Your search keyword '"Bacon, Chelsea"' showing total 30 results

1. Differences in the neural correlates of schizophrenia with positive and negative formal thought disorder in patients with schizophrenia in the ENIGMA dataset.

Author

Sharkey, Rachel, Bacon, Chelsea, Peterson, Zeru, Rootes-Murdy, Kelly, Salvador, Raymond, Pomarol-Clotet, Edith, Karuk, Andriana, Homan, Philipp, Ji, Ellen, Omlor, Wolfgang, Homan, Stephanie, Georgiadis, Foivos, Kaiser, Stefan, Kirschner, Matthias, Ehrlich, Stefan, Dannlowski, Udo, Grotegerd, Dominik, Goltermann, Janik, Meinert, Susanne, Kircher, Tilo, Stein, Frederike, Brosch, Katharina, Krug, Axel, Nenadic, Igor, Sim, Kang, Spalletta, Gianfranco, Banaj, Nerisa, Sponheim, Scott, Demro, Caroline, Ramsay, Ian, King, Margaret, Quidé, Yann, Green, Melissa, Nguyen, Dana, Preda, Adrian, Calhoun, Vince, Turner, Jessica, van Erp, Theo, and Nickl-Jockschat, Thomas

Subjects

Humans, Schizophrenia, Male, Female, Adult, Brain, Middle Aged, Schizophrenic Psychology, Neuroimaging, Cohort Studies, Magnetic Resonance Imaging, Thinking

Abstract

Formal thought disorder (FTD) is a clinical key factor in schizophrenia, but the neurobiological underpinnings remain unclear. In particular, the relationship between FTD symptom dimensions and patterns of regional brain volume loss in schizophrenia remains to be established in large cohorts. Even less is known about the cellular basis of FTD. Our study addresses these major obstacles by enrolling a large multi-site cohort acquired by the ENIGMA Schizophrenia Working Group (752 schizophrenia patients and 1256 controls), to unravel the neuroanatomy of FTD in schizophrenia and using virtual histology tools on implicated brain regions to investigate the cellular basis. Based on the findings of previous clinical and neuroimaging studies, we decided to separately explore positive, negative and total formal thought disorder. We used virtual histology tools to relate brain structural changes associated with FTD to cellular distributions in cortical regions. We identified distinct neural networks positive and negative FTD. Both networks encompassed fronto-occipito-amygdalar brain regions, but positive and negative FTD demonstrated a dissociation: negative FTD showed a relative sparing of orbitofrontal cortical thickness, while positive FTD also affected lateral temporal cortices. Virtual histology identified distinct transcriptomic fingerprints associated for both symptom dimensions. Negative FTD was linked to neuronal and astrocyte fingerprints, while positive FTD also showed associations with microglial cell types. These results provide an important step towards linking FTD to brain structural changes and their cellular underpinnings, providing an avenue for a better mechanistic understanding of this syndrome.

Published

2024

2. Assessing non-Mendelian inheritance in inherited axonopathies

Author

Bis-Brewer, Dana M., Gan-Or, Ziv, Sleiman, Patrick, Rodriguez, Aixa, Bacha, Alexa, Kosikowski, Ashley, Wood, Beth, McCray, Brett, Blume, Brianna, Siskind, Carly, Sumner, Charlotte, Calabrese, Daniela, Walk, David, Vujovic, Dragan, Park, Eun, Muntoni, Francesco, Donlevy, Gabrielle, Acsadi, Gyula, Day, John, Burns, Joshua, Li, Jun, Krajewski, Karen, Eichinger, Kate, Cornett, Kayla, Mullen, Krista, Perez, Laura, Gutmann, Laurie, Barrett, Maria, Saporta, Mario, Skorupinska, Mariola, Grant, Natalie, Bray, Paula, Seyedsadjadi, Reza, Zuccarino, Riccardo, Finkel, Richard, Lewis, Richard, Yum, Sabrina, Hilbert, Sarah, Thomas, Simone, Behrens-Spraggins, Steffen, Jones, Tara, Grider, Tiffany, Estilow, Tim, Fridman, Vera, Reilly, Mary M., Shy, Michael E., Bacon, Chelsea J., Feely, Shawna M.E., Rossor, Alexander M., Herrmann, David N., Hakonarson, Hakon, Fazal, Sarah, Courel, Steve, Cintra, Vivian, Tao, Feifei, Estiar, Mehrdad A., Tarnopolsky, Mark, Boycott, Kym M., Yoon, Grace, Suchowersky, Oksana, Dupré, Nicolas, Cheng, Andrew, Lloyd, Thomas E., Rouleau, Guy, Schüle, Rebecca, and Züchner, Stephan

Published

2020

3. Neural Correlates of Positive and Negative Formal Thought Disorder in Individuals with Schizophrenia: An ENIGMA Schizophrenia Working Group Study

Author

Nickl-Jockschat, Thomas, primary, Sharkey, Rachel, additional, Bacon, Chelsea, additional, Peterson, Zeru, additional, Rootes-Murdy, Kelly, additional, Salvador, Raymond, additional, Pomarol, Edith, additional, Karuk, Andriana, additional, Homan, Philipp, additional, Ji, Ellen, additional, Omlor, Wolfgang, additional, Homan, Stephanie, additional, Georgiadis, Foivos, additional, Kaiser, Stefan, additional, Kirschner, Matthias, additional, Ehrlich, Stefan, additional, Dannlowski, Udo, additional, Grotegerd, Dominik, additional, Goltermann, Janik, additional, Meinert, Susanne, additional, Kircher, Tilo, additional, Stein, Frederike, additional, Brosch, Katharina, additional, Krug, Axel, additional, Nenadic, Igor, additional, Sim, Kang, additional, Piras, Fabrizio, additional, Banaj, Nerisa, additional, Sponheim, Scott, additional, Demro, Caroline, additional, Ramsay, Ian, additional, King, Margaret, additional, Quidé, Yann, additional, Green, Melissa, additional, Nguyen, Dana, additional, Preda, Adrian, additional, Calhoun, Vince, additional, Turner, Jessica, additional, Erp, Theo van, additional, and Spalletta, Gianfranco, additional

Published

2023

4. A longitudinal study of CMT1A using Rasch analysis based CMT neuropathy and examination scores

Author

Fridman, Vera, Sillau, Stefan, Acsadi, Gyula, Bacon, Chelsea, Dooley, Kimberly, Burns, Joshua, Day, John, Feely, Shawna, Finkel, Richard S., Grider, Tiffany, Gutmann, Laurie, Herrmann, David N., Kirk, Callyn A., Knause, Sarrah A., Laurá, Matilde, Lewis, Richard A., Li, Jun, Lloyd, Thomas E., Moroni, Isabella, Muntoni, Francesco, Pagliano, Emanuela, Pisciotta, Chiara, Piscosquito, Giuseppe, Ramchandren, Sindhu, Saporta, Mario, Sadjadi, Reza, Shy, Rosemary R., Siskind, Carly E., Sumner, Charlotte J., Walk, David, Wilcox, Janel, Yum, Sabrina W., Züchner, Stephan, Scherer, Steven S., Pareyson, Davide, Reilly, Mary M., and Shy, Michael E.

Published

2020

5. Neural Correlates of Positive and Negative Formal Thought Disorder in Individuals with Schizophrenia: An ENIGMA Schizophrenia Working Group Study

Author

Sharkey, Rachel J., primary, Bacon, Chelsea, additional, Peterson, Zeru, additional, Rootes-Murdy, Kelly, additional, Salvador, Raymond, additional, Pomarol-Clotet, Edith, additional, Karuk, Andriana, additional, Homan, Philipp, additional, Ji, Ellen, additional, Omlor, Wolfgang, additional, Homan, Stephanie, additional, Georgiadis, Foivos, additional, Kaiser, Stefan, additional, Kirschner, Matthias, additional, Ehrlich, Stefan, additional, Dannlowski, Udo, additional, Grotegerd, Dominik, additional, Goltermann, Janik, additional, Meinert, Susanne, additional, Kircher, Tilo, additional, Stein, Frederike, additional, Brosch, Katharina, additional, Krug, Axel, additional, Nenadić, Igor, additional, Sim, Kang, additional, Spalletta, Gianfranco, additional, Piras, Fabrizio, additional, Banaj, Nerisa, additional, Sponheim, Scott R, additional, Demro, Caroline, additional, Ramsay, Ian S, additional, King, Margaret, additional, Quidé, Yann, additional, Green, Melissa J., additional, Nguyen, Dana, additional, Preda, Adrian, additional, Calhoun, Vince D., additional, Turner, Jessica A., additional, van Erp, Theo G.M., additional, and Nickl-Jockschat, Thomas, additional

Published

2023

6. Neural Correlates of Positive and Negative Formal Thought Disorder in Individuals with Schizophrenia: An ENIGMA Schizophrenia Working Group Study

Author

Sharkey, Rachel J., Bacon, Chelsea, Peterson, Zeru, Rootes-Murdy, Kelly, Salvador, Raymond, Pomarol-Clotet, Edith, Karuk, Andriana, Homan, Philipp, Ji, Ellen, Omlor, Wolfgang, Homan, Stephanie, Georgiadis, Foivos, Kaiser, Stefan, Kirschner, Matthias, Ehrlich, Stefan, Dannlowski, Udo, Grotegerd, Dominik, Goltermann, Janik, Meinert, Susanne, Kircher, Tilo, Stein, Frederike, Brosch, Katharina, Krug, Axel, Nenadić, Igor, Sim, Kang, Spalletta, Gianfranco, Piras, Fabrizio, Banaj, Nerisa, Sponheim, Scott R, Demro, Caroline, Ramsay, Ian S, King, Margaret, Quidé, Yann, Green, Melissa J., Nguyen, Dana, Preda, Adrian, Calhoun, Vince D., Turner, Jessica A., van Erp, Theo G.M., and Nickl-Jockschat, Thomas

Subjects

Article

Abstract

Formal thought disorder (FTD) is a key clinical factor in schizophrenia, but the neurobiological underpinnings remain unclear. In particular, relationship between FTD symptom dimensions and patterns of regional brain volume deficiencies in schizophrenia remain to be established in large cohorts. Even less is known about the cellular basis of FTD. Our study addresses these major obstacles based on a large multi-site cohort through the ENIGMA Schizophrenia Working Group (752 individuals with schizophrenia and 1256 controls), to unravel the neuroanatomy of positive, negative and total FTD in schizophrenia and their cellular bases. We used virtual histology tools to relate brain structural changes associated with FTD to cellular distributions in cortical regions. We identified distinct neural networks for positive and negative FTD. Both networks encompassed fronto-occipito-amygdalar brain regions, but negative FTD showed a relative sparing of orbitofrontal cortical thickness, while positive FTD also affected lateral temporal cortices. Virtual histology identified distinct transcriptomic fingerprints associated for both symptom dimensions. Negative FTD was linked to neuronal and astrocyte fingerprints, while positive FTD was also linked to microglial cell types. These findings relate different dimensions of FTD to distinct brain structural changes and their cellular underpinnings, improve our mechanistic understanding of these key psychotic symptoms.

Published

2023

7. The Charcot-Marie-Tooth Functional Outcome Measure (CMT-FOM)

Author

Eichinger, Katy, Burns, Joshua, Cornett, Kayla, Bacon, Chelsea, Shepherd, Mary Lohse, Mountain, Joan, Sowden, Janet, Shy, Rosemary, Shy, Michael E., and Herrmann, David N.

Published

2018

8. Disease Progression in Charcot–Marie–Tooth Disease Related to MPZ Mutations: A Longitudinal Study.

Author

Fridman, Vera, Sillau, Stefan, Bockhorst, Jacob, Smith, Kaitlin, Moroni, Isabella, Pagliano, Emanuela, Pisciotta, Chiara, Piscosquito, Guiseppe, Laurá, Matilde, Muntoni, Francesco, Bacon, Chelsea, Feely, Shawna, Grider, Tiffany, Gutmann, Laurie, Shy, Rosemary, Wilcox, Janel, Herrmann, David N., Li, Jun, Ramchandren, Sindhu, and Sumner, Charlotte J.

Subjects

CHARCOT-Marie-Tooth disease, DISEASE progression, LONGITUDINAL method, GENETIC mutation, NATURAL history

Abstract

Objective: The paucity of longitudinal natural history studies in MPZ neuropathy remains a barrier to clinical trials. We have completed a longitudinal natural history study in patients with MPZ neuropathies across 13 sites of the Inherited Neuropathies Consortium. Methods: Change in Charcot–Marie–Tooth Examination Score (CMTES) and Rasch modified CMTES (CMTES‐R) were evaluated using longitudinal regression over a 5‐year period in subjects with MPZ neuropathy. Data from 139 patients with MPZ neuropathy were examined. Results: The average baseline CMTES and CMTES‐R were 10.84 (standard deviation [SD] = 6.0, range = 0–28) and 14.60 (SD = 7.56, range = 0–32), respectively. A mixed regression model showed significant change in CMTES at years 2–5 (mean change from baseline of 0.87 points at 2 years, p = 0.008). Subgroup analysis revealed greater change in CMTES at 2 years in subjects with axonal as compared to demyelinating neuropathy (mean change of 1.30 points [p = 0.016] vs 0.06 points [p = 0.889]). Patients with a moderate baseline neuropathy severity also showed more notable change, by estimate, than those with mild or severe neuropathy (mean 2‐year change of 1.14 for baseline CMTES 8–14 [p = 0.025] vs −0.03 for baseline CMTES 0–7 [p = 0.958] and 0.25 for baseline CMTES ≥ 15 [p = 0.6897]). The progression in patients harboring specific MPZ mutations was highly variable. Interpretation: CMTES is sensitive to change over time in adult patients with axonal but not demyelinating forms of MPZ neuropathy. Change in CMTES was greatest in patients with moderate baseline disease severity. These findings will inform future clinical trials of MPZ neuropathies. ANN NEUROL 2023;93:563–576 [ABSTRACT FROM AUTHOR]

Published

2023

9. Genotype–phenotype characteristics and baseline natural history of heritable neuropathies caused by mutations in the MPZ gene

Author

Sanmaneechai, Oranee, Feely, Shawna, Scherer, Steven S., Herrmann, David N., Burns, Joshua, Muntoni, Francesco, Li, Jun, Siskind, Carly E., Day, John W., Laura, Matilde, Sumner, Charlotte J., Lloyd, Thomas E., Ramchandren, Sindhu, Shy, Rosemary R., Grider, Tiffany, Bacon, Chelsea, Finkel, Richard S., Yum, Sabrina W., Moroni, Isabella, Piscosquito, Giuseppe, Pareyson, Davide, Reilly, Mary M., and Shy, Michael E.

Published

2015

10. A novel mutation in VCP causes Charcot–Marie–Tooth Type 2 disease

Author

Gonzalez, Michael A., Feely, Shawna M., Speziani, Fiorella, Strickland, Alleene V., Danzi, Matt, Bacon, Chelsea, Lee, Youjin, Chou, Tsui-Fen, Blanton, Susan H., Weihl, Conrad C., Zuchner, Stephan, and Shy, Michael E.

Published

2014

11. Psychometrics evaluation of Charcot-Marie-Tooth Neuropathy Score (CMTNSv2) second version, using Rasch analysis

Author

Sadjadi, Reza, Reilly, Mary M., Shy, Michael E., Pareyson, Davide, Laura, Matilde, Murphy, Sinead, Feely, Shawna M. E., Grider, Tiffany, Bacon, Chelsea, Piscosquito, Giuseppe, Calabrese, Daniela, and Burns, Ted M.

Published

2014

12. Erratum to: A CADM3 variant causes Charcot-Marie-Tooth disease with marked upper limb involvement

Author

Rebelo, Adriana P, primary, Cortese, Andrea, additional, Abraham, Amit, additional, Eshed-Eisenbach, Yael, additional, Shner, Gal, additional, Vainshtein, Anna, additional, Buglo, Elena, additional, Camarena, Vladimir, additional, Gaidosh, Gabriel, additional, Shiekhattar, Ramin, additional, Abreu, Lisa, additional, Courel, Steve, additional, Burns, Dennis K, additional, Bai, Yunhong, additional, Bacon, Chelsea, additional, Feely, Shawna M E, additional, Castro, Diana, additional, Peles, Elior, additional, Reilly, Mary M, additional, Shy, Michael E, additional, and Zuchner, Stephan, additional

Published

2021

13. A CADM3 variant causes Charcot-Marie-Tooth disease with marked upper limb involvement

Author

Rebelo, Adriana P, primary, Cortese, Andrea, additional, Abraham, Amit, additional, Eshed-Eisenbach, Yael, additional, Shner, Gal, additional, Vainshtein, Anna, additional, Buglo, Elena, additional, Camarena, Vladimir, additional, Gaidosh, Gabriel, additional, Shiekhattar, Ramin, additional, Abreu, Lisa, additional, Courel, Steve, additional, Burns, Dennis K, additional, Bai, Yunhong, additional, Bacon, Chelsea, additional, Feely, Shawna M E, additional, Castro, Diana, additional, Peles, Elior, additional, Reilly, Mary M, additional, Shy, Michael E, additional, and Zuchner, Stephan, additional

Published

2021

14. Mutations in ATP1A1 Cause Dominant Charcot-Marie-Tooth Type 2

Author

Lassuthova, Petra, Rebelo, Adriana P., Ravenscroft, Gianina, Lamont, Phillipa J., Davis, Mark R., Manganelli, Fiore, Feely, Shawna M., Bacon, Chelsea, Brožková, Dana Šafka, Haberlova, Jana, Mazanec, Radim, Tao, Feifei, Saghira, Cima, Abreu, Lisa, Courel, Steve, Powell, Eric, Buglo, Elena, Bis, Dana M., Baxter, Megan F., Ong, Royston W., Marns, Lorna, Lee, Yi-Chung, Bai, Yunhong, Isom, Daniel G., Barro-Soria, René, Chung, Ki W., Scherer, Steven S., Larsson, H. Peter, Laing, Nigel G., Choi, Byung-Ok, Seeman, Pavel, Shy, Michael E., Santoro, Lucio, and Zuchner, Stephan

Published

2018

15. Transmembrane protease serine 5: a novel Schwann cell plasma marker for CMT1A

Author

Wang, Hongge, primary, Davison, Matthew, additional, Wang, Kathryn, additional, Xia, Tai‐He, additional, Kramer, Martin, additional, Call, Katherine, additional, Luo, Jun, additional, Wu, Xingyao, additional, Zuccarino, Riccardo, additional, Bacon, Chelsea, additional, Bai, Yunhong, additional, Moran, John J., additional, Gutmann, Laurie, additional, Feely, Shawna M. E., additional, Grider, Tiffany, additional, Rossor, Alexander M., additional, Reilly, Mary M., additional, Svaren, John, additional, and Shy, Michael E., additional

Published

2019

16. A recurrent GARS mutation causes distal hereditary motor neuropathy

Author

Lee, Diana C., primary, Meyer‐Schuman, Rebecca, additional, Bacon, Chelsea, additional, Shy, Michael E., additional, Antonellis, Anthony, additional, and Scherer, Steven S., additional

Published

2019

17. A multicenter retrospective study of charcot‐marie‐tooth disease type 4B (CMT4B) associated with mutations in myotubularin‐related proteins (MTMRs)

Author

Pareyson, Davide, primary, Stojkovic, Tanya, additional, Reilly, Mary M., additional, Leonard‐Louis, Sarah, additional, Laurà, Matilde, additional, Blake, Julian, additional, Parman, Yesim, additional, Battaloglu, Esra, additional, Tazir, Meriem, additional, Bellatache, Mounia, additional, Bonello‐Palot, Nathalie, additional, Lévy, Nicolas, additional, Sacconi, Sabrina, additional, Guimarães‐Costa, Raquel, additional, Attarian, Sharham, additional, Latour, Philippe, additional, Solé, Guilhem, additional, Megarbane, André, additional, Horvath, Rita, additional, Ricci, Giulia, additional, Choi, Byung‐Ok, additional, Schenone, Angelo, additional, Gemelli, Chiara, additional, Geroldi, Alessandro, additional, Sabatelli, Mario, additional, Luigetti, Marco, additional, Santoro, Lucio, additional, Manganelli, Fiore, additional, Quattrone, Aldo, additional, Valentino, Paola, additional, Murakami, Tatsufumi, additional, Scherer, Steven S., additional, Dankwa, Lois, additional, Shy, Michael E., additional, Bacon, Chelsea J., additional, Herrmann, David N., additional, Zambon, Alberto, additional, Tramacere, Irene, additional, Pisciotta, Chiara, additional, Magri, Stefania, additional, Previtali, Stefano C., additional, and Bolino, Alessandra, additional

Published

2019

18. Schwann cell transcript biomarkers for hereditary neuropathy skin biopsies

Author

Svaren, John, primary, Moran, John J., additional, Wu, Xingyao, additional, Zuccarino, Riccardo, additional, Bacon, Chelsea, additional, Bai, Yunhong, additional, Ramesh, Raghu, additional, Gutmann, Laurie, additional, Anderson, Daniel M., additional, Pavelec, Derek, additional, and Shy, Michael E., additional

Published

2019

19. Mutations in BAG3 cause adult-onset Charcot-Marie-Tooth disease

Author

Shy, Michael, primary, Rebelo, Adriana P, additional, Feely, Shawna ME, additional, Abreu, Lisa A, additional, Tao, Feifei, additional, Swenson, Andrea, additional, Bacon, Chelsea, additional, and Zuchner, Stephan, additional

Published

2017

20. Biallelic mutations in SORDcause a common and potentially treatable hereditary neuropathy with implications for diabetes

Author

Cortese, Andrea, Zhu, Yi, Rebelo, Adriana P., Negri, Sara, Courel, Steve, Abreu, Lisa, Bacon, Chelsea J., Bai, Yunhong, Bis-Brewer, Dana M., Bugiardini, Enrico, Buglo, Elena, Danzi, Matt C., Feely, Shawna M. E., Athanasiou-Fragkouli, Alkyoni, Haridy, Nourelhoda A., Isasi, Rosario, Khan, Alaa, Laurà, Matilde, Magri, Stefania, Pipis, Menelaos, Pisciotta, Chiara, Powell, Eric, Rossor, Alexander M., Saveri, Paola, Sowden, Janet E., Tozza, Stefano, Vandrovcova, Jana, Dallman, Julia, Grignani, Elena, Marchioni, Enrico, Scherer, Steven S., Tang, Beisha, Lin, Zhiqiang, Al-Ajmi, Abdullah, Schüle, Rebecca, Synofzik, Matthis, Maisonobe, Thierry, Stojkovic, Tanya, Auer-Grumbach, Michaela, Abdelhamed, Mohamed A., Hamed, Sherifa A., Zhang, Ruxu, Manganelli, Fiore, Santoro, Lucio, Taroni, Franco, Pareyson, Davide, Houlden, Henry, Herrmann, David N., Reilly, Mary M., Shy, Michael E., Zhai, R. Grace, and Zuchner, Stephan

Abstract

Here we report biallelic mutations in the sorbitol dehydrogenase gene (SORD) as the most frequent recessive form of hereditary neuropathy. We identified 45 individuals from 38 families across multiple ancestries carrying the nonsense c.757delG (p.Ala253GlnfsTer27) variant in SORD, in either a homozygous or compound heterozygous state. SORD is an enzyme that converts sorbitol into fructose in the two-step polyol pathway previously implicated in diabetic neuropathy. In patient-derived fibroblasts, we found a complete loss of SORD protein and increased intracellular sorbitol. Furthermore, the serum fasting sorbitol levels in patients were dramatically increased. In Drosophila, loss of SORDorthologs caused synaptic degeneration and progressive motor impairment. Reducing the polyol influx by treatment with aldose reductase inhibitors normalized intracellular sorbitol levels in patient-derived fibroblasts and in Drosophila, and also dramatically ameliorated motor and eye phenotypes. Together, these findings establish a novel and potentially treatable cause of neuropathy and may contribute to a better understanding of the pathophysiology of diabetes.

Published

2020

21. Transmembrane protease serine 5: a novel Schwann cell plasma marker for CMT1A.

Author

Wang, Hongge, Davison, Matthew, Wang, Kathryn, Xia, Tai‐He, Kramer, Martin, Call, Katherine, Luo, Jun, Wu, Xingyao, Zuccarino, Riccardo, Bacon, Chelsea, Bai, Yunhong, Moran, John J., Gutmann, Laurie, Feely, Shawna M. E., Grider, Tiffany, Rossor, Alexander M., Reilly, Mary M., Svaren, John, and Shy, Michael E.

Subjects

SCHWANN cells, PLASMA cells, NEURONS, PERIPHERAL nervous system, NEURAL conduction, LEUKODYSTROPHY

Abstract

Objective: Development of biomarkers for Charcot‐Marie‐Tooth (CMT) disease is critical for implementing effective clinical trials. The most common form of CMT, type 1A, is caused by a genomic duplication surrounding the PMP22 gene. A recent report (Neurology 2018;90:e518–3524) showed elevation of neurofilament light (NfL) in plasma of CMT1A disease patients, which correlated with disease severity. However, no plasma/serum biomarker has been identified that is specific to Schwann cells, the most directly affected cells in CMT1A. Methods: We used the Olink immuno PCR platform to profile CMT1A patient (n = 47, 2 cohorts) and normal control plasma (n = 41, two cohorts) on five different Olink panels to screen 398 unique proteins. Results: The TMPRSS5 protein (Transmembrane protease serine 5) was elevated 2.07‐fold (P = <0.0001) in two independent cohorts of CMT1A samples relative to controls. TMPRSS5 is most highly expressed in Schwann cells of peripheral nerve. Consistent with early myelination deficits in CMT1A, TMPRSS5 was not significantly correlated with disease score (CMTES‐R, CMTNS‐R), nerve conduction velocities (Ulnar CMAP, Ulnar MNCV), or with age. TMPRSS5 was not significantly elevated in smaller sample sets from patients with CMT2A, CMT2E, CMT1B, or CMT1X. The Olink immuno PCR assays confirmed elevated levels of NfL (average 1.58‐fold, P < 0.0001), which correlated with CMT1A patient disease score. Interpretation: These data identify the first Schwann cell‐specific protein that is elevated in plasma of CMT1A patients, and may provide a disease marker and a potentially treatment‐responsive biomarker with good disease specificity for clinical trials. [ABSTRACT FROM AUTHOR]

Published

2020

22. Schwann cell transcript biomarkers for hereditary neuropathy skin biopsies.

Author

Moran, John J., Ramesh, Raghu, Svaren, John, Wu, Xingyao, Bacon, Chelsea, Bai, Yunhong, Gutmann, Laurie, Anderson, Daniel M., Shy, Michael E., Zuccarino, Riccardo, and Pavelec, Derek

Subjects

SCHWANN cells, SKIN biopsy, MYELIN proteins, BIOMARKERS, LEBER'S hereditary optic atrophy, CLINICAL trials, RESEARCH, NERVE tissue proteins, BIOPSY, SKIN, ANIMAL experimentation, RESEARCH methodology, PERIPHERAL nervous system, EVALUATION research, MEDICAL cooperation, COMPARATIVE studies, CHARCOT-Marie-Tooth disease, RESEARCH funding, MICE

Abstract

Objective: Charcot-Marie-Tooth (CMT) disease is most commonly caused by duplication of a chromosomal segment surrounding Peripheral Myelin Protein 22, or PMP22 gene, which is classified as CMT1A. Several candidate therapies reduce Pmp22 mRNA levels in CMT1A rodent models, but development of biomarkers for clinical trials in CMT1A is a challenge given its slow progression and difficulty in obtaining nerve samples. Quantitative PCR measurements of PMP22 mRNA in dermal nerves were performed using skin biopsies in human clinical trials for CMT1A, but this approach did not show increased PMP22 mRNA in CMT1A patients compared to controls. One complicating factor is the variable amounts of Schwann cells (SCs) in skin. The objective of the study was to develop a novel method for precise evaluation of PMP22 levels in skin biopsies that can discriminate CMT1A patients from controls.Methods: We have developed methods to normalize PMP22 transcript levels to SC-specific genes that are not altered by CMT1A status. Several CMT1A-associated genes were assembled into a custom Nanostring panel to enable precise transcript measurements that can be normalized to variable SC content.Results: The digital expression data from Nanostring analysis showed reproducible elevation of PMP22 levels in CMT1A versus control skin biopsies, particularly after normalization to SC-specific genes.Interpretation: This platform should be useful in clinical trials for CMT1A as a biomarker of target engagement that can be used to optimize dosing, and the same normalization framework is applicable to other types of CMT. ANN NEUROL 2019;85:887-898. [ABSTRACT FROM AUTHOR]

Published

2019

23. Mutations in BAG3 cause adult-onset Charcot-Marie-Tooth disease.

Author

Shy, Michael, Rebelo, Adriana P., Feely, Shawna M. E., Abreu, Lisa A., Tao, Feifei, Swenson, Andrea, Bacon, Chelsea, Zuchner, Stephan, and Feely, Shawna Me

Subjects

GENETIC mutation, CHARCOT-Marie-Tooth disease, PERIPHERAL neuropathy, EXOMES, NUCLEOTIDE sequence

Published

2018

24. Biallelic mutations in sord are a common cause of potentially treatable genetic neuropathy

Author

Cortese, Andrea, Zhu, Yi, Rebelo, Adriana, Negri, Sara, Courel, Steve, Abreu, Lisa, Bacon, Chelsea J, Bai, Yunhong, and Bis-Brewer, Dana M

Abstract

IntroductionAs opposed to CMT1, for which over 90% of cases have mutations in known genes, only 20–30% of CMT2/dHMN patients receive a genetic diagnosis. Since up to 70% of CMT2 and dHMN cases are sporadic, identifying candidate pathogenic genes from single cases remains challenging also for next-generation sequencing techniques.MethodsWe took advantage of the largest collection of over 1,100 CMT patients in whom WES and/or WGS has been performed in the GENESIS analysis platform. We specifically looked for genes for which significant DNA variants are present in multiple families as well as for individual alleles overrepresented in CMT cases.ResultsWe identified 45 cases from 38 families across multiple ethnicities, carrying a particular nonsense mutation in SORD, c.753delG;p.Ala253GlnfsTer27, either in homozygous or compound heterozygous state with a second variant. With an allele frequency of 0.004 in healthy controls, the p.Ala253GlnfsTer27 variant represents one of the most common pathogenic alleles in humans. SORD is an enzyme that converts sorbitol into fructose, in the two-step polyol pathway that has been implicated in diabetic neuropathy. In patient-derived fibroblasts, we find a complete loss of SORD protein and increased intracellular sorbitol. Also, as a biomarker, serum fasting sorbitol level was over 100 times higher in patients compared to healthy individuals. In Drosophila, we show that loss of SORD orthologues causes synaptic degeneration and progressive motor impairment. Reducing the polyol influx by treatment with aldose reductase inhibi- tors normalized intracellular sorbitol levels in patient fibroblasts and in Drosophila, and also dramatically ameliorated motor and eye phenotypes.ConclusionsWe demonstrate biallelic mutations in sorbitol dehydrogenase (SORD) as the most frequent recessive form of hereditary neuropathies. These findings establish a potentially treatable cause in a sig- nificant fraction of patients with inherited neuropathies and may contribute to a better understanding of the pathophysiology of diabetic neuropathy.andrea.cortese@ucl.ac.uk

Published

2022

25. Author Correction: Biallelic mutations in SORDcause a common and potentially treatable hereditary neuropathy with implications for diabetes

Author

Cortese, Andrea, Zhu, Yi, Rebelo, Adriana P., Negri, Sara, Courel, Steve, Abreu, Lisa, Bacon, Chelsea J., Bai, Yunhong, Bis-Brewer, Dana M., Bugiardini, Enrico, Buglo, Elena, Danzi, Matt C., Feely, Shawna M. E., Athanasiou-Fragkouli, Alkyoni, Haridy, Nourelhoda A., Isasi, Rosario, Khan, Alaa, Laurà, Matilde, Magri, Stefania, Pipis, Menelaos, Pisciotta, Chiara, Powell, Eric, Rossor, Alexander M., Saveri, Paola, Sowden, Janet E., Tozza, Stefano, Vandrovcova, Jana, Dallman, Julia, Grignani, Elena, Marchioni, Enrico, Scherer, Steven S., Tang, Beisha, Lin, Zhiqiang, Al-Ajmi, Abdullah, Schüle, Rebecca, Synofzik, Matthis, Maisonobe, Thierry, Stojkovic, Tanya, Auer-Grumbach, Michaela, Abdelhamed, Mohamed A., Hamed, Sherifa A., Zhang, Ruxu, Manganelli, Fiore, Santoro, Lucio, Taroni, Franco, Pareyson, Davide, Houlden, Henry, Herrmann, David N., Reilly, Mary M., Shy, Michael E., Zhai, R. Grace, and Zuchner, Stephan

Abstract

An amendment to this paper has been published and can be accessed via a link at the top of the paper.

Published

2020

26. A multicenter retrospective study of charcot-marie-tooth disease type 4B (CMT4B) associated with mutations in myotubularin-related proteins (MTMRs)

Author

Pareyson, Davide, Stojkovic, Tanya, Reilly, Mary M, Leonard-Louis, Sarah, Laurà, Matilde, Blake, Julian, Parman, Yesim, Battaloglu, Esra, Tazir, Meriem, Bellatache, Mounia, Bonello-Palot, Nathalie, Lévy, Nicolas, Sacconi, Sabrina, Guimarães-Costa, Raquel, Attarian, Sharham, Latour, Philippe, Solé, Guilhem, Megarbane, André, Horvath, Rita, Ricci, Giulia, Choi, Byung-Ok, Schenone, Angelo, Gemelli, Chiara, Geroldi, Alessandro, Sabatelli, Mario, Luigetti, Marco, Santoro, Lucio, Manganelli, Fiore, Quattrone, Aldo, Valentino, Paola, Murakami, Tatsufumi, Scherer, Steven S, Dankwa, Lois, Shy, Michael E, Bacon, Chelsea J, Herrmann, David N, Zambon, Alberto, Tramacere, Irene, Pisciotta, Chiara, Magri, Stefania, Previtali, Stefano C, and Bolino, Alessandra

Subjects

Adult, Male, Adolescent, Middle Aged, Protein Tyrosine Phosphatases, Non-Receptor, 3. Good health, Young Adult, Charcot-Marie-Tooth Disease, Child, Preschool, Mutation, Humans, Female, Child, Retrospective Studies

Abstract

OBJECTIVE: Charcot-Marie-Tooth (CMT) disease 4B1 and 4B2 (CMT4B1/B2) are characterized by recessive inheritance, early onset, severe course, slowed nerve conduction, and myelin outfoldings. CMT4B3 shows a more heterogeneous phenotype. All are associated with myotubularin-related protein (MTMR) mutations. We conducted a multicenter, retrospective study to better characterize CMT4B. METHODS: We collected clinical and genetic data from CMT4B subjects in 18 centers using a predefined minimal data set including Medical Research Council (MRC) scores of nine muscle pairs and CMT Neuropathy Score. RESULTS: There were 50 patients, 21 of whom never reported before, carrying 44 mutations, of which 21 were novel and six representing novel disease associations of known rare variants. CMT4B1 patients had significantly more-severe disease than CMT4B2, with earlier onset, more-frequent motor milestones delay, wheelchair use, and respiratory involvement as well as worse MRC scores and motor CMT Examination Score components despite younger age at examination. Vocal cord involvement was common in both subtypes, whereas glaucoma occurred in CMT4B2 only. Nerve conduction velocities were similarly slowed in both subtypes. Regression analyses showed that disease severity is significantly associated with age in CMT4B1. Slopes are steeper for CMT4B1, indicating faster disease progression. Almost none of the mutations in the MTMR2 and MTMR13 genes, responsible for CMT4B1 and B2, respectively, influence the correlation between disease severity and age, in agreement with the hypothesis of a complete loss of function of MTMR2/13 proteins for such mutations. INTERPRETATION: This is the largest CMT4B series ever reported, demonstrating that CMT4B1 is significantly more severe than CMT4B2, and allowing an estimate of prognosis. ANN NEUROL 2019.

27. Neural Correlates of Positive and Negative Formal Thought Disorder in Individuals with Schizophrenia: An ENIGMA Schizophrenia Working Group Study.

Author

Nickl-Jockschat T, Sharkey R, Bacon C, Peterson Z, Rootes-Murdy K, Salvador R, Pomarol E, Karuk A, Homan P, Ji E, Omlor W, Homan S, Georgiadis F, Kaiser S, Kirschner M, Ehrlich S, Dannlowski U, Grotegerd D, Goltermann J, Meinert S, Kircher T, Stein F, Brosch K, Krug A, Nenadic I, Sim K, Piras F, Banaj N, Sponheim S, Demro C, Ramsay I, King M, Quidé Y, Green M, Nguyen D, Preda A, Calhoun V, Turner J, van Erp T, and Spalletta G

Abstract

Formal thought disorder (FTD) is a key clinical factor in schizophrenia, but the neurobiological underpinnings remain unclear. In particular, relationship between FTD symptom dimensions and patterns of regional brain volume deficiencies in schizophrenia remain to be established in large cohorts. Even less is known about the cellular basis of FTD. Our study addresses these major obstacles based on a large multi-site cohort through the ENIGMA Schizophrenia Working Group (752 individuals with schizophrenia and 1256 controls), to unravel the neuroanatomy of positive, negative and total FTD in schizophrenia and their cellular bases. We used virtual histology tools to relate brain structural changes associated with FTD to cellular distributions in cortical regions. We identified distinct neural networks for positive and negative FTD. Both networks encompassed fronto-occipito-amygdalar brain regions, but negative FTD showed a relative sparing of orbitofrontal cortical thickness, while positive FTD also affected lateral temporal cortices. Virtual histology identified distinct transcriptomic fingerprints associated for both symptom dimensions. Negative FTD was linked to neuronal and astrocyte fingerprints, while positive FTD was also linked to microglial cell types. These findings relate different dimensions of FTD to distinct brain structural changes and their cellular underpinnings, improve our mechanistic understanding of these key psychotic symptoms., Competing Interests: Confiicts of Interest The authors declare that there is no conflict of interest.

Published

2023

28. Neural Correlates of Positive and Negative Formal Thought Disorder in Individuals with Schizophrenia: An ENIGMA Schizophrenia Working Group Study.

Author

Sharkey RJ, Bacon C, Peterson Z, Rootes-Murdy K, Salvador R, Pomarol-Clotet E, Karuk A, Homan P, Ji E, Omlor W, Homan S, Georgiadis F, Kaiser S, Kirschner M, Ehrlich S, Dannlowski U, Grotegerd D, Goltermann J, Meinert S, Kircher T, Stein F, Brosch K, Krug A, Nenadić I, Sim K, Spalletta G, Piras F, Banaj N, Sponheim SR, Demro C, Ramsay IS, King M, Quidé Y, Green MJ, Nguyen D, Preda A, Calhoun VD, Turner JA, van Erp TGM, and Nickl-Jockschat T

Abstract

Formal thought disorder (FTD) is a key clinical factor in schizophrenia, but the neurobiological underpinnings remain unclear. In particular, relationship between FTD symptom dimensions and patterns of regional brain volume deficiencies in schizophrenia remain to be established in large cohorts. Even less is known about the cellular basis of FTD. Our study addresses these major obstacles based on a large multi-site cohort through the ENIGMA Schizophrenia Working Group (752 individuals with schizophrenia and 1256 controls), to unravel the neuroanatomy of positive, negative and total FTD in schizophrenia and their cellular bases. We used virtual histology tools to relate brain structural changes associated with FTD to cellular distributions in cortical regions. We identified distinct neural networks for positive and negative FTD. Both networks encompassed fronto-occipito-amygdalar brain regions, but negative FTD showed a relative sparing of orbitofrontal cortical thickness, while positive FTD also affected lateral temporal cortices. Virtual histology identified distinct transcriptomic fingerprints associated for both symptom dimensions. Negative FTD was linked to neuronal and astrocyte fingerprints, while positive FTD was also linked to microglial cell types. These findings relate different dimensions of FTD to distinct brain structural changes and their cellular underpinnings, improve our mechanistic understanding of these key psychotic symptoms.

Published

2023

29. Author Correction: Biallelic mutations in SORD cause a common and potentially treatable hereditary neuropathy with implications for diabetes.

Author

Cortese A, Zhu Y, Rebelo AP, Negri S, Courel S, Abreu L, Bacon CJ, Bai Y, Bis-Brewer DM, Bugiardini E, Buglo E, Danzi MC, Feely SME, Athanasiou-Fragkouli A, Haridy NA, Isasi R, Khan A, Laurà M, Magri S, Pipis M, Pisciotta C, Powell E, Rossor AM, Saveri P, Sowden JE, Tozza S, Vandrovcova J, Dallman J, Grignani E, Marchioni E, Scherer SS, Tang B, Lin Z, Al-Ajmi A, Schüle R, Synofzik M, Maisonobe T, Stojkovic T, Auer-Grumbach M, Abdelhamed MA, Hamed SA, Zhang R, Manganelli F, Santoro L, Taroni F, Pareyson D, Houlden H, Herrmann DN, Reilly MM, Shy ME, Zhai RG, and Zuchner S

Abstract

An amendment to this paper has been published and can be accessed via a link at the top of the paper.

Published

2020

30. Biallelic mutations in SORD cause a common and potentially treatable hereditary neuropathy with implications for diabetes.

Author

Cortese A, Zhu Y, Rebelo AP, Negri S, Courel S, Abreu L, Bacon CJ, Bai Y, Bis-Brewer DM, Bugiardini E, Buglo E, Danzi MC, Feely SME, Athanasiou-Fragkouli A, Haridy NA, Isasi R, Khan A, Laurà M, Magri S, Pipis M, Pisciotta C, Powell E, Rossor AM, Saveri P, Sowden JE, Tozza S, Vandrovcova J, Dallman J, Grignani E, Marchioni E, Scherer SS, Tang B, Lin Z, Al-Ajmi A, Schüle R, Synofzik M, Maisonobe T, Stojkovic T, Auer-Grumbach M, Abdelhamed MA, Hamed SA, Zhang R, Manganelli F, Santoro L, Taroni F, Pareyson D, Houlden H, Herrmann DN, Reilly MM, Shy ME, Zhai RG, and Zuchner S

Abstract

Here we report biallelic mutations in the sorbitol dehydrogenase gene (SORD) as the most frequent recessive form of hereditary neuropathy. We identified 45 individuals from 38 families across multiple ancestries carrying the nonsense c.757delG (p.Ala253GlnfsTer27) variant in SORD, in either a homozygous or compound heterozygous state. SORD is an enzyme that converts sorbitol into fructose in the two-step polyol pathway previously implicated in diabetic neuropathy. In patient-derived fibroblasts, we found a complete loss of SORD protein and increased intracellular sorbitol. Furthermore, the serum fasting sorbitol levels in patients were dramatically increased. In Drosophila, loss of SORD orthologs caused synaptic degeneration and progressive motor impairment. Reducing the polyol influx by treatment with aldose reductase inhibitors normalized intracellular sorbitol levels in patient-derived fibroblasts and in Drosophila, and also dramatically ameliorated motor and eye phenotypes. Together, these findings establish a novel and potentially treatable cause of neuropathy and may contribute to a better understanding of the pathophysiology of diabetes.

Published

2020