, Jinyu, Ali, Amin, Golijanin, Dragan J, Holder, Sheldon L, Lagos, Galina G, Safran, Howard, El-Deiry, Wafik S, and Carneiro, Benedito A

Subjects
Original Article
Abstract

Advanced urothelial carcinoma continues to have a dismal prognosis despite several new therapies in the last 5 years. FGFR2 and FGFR3 mutations and fusions, PD-L1 expression, tumor mutational burden, and microsatellite instability are established predictive biomarkers in advanced urothelial carcinoma. Novel biomarkers can optimize the sequencing of available treatments and improve outcomes. We describe herein the clinical and pathologic features of patients with an emerging subtype of bladder cancer characterized by deletion of the gene MTAP encoding the enzyme S-Methyl-5’-thioadenosine phosphatase, a potential biomarker of response to pemetrexed. We performed a retrospective analysis of 61 patients with advanced urothelial carcinoma for whom demographics, pathologic specimens, next generation sequencing, and clinical outcomes were available. We compared the frequency of histology variants, upper tract location, pathogenic gene variants, tumor response, progression free survival (PFS) and overall survival (OS) between patients with tumors harboring MTAP deletion (MTAP-del) and wild type tumors (MTAP-WT). A propensity score matching of 5 covariates (age, gender, presence of variant histology, prior surgery, and prior non-muscle invasive bladder cancer) was calculated to compensate for disparity when comparing survival in these subgroups. Non-supervised clustering analysis of differentially expressed genes between MTAP-del and MTAP-WT urothelial carcinomas was performed. MTAP-del occurred in 19 patients (31%). Tumors with MTAP-del were characterized by higher prevalence of squamous differentiation (47.4 vs 11.9%), bone metastases (52.6 vs 23.5%) and lower frequency of upper urinary tract location (5.2% vs 26.1%). Pathway gene set enrichment analysis showed that among the genes upregulated in the MTAP-del cohort, at least 5 were linked to keratinization (FOXN1, KRT33A/B, KRT84, RPTN) possibly contributing to the higher prevalence of squamous differentiation. Alterations in the PIK3 and MAPK pathways were more frequent when MTAP was deleted. There was a trend to inferior response to chemotherapy among MTAP-del tumors, but no difference in the response to immune checkpoint inhibitors or enfortumab. Median progression free survival after first line therapy (PFS1) was 5.5 months for patients with MTAP-WT and 4.5 months for patients with MTAP-del (HR = 1.30; 95% CI, 0.64-2.63; P = 0.471). There was no difference in the time from metastatic diagnosis to death (P = 0.6346). Median OS from diagnosis of localized or de novo metastatic disease was 16 months (range 1.5-60, IQR 8-26) for patients with MTAP-del and 24.5 months (range 3-156, IQR 16-48) for patients with MTAP-WT (P = 0.0218), suggesting that time to progression to metastatic disease is shorter in MTAP-del patients. Covariates did not impact significantly overall survival on propensity score matching. In conclusion, MTAP -del occurs in approximately 30% of patients with advanced urothelial carcinoma and defines a subgroup of patients with aggressive features, such as squamous differentiation, frequent bone metastases, poor response to chemotherapy, and shorter time to progression to metastatic disease.

Published
2023

9. Dysregulation of The Chromatin Environment Leads to Differential Alternative Splicing as A Mechanism Of Disease In a Human Model of Autism Spectrum Disorders

Author

Leung, Calvin S., primary, Rosenzweig, Shoshanna, additional, Yoon, Brian, additional, Marinelli, Nicholas A., additional, Hollingsworth, Ethan W., additional, Maguire, Abbie M., additional, Cowen, Mara M., additional, Schmidt, Michael, additional, Imitola, Jaime, additional, Gamsiz Uzun, Ece D., additional, and Lizarraga, Sofia B., additional

Published
2022
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10. Additional file 2 of Somatic mutations in collagens are associated with a distinct tumor environment and overall survival in gastric cancer

Author

Brodsky, Alexander S., Khurana, Jay, Guo, Kevin S., Wu, Elizabeth Y., Yang, Dongfang, Siddique, Ayesha S., Wong, Ian Y., Gamsiz Uzun, Ece D., and Resnick, Murray B.

Abstract

Additional file 2 : Table S2. MutSig 2CV v3.1 analysis of significantly mutated collagen genes in STAD TCGA cohort. Data downloaded from Firebrowse.

Published
2022
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11. Additional file 6 of Somatic mutations in collagens are associated with a distinct tumor environment and overall survival in gastric cancer

Author

Brodsky, Alexander S., Khurana, Jay, Guo, Kevin S., Wu, Elizabeth Y., Yang, Dongfang, Siddique, Ayesha S., Wong, Ian Y., Gamsiz Uzun, Ece D., and Resnick, Murray B.

Abstract

Additional file 6 : Figure S1. Alteration frequencies of collagens in ACRG and HK/Pfizer datasets. A. Alteration frequencies of sequenced collagens in other stomach cancer cohorts. B. Kaplan-Meier analysis of COl11A1, COL5, COL4, COL6 mutations in the ACRG targeted sequencing dataset compared to the same set of collagen genes in the TCGA cohort. Figure S2. Survival analysis of somatic mutations in each collagen gene. A. Kaplan Maier analysis of tumors with any type of mutation in each collagen gene across the whole STAD TCGA cohort. Tumors with the designated collagen mutation are in red. Wild-type tumors are in blue. P-values determined by log-rank test. B. Kaplan Maier analysis of tumors with truncation mutations in each collagen gene across the whole STAD TCGA cohort. C. Kaplan Maier analysis of tumors with any type of mutation in each collagen gene in MSIH cases. D. Kaplan Maier analysis of tumors with truncation mutation in each collagen gene in MSIH cases. Figure S3. Identification of combinations of collagens genes associated with overall survival relative to background. A. All mutations across the whole TCGA cohort. B. Representative examples of combinations of 2 collagens associated with overall survival. C. Combinations of all mutations in MSS tumors only. D. Combinations of all mutations in MSIH tumors only. E. Example of collagen genes with truncation mutations most frequently associated with overall survival when combined, classify MSIH tumors into high and low overall survival risk. Figure S4. Collagen mutations have MSIH and MSS context dependent differences in overall survival. Mutations in COL5A3 and COL14A1 have different associations in MSIH and MSS tumors even though the total number of mutations is similar. Figure S5. MSIH and MSS tumors have distinct microenvironments in TCGA. A. MSI status was associated with outcome in ACRG but not in TCGA. B. Comparison of MSIH and MSS stomach tumors by pre-ranked GSEA reveals differences in expression. Each heatmap plots the Normalized Enrichment Scores (NES) from the GSEA. NABA ECM gene sets were expressed higher in MSS tumors compared to MSIH tumors. Many immune cell expression signatures including cytotoxic cells were expressed higher in MSIH tumors compared to MSS tumors. B cells were expressed higher in MSS tumors. The majority of cancer hallmark expression signatures were expressed significantly higher in MSIH tumors compared to MSS tumors. Figure S6. Pre-ranked GSEA of collagen mutation combinations in Table S4 for the whole TCGA STAD cohort shows consistent impact for each mutation combination. A. Hallmarks for combinations with both missense and truncation mutations. B. The NABA and immune signature genes sets for combinations with both missense and truncation mutations. C. Hallmark, NABA, and immune signature gene sets for combinations with just truncation mutations. D. Clustering of hallmark gene sets for tumors with missense mutations only in the whole TCGA cohort showed significant difference for the EMT hallmark relative to overall survival. P-value calculated by Kolmogorov-Smirnov. Figure S7. In MSS cases, pre-ranked GSEA of tumors with either a missense or truncation mutation combination as listed in Table S4 show impact of collagen mutations on pathways some of which are correlated with overall survival. A. For all mutations in MSS cases, some hallmarks such as EMT were associated with overall survival as shown in the heat map and box plot. P-value calculated by Kolmogorov-Smirnov. B. NABA ECM and immune signature gene sets in MSS tumors. Basement membrane and macrophage signature gene sets were among the gene sets most associated with overall survival, showing consistent downregulation in tumors with mutant collagens and higher expression in wild-type tumors. P-value calculated by Kolmogorov-Smirnov. Figure S8. In MSIH cases, pre-ranked GSEA of tumors with either a missense or truncation mutation combination as listed in Table S4 show impact of collagen mutations on pathways some of which are correlated with overall survival. A. Clustering of hallmark gene sets partitions tumors with collagen combinations by overall survival. Box plot shows the significant difference in the EMT hallmark as defined by combinations associated with high or low risk of overall survival. B. NABA gene sets showing large differences in Basement Membrane and ECM Affiliated gene sets relative to overall survival. C. Immune cell signature gene sets showing large difference in Tregs and Macrophage expression signatures. P-value calculated by Kolmogorov-Smirnov. Figure S9. In MSIH cases, pre-ranked GSEA of tumors with only missense mutation combinations as listed in Table S4 show impact of collagen mutations on pathways some of which are correlated with overall survival. A. Hallmark gene sets. B. NABA ECM sets. C. Immune cell gene signatures. P-value calculated by Kolmogorov-Smirnov. Figure S10. In MSIH cases, pre-ranked GSEA of tumors with only truncation mutation combinations as listed in Table S4 show impact of collagen mutations on pathways some of which are correlated with overall survival. A. Hallmark gene sets. B. NABA ECM and immune cell signature gene sets. P-value calculated by Kolmogorov-Smirnov. Figure S11. COL7A1 is expressed in some tumor cells in STAD. Representative images of COL7A1 protein and RNA expression in stomach adenocarcinoma. A. Immunohistochemistry (A, C, E) and in situ hybridization (B, D, F) for COL7. Stromal localization in C, E, D, and F, and mixed stromal and carcinoma localization (at white arrows; A, B). B. Higher magnification of panels A and B from S7A showing expression by IHC in panel A and ISH in panel B of COL7A1 in epithelial regions. The arrow shows ISH signal in tumor cells. C. Representative images at higher power of COL7A1 protein expression by IHC in the epithelium and stroma. D. Representative image of COL7A1 protein expression in normal human skin. Note the line of expression in the ECM between the dermal and epidermal layers (red arrow). Cells expressing COL7A1 show cytoplasmic signal as they are overexpressing COL7A1 to be secreted to form the ���anchorage��� line. Figure S12. Comparison of pathological germline and somatic mutations in STAD in three collagens. Comparison of the distribution of mutations across each gene and a lollipop plot mapping the somatic mutations to the protein domains. A. COL1A1 and COL1A2. B. COL4A1 and COL4A2. C. COL5A1 and COL5A2.

Published
2022
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12. Additional file 1 of Somatic mutations in collagens are associated with a distinct tumor environment and overall survival in gastric cancer

Author

Brodsky, Alexander S., Khurana, Jay, Guo, Kevin S., Wu, Elizabeth Y., Yang, Dongfang, Siddique, Ayesha S., Wong, Ian Y., Gamsiz Uzun, Ece D., and Resnick, Murray B.

Subjects
digestive, oral, and skin physiology
Abstract

Additional file 1 : Table S1. Collagen family for collagens of interest in stomach cancer.

Published
2022
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13. Additional file 5 of Somatic mutations in collagens are associated with a distinct tumor environment and overall survival in gastric cancer

Author

Brodsky, Alexander S., Khurana, Jay, Guo, Kevin S., Wu, Elizabeth Y., Yang, Dongfang, Siddique, Ayesha S., Wong, Ian Y., Gamsiz Uzun, Ece D., and Resnick, Murray B.

Subjects
education
Abstract

Additional file 5 : Table S5. Summary of COL7A1 protein expression in stomach tumors from Rhode Island Hospital as assessed by immunohistochemical staining.

Published
2022
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15. Human neurons from Christianson syndrome iPSCs reveal mutation-specific responses to rescue strategies

Author

Lizarraga, Sofia B., primary, Ma, Li, additional, Maguire, Abbie M., additional, van Dyck, Laura I., additional, Wu, Qing, additional, Ouyang, Qing, additional, Kavanaugh, Brian C., additional, Nagda, Dipal, additional, Livi, Liane L., additional, Pescosolido, Matthew F., additional, Schmidt, Michael, additional, Alabi, Shanique, additional, Cowen, Mara H., additional, Brito-Vargas, Paul, additional, Hoffman-Kim, Diane, additional, Gamsiz Uzun, Ece D., additional, Schlessinger, Avner, additional, Jones, Richard N., additional, and Morrow, Eric M., additional

Published
2021
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18. Autism Heterogeneity in a Densely Sampled U.S. Population: Results From the First 1,000 Participants in the RI‐CART Study.

Author

McCormick, Carolyn E. B., Kavanaugh, Brian C., Sipsock, Danielle, Righi, Giulia, Oberman, Lindsay M., Moreno De Luca, Daniel, Gamsiz Uzun, Ece D., Best, Carrie R., Jerskey, Beth A., Quinn, Joanne G., Jewel, Susan B., Wu, Pei‐Chi, McLean, Rebecca L., Levine, Todd P., Tokadjian, Hasmik, Perkins, Kayla A., Clarke, Elaine B., Dunn, Brittany, Gerber, Alan H., and Tenenbaum, Elena J.

Abstract

The objective of this study was to establish a large, densely sampled, U.S. population‐based cohort of people with autism spectrum disorder (ASD). The Rhode Island Consortium for Autism Research and Treatment (RI‐CART) represents a unique public‐private‐academic collaboration involving all major points of service for families in Rhode Island affected by ASD. Diagnosis was based on direct behavioral observation via the Autism Diagnostic Observation Schedule, Second Edition. For the first 1,000 participants, ages ranged from 21 months to 64 years. Using Geographic Information System and published prevalence rates, the overall cohort is estimated to represent between 20% and 49% of pediatric age persons in Rhode Island with ASD, with demographics representative of U.S. Census. We observed a high rate of co‐occurring medical and psychiatric conditions in affected individuals. Among the most prominent findings of immediate clinical importance, we found that females received a first diagnosis of ASD at a later age than males, potentially due to more advanced language abilities in females with ASD. In summary, this is the first analysis of a large, population‐based U.S. cohort with ASD. Given the depth of sampling, the RI‐CART study reflects an important new resource for studying ASD in a representative U.S. population. Psychiatric and medical comorbidities in ASD constitute a substantial burden and warrant adequate attention as part of overall treatment. Our study also suggests that new strategies for earlier diagnosis of ASD in females may be warranted. Autism Res 2020, 13: 474–488. © 2020 International Society for Autism Research, Wiley Periodicals, Inc. Lay Summary The Rhode Island Consortium for Autism Research and Treatment (RI‐CART) represents a unique public‐private‐academic collaboration involving all major points of service for families in Rhode Island affected by autism spectrum disorder (ASD). In this article, we provide results from the first 1,000 participants, estimated to represent >20% of affected families in the state. Importantly, we find a later age at first diagnosis of ASD in females, which potentially calls attention to the need for improved early diagnosis in girls. Also, we report a high rate of co‐occurring medical and psychiatric conditions in affected individuals. [ABSTRACT FROM AUTHOR]

Published
2020
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19. Human neurons from Christianson syndrome iPSCs reveal allele-specific responses to rescue strategies

Author

Lizarraga, Sofia B., primary, Maguire, Abbie M., additional, Ma, Li, additional, van Dyck, Laura I., additional, Wu, Qing, additional, Nagda, Dipal, additional, Livi, Liane L., additional, Pescosolido, Matthew F., additional, Schmidt, Michael, additional, Alabi, Shanique, additional, Cowen, Mara H., additional, Brito-Vargas, Paul, additional, Hoffman-Kim, Diane, additional, Gamsiz Uzun, Ece D., additional, Schlessinger, Avner, additional, Jones, Richard N., additional, and Morrow, Eric M., additional

Published
2018
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22. Clinical features of patients with MTAP -deleted bladder cancer.

Author

De Souza AL, Mega AE, Douglass J, Olszewski AJ, Gamsiz Uzun ED, Uzun A, Chou C, Duan F, Wang J, Ali A, Golijanin DJ, Holder SL, Lagos GG, Safran H, El-Deiry WS, and Carneiro BA

Abstract

Advanced urothelial carcinoma continues to have a dismal prognosis despite several new therapies in the last 5 years. FGFR2 and FGFR3 mutations and fusions, PD-L1 expression, tumor mutational burden, and microsatellite instability are established predictive biomarkers in advanced urothelial carcinoma. Novel biomarkers can optimize the sequencing of available treatments and improve outcomes. We describe herein the clinical and pathologic features of patients with an emerging subtype of bladder cancer characterized by deletion of the gene MTAP encoding the enzyme S-Methyl-5'-thioadenosine phosphatase, a potential biomarker of response to pemetrexed. We performed a retrospective analysis of 61 patients with advanced urothelial carcinoma for whom demographics, pathologic specimens, next generation sequencing, and clinical outcomes were available. We compared the frequency of histology variants, upper tract location, pathogenic gene variants, tumor response, progression free survival (PFS) and overall survival (OS) between patients with tumors harboring MTAP deletion ( MTAP -del) and wild type tumors ( MTAP -WT). A propensity score matching of 5 covariates (age, gender, presence of variant histology, prior surgery, and prior non-muscle invasive bladder cancer) was calculated to compensate for disparity when comparing survival in these subgroups. Non-supervised clustering analysis of differentially expressed genes between MTAP -del and MTAP -WT urothelial carcinomas was performed. MTAP -del occurred in 19 patients (31%). Tumors with MTAP -del were characterized by higher prevalence of squamous differentiation (47.4 vs 11.9%), bone metastases (52.6 vs 23.5%) and lower frequency of upper urinary tract location (5.2% vs 26.1%). Pathway gene set enrichment analysis showed that among the genes upregulated in the MTAP -del cohort, at least 5 were linked to keratinization (FOXN1, KRT33A/B, KRT84, RPTN) possibly contributing to the higher prevalence of squamous differentiation. Alterations in the PIK3 and MAPK pathways were more frequent when MTAP was deleted. There was a trend to inferior response to chemotherapy among MTAP -del tumors, but no difference in the response to immune checkpoint inhibitors or enfortumab. Median progression free survival after first line therapy (PFS1) was 5.5 months for patients with MTAP -WT and 4.5 months for patients with MTAP -del (HR = 1.30; 95% CI, 0.64-2.63; P = 0.471). There was no difference in the time from metastatic diagnosis to death (P = 0.6346). Median OS from diagnosis of localized or de novo metastatic disease was 16 months (range 1.5-60, IQR 8-26) for patients with MTAP-del and 24.5 months (range 3-156, IQR 16-48) for patients with MTAP-WT (P = 0.0218), suggesting that time to progression to metastatic disease is shorter in MTAP-del patients. Covariates did not impact significantly overall survival on propensity score matching. In conclusion, MTAP -del occurs in approximately 30% of patients with advanced urothelial carcinoma and defines a subgroup of patients with aggressive features, such as squamous differentiation, frequent bone metastases, poor response to chemotherapy, and shorter time to progression to metastatic disease., Competing Interests: None., (AJCR Copyright © 2023.)

Published
2023

23. VarStack: a web tool for data retrieval to interpret somatic variants in cancer.

Author

Howard M, Kane B, Lepry M, Stey P, Ragavendran A, and Gamsiz Uzun ED

Subjects
Computational Biology, Databases, Genetic, Humans, Information Storage and Retrieval, Internet, Software, Neoplasms genetics, User-Computer Interface
Abstract

Advances in tumor genome sequencing created an urgent need for bioinformatics tools to support the interpretation of the clinical significance of the variants detected. VarStack is a web tool which is a base to retrieve somatic variant data relating to cancer from existing databases. VarStack incorporates data from several publicly available databases and presents them with an easy-to-navigate user interface. It currently supports data from the Catalogue of Somatic Mutations in Cancer, gnomAD, cBioPortal, ClinVar, OncoKB, CiViC and UCSC Genome Browser. It retrieves the data from these databases and returns them back to the user in a fraction of the time it would take to manually navigate each site independently. Users submit a variant with a gene symbol, peptide change and coding sequence change. They may select a variety of tumor-specific studies in cBioPortal to search through in addition to their original query. The results from the databases are presented in tabs. Users can export the results as an Excel file. VarStack also has the batch search feature in which the user can submit a list of variants and download an Excel file with the data from the databases. With the batch search and data download options, users can easily incorporate VarStack into their workflow or tools. VarStack saves time by providing somatic variant information to the user from multiple databases in an easy-to-export and interpretable format. VarStack is freely available under https://varstack.brown.edu., (© The Author(s) 2020. Published by Oxford University Press.)

Published
2020
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24. Autism Heterogeneity in a Densely Sampled U.S. Population: Results From the First 1,000 Participants in the RI-CART Study.

Author

McCormick CEB, Kavanaugh BC, Sipsock D, Righi G, Oberman LM, Moreno De Luca D, Gamsiz Uzun ED, Best CR, Jerskey BA, Quinn JG, Jewel SB, Wu PC, McLean RL, Levine TP, Tokadjian H, Perkins KA, Clarke EB, Dunn B, Gerber AH, Tenenbaum EJ, Anders TF, Sheinkopf SJ, and Morrow EM

Subjects
Adolescent, Adult, Autism Spectrum Disorder physiopathology, Child, Child, Preschool, Cohort Studies, Comorbidity, Female, Humans, Infant, Male, Middle Aged, Prevalence, Registries, Rhode Island epidemiology, Social Behavior, Young Adult, Autism Spectrum Disorder epidemiology, Autism Spectrum Disorder psychology
Abstract

The objective of this study was to establish a large, densely sampled, U.S. population-based cohort of people with autism spectrum disorder (ASD). The Rhode Island Consortium for Autism Research and Treatment (RI-CART) represents a unique public-private-academic collaboration involving all major points of service for families in Rhode Island affected by ASD. Diagnosis was based on direct behavioral observation via the Autism Diagnostic Observation Schedule, Second Edition. For the first 1,000 participants, ages ranged from 21 months to 64 years. Using Geographic Information System and published prevalence rates, the overall cohort is estimated to represent between 20% and 49% of pediatric age persons in Rhode Island with ASD, with demographics representative of U.S. Census. We observed a high rate of co-occurring medical and psychiatric conditions in affected individuals. Among the most prominent findings of immediate clinical importance, we found that females received a first diagnosis of ASD at a later age than males, potentially due to more advanced language abilities in females with ASD. In summary, this is the first analysis of a large, population-based U.S. cohort with ASD. Given the depth of sampling, the RI-CART study reflects an important new resource for studying ASD in a representative U.S. population. Psychiatric and medical comorbidities in ASD constitute a substantial burden and warrant adequate attention as part of overall treatment. Our study also suggests that new strategies for earlier diagnosis of ASD in females may be warranted. Autism Res 2020, 13: 474-488. © 2020 International Society for Autism Research, Wiley Periodicals, Inc. LAY SUMMARY: The Rhode Island Consortium for Autism Research and Treatment (RI-CART) represents a unique public-private-academic collaboration involving all major points of service for families in Rhode Island affected by autism spectrum disorder (ASD). In this article, we provide results from the first 1,000 participants, estimated to represent >20% of affected families in the state. Importantly, we find a later age at first diagnosis of ASD in females, which potentially calls attention to the need for improved early diagnosis in girls. Also, we report a high rate of co-occurring medical and psychiatric conditions in affected individuals., (© 2020 International Society for Autism Research, Wiley Periodicals, Inc.)

Published
2020
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25. Mixed Neurodevelopmental and Neurodegenerative Pathology in Nhe6 -Null Mouse Model of Christianson Syndrome.

Author

Xu M, Ouyang Q, Gong J, Pescosolido MF, Pruett BS, Mishra S, Schmidt M, Jones RN, Gamsiz Uzun ED, Lizarraga SB, and Morrow EM

Subjects
Aging pathology, Animals, Animals, Newborn, Disease Models, Animal, Female, Male, Mice, Inbred C57BL, Mice, Knockout, Microglia pathology, Organ Size, Sodium-Hydrogen Exchangers genetics, Ataxia pathology, Brain growth & development, Brain pathology, Epilepsy pathology, Genetic Diseases, X-Linked pathology, Intellectual Disability pathology, Microcephaly pathology, Nerve Degeneration pathology, Ocular Motility Disorders pathology, Sodium-Hydrogen Exchangers deficiency
Abstract

Christianson syndrome (CS) is an X-linked disorder resulting from loss-of-function mutations in SLC9A6 , which encodes the endosomal Na + /H + exchanger 6 (NHE6). Symptoms include early developmental delay, seizures, intellectual disability, nonverbal status, autistic features, postnatal microcephaly, and progressive ataxia. Neuronal development is impaired in CS, involving defects in neuronal arborization and synaptogenesis, likely underlying diminished brain growth postnatally. In addition to neurodevelopmental defects, some reports have supported neurodegenerative pathology in CS with age. The objective of this study was to determine the nature of progressive changes in the postnatal brain in Nhe6 -null mice. We examined the trajectories of brain growth and atrophy in mutant mice from birth until very old age (2 yr). We report trajectories of volume changes in the mutant that likely reflect both brain undergrowth as well as tissue loss. Reductions in volume are first apparent at 2 mo, particularly in the cerebellum, which demonstrates progressive loss of Purkinje cells (PCs). We report PC loss in two distinct Nhe6 -null mouse models. More widespread reductions in tissue volumes, namely, in the hippocampus, striatum, and cortex, become apparent after 2 mo, largely reflecting delays in growth with more limited tissue losses with aging. Also, we identify pronounced glial responses, particularly in major fiber tracts such as the corpus callosum, where the density of activated astrocytes and microglia are substantially increased. The prominence of the glial response in axonal tracts suggests a primary axonopathy. Importantly, therefore, our data support both neurodevelopmental and degenerative mechanisms in the pathobiology of CS.

Published
2018
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