Your search keyword '"MNGIE"' showing total 209 results

1. Lysosomal dysfunction and overload of nucleosides in thymidine phosphorylase deficiency of MNGIE

Author

Jixiang Du, Fuchen Liu, Xihan Liu, Dandan Zhao, Dongdong Wang, Hongsheng Sun, Chuanzhu Yan, and Yuying Zhao

Subjects

TYMP, Thymidine phosphorylase, MNGIE, Lysosomal dysfunction, Nucleotide metabolism, Medicine

Abstract

Abstract Inherited deficiency of thymidine phosphorylase (TP), encoded by TYMP, leads to a rare disease with multiple mitochondrial DNA (mtDNA) abnormalities, mitochondrial neurogastrointestinal encephalomyopathy (MNGIE). However, the impact of TP deficiency on lysosomes remains unclear, which are important for mitochondrial quality control and nucleic acid metabolism. Muscle biopsy tissue and skin fibroblasts from MNGIE patients, patients with m.3243 A > G mitochondrial encephalopathy, lactic acidosis and stroke-like episodes (MELAS) and healthy controls (HC) were collected to perform mitochondrial and lysosomal functional analyses. In addition to mtDNA abnormalities, compared to controls distinctively reduced expression of LAMP1 and increased mitochondrial content were detected in the muscle tissue of MNGIE patients. Skin fibroblasts from MNGIE patients showed decreased expression of LAMP2, lowered lysosomal acidity, reduced enzyme activity and impaired protein degradation ability. TYMP knockout or TP inhibition in cells can also induce the similar lysosomal dysfunction. Using lysosome immunoprecipitation (Lyso- IP), increased mitochondrial proteins, decreased vesicular proteins and V-ATPase enzymes, and accumulation of various nucleosides were detected in lysosomes with TP deficiency. Treatment of cells with high concentrations of dThd and dUrd also triggers lysosomal dysfunction and disruption of mitochondrial homeostasis. Therefore, the results provided evidence that TP deficiency leads to nucleoside accumulation in lysosomes and lysosomal dysfunction, revealing the widespread disruption of organelles underlying MNGIE. Graphical Abstract

Published

2024

2. Lysosomal dysfunction and overload of nucleosides in thymidine phosphorylase deficiency of MNGIE.

Author

Du, Jixiang, Liu, Fuchen, Liu, Xihan, Zhao, Dandan, Wang, Dongdong, Sun, Hongsheng, Yan, Chuanzhu, and Zhao, Yuying

Subjects

*MELAS syndrome, *THYMIDINE, *NUCLEOSIDES, *MITOCHONDRIAL DNA, *NUCLEIC acids, *MITOCHONDRIAL proteins

Abstract

Inherited deficiency of thymidine phosphorylase (TP), encoded by TYMP, leads to a rare disease with multiple mitochondrial DNA (mtDNA) abnormalities, mitochondrial neurogastrointestinal encephalomyopathy (MNGIE). However, the impact of TP deficiency on lysosomes remains unclear, which are important for mitochondrial quality control and nucleic acid metabolism. Muscle biopsy tissue and skin fibroblasts from MNGIE patients, patients with m.3243 A > G mitochondrial encephalopathy, lactic acidosis and stroke-like episodes (MELAS) and healthy controls (HC) were collected to perform mitochondrial and lysosomal functional analyses. In addition to mtDNA abnormalities, compared to controls distinctively reduced expression of LAMP1 and increased mitochondrial content were detected in the muscle tissue of MNGIE patients. Skin fibroblasts from MNGIE patients showed decreased expression of LAMP2, lowered lysosomal acidity, reduced enzyme activity and impaired protein degradation ability. TYMP knockout or TP inhibition in cells can also induce the similar lysosomal dysfunction. Using lysosome immunoprecipitation (Lyso- IP), increased mitochondrial proteins, decreased vesicular proteins and V-ATPase enzymes, and accumulation of various nucleosides were detected in lysosomes with TP deficiency. Treatment of cells with high concentrations of dThd and dUrd also triggers lysosomal dysfunction and disruption of mitochondrial homeostasis. Therefore, the results provided evidence that TP deficiency leads to nucleoside accumulation in lysosomes and lysosomal dysfunction, revealing the widespread disruption of organelles underlying MNGIE. [ABSTRACT FROM AUTHOR]

Published

2024

3. Distinctive metabolic remodeling in TYMP deficiency beyond mitochondrial dysfunction.

Author

Du, Jixiang, Zhang, Chao, Liu, Fuchen, Liu, Xihan, Wang, Dongdong, Zhao, Dandan, Shui, Guanghou, Zhao, Yuying, and Yan, Chuanzhu

Subjects

*MELAS syndrome, *CHOLESTEROL metabolism, *MITOCHONDRIA, *MITOCHONDRIAL DNA, *DNA replication, *BILE acids

Abstract

Mitochondrial neurogastrointestinal encephalomyopathy (MNGIE) is caused by mutations in the TYMP gene, which encodes thymidine phosphorylase (TP). As a cytosolic metabolic enzyme, TP defects affect biological processes that are thought to not be limited to the abnormal replication of mitochondrial DNA. This study aimed to elucidate the characteristic metabolic alterations and associated homeostatic regulation caused by TYMP deficiency. The pathogenicity of novel TYMP variants was evaluated in terms of clinical features, genetic analysis, and structural instability. We analyzed plasma samples from three patients with MNGIE; three patients with m.3243A > G mitochondrial encephalopathy, lactic acidosis, and stroke-like episodes (MELAS); and four healthy controls (HC) using both targeted and untargeted metabolomics techniques. Transcriptomics analysis and bioenergetic studies were performed on skin fibroblasts from participants in these three groups. A TYMP overexpression experiment was conducted to rescue the observed changes. Compared with controls, specific alterations in nucleosides, bile acids, and steroid metabolites were identified in the plasma of MNGIE patients. Comparable mitochondrial dysfunction was present in fibroblasts from patients with TYMP deficiency and in those from patients with the m.3243A > G mutation. Distinctively decreased sterol regulatory element binding protein (SREBP) regulated cholesterol metabolism and fatty acid (FA) biosynthesis as well as reduced FA degradation were revealed in fibroblasts with TYMP deficiency. The restoration of thymidine phosphorylase activity rescued the observed changes in MNGIE fibroblasts. Our findings indicated that more widespread metabolic disturbance may be caused by TYMP deficiency in addition to mitochondrial dysfunction, which expands our knowledge of the biochemical outcome of TYMP deficiency. Key messages: Distinct metabolic profiles in patients with TYMP deficiency compared to those with m.3243A > G mutation. TYMP deficiency leads to a global disruption of nucleoside metabolism. Cholesterol and fatty acid metabolism are inhibited in individuals with MNGIE. TYMP is functionally related to SREBP-regulated pathways. Potential metabolite biomarkers that could be valuable clinical tools to improve the diagnosis of MNGIE. [ABSTRACT FROM AUTHOR]

Published

2023

4. Distinctive gastrointestinal motor dysfunction in patients with MNGIE.

Author

Alcalá‐González, Luis G., Accarino, Anna, Martí, Ramon, Sánchez‐Tejerina, Daniel, Llauradó, Arnau, Azpiroz, Fernando, and Malagelada, Carolina

Subjects

*ESOPHAGEAL motility disorders, *GASTROPARESIS, *ESOPHAGEAL motility, *SMALL intestine, *GASTRIC emptying, *ART techniques

Abstract

Background: Mitochondrial neurogastrointestinal encephalomyopathy (MNGIE) is a rare mitochondrial disease caused by mutations in TYMP, encoding thymidine phosphorylase. Clinically it is characterized by severe gastrointestinal dysmotility associated with cachexia and a demyelinating sensorimotor polyneuropathy. Even though digestive manifestations are progressive and invariably lead to death, the features of gastrointestinal motor dysfunction have not been systematically evaluated. The objective of this study was to describe gastrointestinal motor dysfunction in MNGIE using state‐of‐the art techniques and to evaluate the relationship between motor abnormalities and symptoms. Methods: Prospective study evaluating gastrointestinal motor function and digestive symptoms in all patients with MNGIE attended at a national referral center in Spain between January 2018 and July 2022. Key Results: In this period, five patients diagnosed of MNGIE (age range 16–46 years, four men) were evaluated. Esophageal motility by high‐resolution manometry was abnormal in four patients (two hypoperistalsis, two aperistalsis). Gastric emptying by scintigraphy was mildly delayed in four and indicative of gastroparesis in one. In all patients, small bowel high‐resolution manometry exhibited a common, distinctive dysmotility pattern, characterized by repetitive bursts of spasmodic contractions, without traces of normal fasting and postprandial motility patterns. Interestingly, objective motor dysfunctions were detected in the absence of severe digestive symptoms. Conclusions and Inferences: MNGIE patients exhibit a characteristic motor dysfunction, particularly of the small bowel, even in patients with mild digestive symptoms and in the absence of morphological signs of intestinal failure. Since symptoms are not predictive of objective findings, early investigation is indicated. [ABSTRACT FROM AUTHOR]

Published

2023

5. A new mutation in the TYMP-gene: clinical and morphological characteristics of a patient with MNGIE syndrome

Author

S. N. Bardakov, I. S. Limaev, A. M. Emelin, V. Nikitins, E. V. Presnyakov, S. A. Kurbatov, P. G. Tsygankova, V. A. Tsargush, I. A. Chekmareva, E. V. Kolmakova, N. V. Bakulina, and R. V. Deev

Subjects

mitochondrial neurogastrointestinal encephalomyopathy, mngie, tymp, telocytes, cd117, s100, Neurology. Diseases of the nervous system, RC346-429

Abstract

Mitochondrial neurogastrointestinal encephalomyopathy is an extremely rare (1–9:1 000 000, Orphanet, 2021) multisystem genetic disease caused by mutations in the TYMP gene encoding the enzyme thymidine phosphorylase.The article presents the data of a thirteen‑year survey on 40‑year‑old patient D. with clinical manifestations of mitochondrial neurogastrointestinal encephalomyopathy syndrome associated with the previously undescribed missense mutation c.1301G>T (p.Gly434Val) of the TYMP gene. Detailed clinical picture (gastrointestinal dysfunction, cachexia, blepharoptosis, ophthalmoparesis, peripheral polyneuropathy and leukoaraiosis), electroneuromyography data (demyelination with secondary axonopathy), high blood serum level of dihydrothymine together with normal levels of thymidine and deoxyuridine made it possible to verify the diagnosis. Histopathological examination revealed atrophy of the longitudinal (outer) muscle layer of the small and large intestines and a significant decrease in the number of CD117+ cells (telocytes), signs of damage to the striated skeletal muscles of a mixed nature with a predominance of the myogenic pattern, as well the destruction of the myelin sheaths of peripheral nerves. Histochemical examination did not reveal “ragged red fibers” characteristic of mitochondrial pathology. Transmission electron microscopy demonstrated the presence of megalomitochondria in the myocardium.

Published

2022

6. Mitochondrial neurogastrointestinal encephalomyopathy in a Pakistani female: a case report

Author

Zaraq Rashid Khan, Alvina Karam, Mian Ayaz ul Haq, Aleena Aman, and Ahmad Sharjeel Karam

Subjects

MNGIE, Asymptomatic leukoencephalopathy, Mitochondrial disorders, Genetic studies, Gastroparesis, Medicine

Abstract

Abstract Background Mitochondrial neurogastrointestinal encephalopathy is a rare multisystem autosomal recessive disease caused by mutations in the TYMP gene, that encodes for thymidine phosphorylase. Mitochondrial neurogastrointestinal encephalopathy is a progressive degenerative disease characterized by a distinctive tetrad of gastrointestinal dysmotility, peripheral neuropathy, ophthalmoplegia with ptosis, and asymptomatic leukoencephalopathy. It provides a diagnostic dilemma to physicians in regions like Pakistan because of a lack of genetic study availability and associated financial constraints of the population. However, with careful examination and a few basic investigations, mitochondrial neurogastrointestinal encephalopathy can be diagnosed by ruling out most of the close differentials. Case presentation We report the case of a 23-year-old Asian female whose chief complaints were epigastric pain, bilious emesis, weight loss for 3 months, and bilateral lower limb weakness for 20 days. All clinical signs and symptoms along with relevant investigations including nerve conduction studies, electromyography, and magnetic resonance imaging of the brain were highly suggestive of mitochondrial neurogastrointestinal encephalopathy syndrome. Because of financial constraints, genetic studies could not be performed. The patient was managed with a multidisciplinary approach involving gastroenterology, physiotherapy, and nutrition departments. Currently, therapeutic options for the disease include allogeneic hematopoietic stem cell transplant and carrier erythrocyte entrapped thymidine phosphorylase; however, these could not be provided to the patient owing to certain limitations. Conclusions As misdiagnosis and delayed diagnosis are quite common in this disease, the prime objective of this case report is to increase the basic understanding of this disease, especially its signs and symptoms, and address the limitations regarding the diagnostic investigations and management of patients with mitochondrial neurogastrointestinal encephalopathy.

Published

2022

7. Diagnosing mitochondrial, neurogastrointestinal leukoencephalopathy requires mutations in TYMP1, POLG1, LIG1, or RRM2B

Author

Josef Finsterer

Subjects

MNGIE, Mitochondrial disorder, Vomiting, White matter lesions, TYMP1, Lactic acidosis, Medicine

Published

2023

8. Diagnosing mitochondrial, neurogastrointestinal leukoencephalopathy requires mutations in TYMP1, POLG1, LIG1, or RRM2B

Author

Finsterer, Josef

Published

2023

9. Anatomical Laser Microdissection of the Ileum Reveals mtDNA Depletion Recovery in A Mitochondrial Neuro-Gastrointestinal Encephalomyopathy (MNGIE) Patient Receiving Liver Transplant.

Author

Boschetti, Elisa, Caporali, Leonardo, D'Angelo, Roberto, Malagelada, Carolina, Accarino, Anna, Dotti, Maria Teresa, Costa, Roberta, Cenacchi, Giovanna, Pironi, Loris, Rinaldi, Rita, Stanghellini, Vincenzo, Ratti, Stefano, Manzoli, Lucia, Carelli, Valerio, and De Giorgio, Roberto

Subjects

*MITOCHONDRIAL DNA, *LIVER transplantation, *HEMATOPOIETIC stem cell transplantation, *MITOCHONDRIA, *MICRODISSECTION, *ILEUM

Abstract

mitochondrial neuro-gastrointestinal encephalomyopathy (MNGIE) is a rare genetic disorder characterized by thymidine phosphorylase (TP) enzyme defect. The absence of TP activity induces the imbalance of mitochondrial nucleotide pool, leading to impaired mitochondrial DNA (mtDNA) replication and depletion. Since mtDNA is required to ensure oxidative phosphorylation, metabolically active tissues may not achieve sufficient energy production. The only effective life-saving approach in MNGIE has been the permanent replacement of TP via allogeneic hematopoietic stem cell or liver transplantation. However, the follow-up of transplanted patients showed that gut tissue changes do not revert and fatal complications, such as massive gastrointestinal bleeding, can occur. The purpose of this study was to clarify whether the reintroduction of TP after transplant can recover mtDNA copy number in a normal range. Using laser capture microdissection and droplet-digital-PCR, we assessed the mtDNA copy number in each layer of full-thickness ileal samples of a naive MNGIE cohort vs. controls and in a patient pre- and post-TP replacement. The treatment led to a significant recovery of gut tissue mtDNA amount, thus showing its efficacy. Our results indicate that a timely TP replacement is needed to maximize therapeutic success before irreversible degenerative tissue changes occur in MNGIE. [ABSTRACT FROM AUTHOR]

Published

2022

10. A Novel Mutation in an MNGIE Patient Presenting with More Prominent Neurological Symptoms than GI Symptoms.

Author

Xiaoyan Chen, Xiaoyi Xiong, Shu Liu, Chunmei Duan, Rui Xu, and Qingwu Yang

Subjects

*NERVE conduction studies, *GAIN-of-function mutations, *GENETIC testing

Abstract

Mitochondrial neurogastrointestinal encephalopathy (MNGIE) is an autosomal recessive disease associated with the mutation of the TYMP gene. MNGIE causes gastrointestinal and neurological symptoms, and the gastrointestinal symptoms are usually notable, which may lead to misdiagnosis. However, we herein report a 29‑year‑old female who presented with prominent neurological symptoms, while her gastrointestinal symptoms were mild. Brain MRI revealed prominent diffused leukoencephalopathy and peripheral neuropathy was confirmed by the nerve conduction velocity test. Biochemical tests showed elevated plasma thymidine, deoxyuridine, and lactate levels. Molecular genetic testing demonstrated a novel homozygous TYMP c. 447 dupG mutation and the patient’s mother was heterozygous for the mutation but had no clinical features. MNGIE was diagnosed based on the results. Unlike other patients who had notable gastrointestinal symptoms, this patient presented with more prominent neurological symptoms than gastrointestinal symptoms, which might have been caused by the novel mutation in the TYMP gene. [ABSTRACT FROM AUTHOR]

Published

2023

11. Mitochondrial Neurogastrointestinal Encephalomyopathy Disease (MNGIE)

Author

Li, Shufang, Martí, Ramon, Hirano, Michio, Mancuso, Michelangelo, editor, and Klopstock, Thomas, editor

Published

2019

12. Mitochondrial neurogastrointestinal encephalomyopathy: Clinical and biochemical impact of allogeneic stem cell transplantation in a Greek patient with one novel TYMP mutation

Author

A. Paisiou, M. Rogalidou, R. Pons, E. Ioannidou, K. Dimakou, A. Papadopoulou, F.M. Vaz, G. Vessalas, S.M.I. Goorden, J. Roelofsen, A. Zoetekouw, M.M. Nieman, E. Dimitriou, M. Moraitou, I. Peristeri, H. Michelakakis, and A.B.P. van Kuilenburg

Subjects

Mitochondrial neurogastrointestinal encephalomyopathy, MNGIE, Mutation analysis, Allogeneic hematopoietic stem cell transplantation, AHSCT, Medicine (General), R5-920, Biology (General), QH301-705.5

Abstract

We describe the case of a Greek female patient with the Classic form of the ultra- rare and fatal autosomal recessive disorder Mitochondrial neurogastrointestinal encephalomyopathy (MNGIE) and the impact of allogeneic hematopoietic stem cell transplantation on the biochemical and clinical aspects of the disease.The patient presented at the age of 15 years with severe gastrointestinal symptoms, cachexia, peripheral neuropathy and diffuse leukoencephalopathy. The diagnosis of MNGIE disease was established by the increased levels of thymidine and deoxyuridine in plasma and the complete deficiency of thymidine phosphorylase activity. The novel c.[978dup] (p.Ala327Argfs*?) variant and the previously described variant c.[417 + 1G > A] were identified in TYMP. The donor for the allogeneic hematopoietic stem cell transplantation was her fully compatible sister, a carrier of the disease. The patient had a completely uneventful post- transplant period and satisfactory PB chimerism levels. A marked and rapid decrease in thymidine and deoxyuridine plasma levels and an increase of the thymidine phosphorylase activity to the levels measured in her donor sister was observed and is still present sixteen months post-transplant. Disease symptoms stabilized and some improvement was also observed both in her neurological and gastrointestinal symptoms. Follow up studies will be essential for determining the long term impact of allogeneic hematopoietic stem cell transplantation in our patient.

Published

2022

13. Novel Mutations of the TYMP Gene in Mitochondrial Neurogastrointestinal Encephalomyopathy: Case Series and Literature Review.

Author

Mojtabavi, Helia, Fatehi, Farzad, Shahkarami, Sepideh, Rezaei, Nima, and Nafissi, Shahriar

Abstract

Mitochondrial neurogastrointestinal encephalomyopathy (MNGIE) is a multi-system disorder caused by several homozygous or compound heterozygous mutations, mostly in the nuclear gene of TYMP. Our current knowledge on the underlying pathology of the disease is derived through the study of about 200 cases of different ethnicities. Clinical presentations include severe cachexia, weakness, ptosis, diplopia, abdominal cramps or digestive tract disorders, hearing impairment, and paresthesia. Herein, we aim to present five novel mutations of the nuclear gene of TYMP in six Iranian patients diagnosed with MNGIE. In our population, age at the time of diagnosis was 18 to 49 years, while the onset of the symptoms varied from 13 to 20 years. We detected two pathogenic non-frameshift nonsense premature stop codon mutations (c.1013C > A, and c.130C > T), one variant of uncertain significance (VUS) non-frameshift missense mutation (c.345G > T), one likely pathogenic frameshift insertion (c.801_802insCGCG), and one likely benign homozygous non-frameshift deletion (c.1176_1187del) from two siblings. Our findings also confirm the autosomal recessive inheritance pattern of MNGIE in the Iranian population. The lack of knowledge in the area of nuclear gene-modifier genes shadows the genotype–phenotype relationships of MNGIE. [ABSTRACT FROM AUTHOR]

Published

2021

14. Preclinical Assessment of a Gene-Editing Approach in a Mouse Model of Mitochondrial Neurogastrointestinal Encephalomyopathy.

Author

Parés, Marta, Fornaguera, Cristina, Vila-Julià, Ferran, Oh, Sejin, Fan, Steven H.Y., Tam, Ying K., Comes, Natalia, Vidal, Francisco, Martí, Ramon, Borrós, Salvador, and Barquinero, Jordi

Subjects

*LABORATORY mice, *MITOCHONDRIA, *COMPLEMENTARY DNA, *TRANSGENE expression, *ANIMAL disease models, *URIDINE, *GENOME editing

Abstract

Mitochondrial neurogastrointestinal encephalomyopathy (MNGIE) is a rare disease caused by recessive mutations in the TYMP gene, which encodes the enzyme thymidine phosphorylase (TP). In this study, the efficient integration of a TYMP transgene into introns of the Tymp and Alb loci of hepatocytes in a murine model of MNGIE was achieved by the coordinated delivery and activity of CRISPR/Cas9 and a TYMP cDNA. CRISPR/Cas9 was delivered either as mRNA using lipid nanoparticle (LNP) or polymeric nanoparticle, respectively, or in an AAV2/8 viral vector; the latter was also used to package the TYMP cDNA. Insertion of the cDNA template downstream of the Tymp and Alb promoters ensured transgene expression. The best in vivo results were obtained using LNP carrying the CRISPR/Cas9 mRNAs. Treated mice showed a consistent long-term (1 year) reduction in plasma nucleoside (thymidine and deoxyuridine) levels that correlated with the presence of TYMP mRNA and functional enzyme in liver cells. In mice with an edited Alb locus, the transgene produced a hybrid Alb-hTP protein that was secreted, with supraphysiological levels of TP activity detected in the plasma. Equivalent results were obtained in mice edited at the Tymp locus. Finally, some degree of gene editing was found in animals treated only with AAV vectors containing the DNA templates, in the absence of nucleases, although there was no impact on plasma nucleoside levels. Overall, these results demonstrate the feasibility of liver-directed genome editing in the long-term correction of MNGIE, with several advantages over other methods. [ABSTRACT FROM AUTHOR]

Published

2021

15. Gastrointestinal Dysmotility in MNGIE: from thymidine phosphorylase enzyme deficiency to altered interstitial cells of Cajal

Author

Rana Yadak, Marjolein Breur, and Marianna Bugiani

Subjects

MNGIE, Mitochondrial neurogastrointestinal encephalomyopathy, Chronic intestinal pseudo-obstruction, CIPO, Interstitial cells of Cajal, ICC, Medicine

Abstract

Abstract Background MNGIE is a rare and fatal disease in which absence of the enzyme thymidine phosphorylase induces systemic accumulation of thymidine and deoxyuridine and secondary mitochondrial DNA alterations. Gastrointestinal (GI) symptoms are frequently reported in MNGIE patients, however, they are not resolved with the current treatment interventions. Recently, our understanding of the GI pathology has increased, which rationalizes the pursuit of more targeted therapeutic strategies. In particular, interstitial cells of Cajal (ICC) play key roles in GI physiology and are involved in the pathogenesis of the GI dysmotility. However, understanding of the triggers of ICC deficits in MNGIE is lacking. Herein, we review the current knowledge about the pathology of GI dysmotility in MNGIE, discuss potential mechanisms in relation to ICC loss/dysfunction, remark on the limited contribution of the current treatments, and propose intervention strategies to overcome ICC deficits. Finally, we address the advances and new research avenues offered by organoids and tissue engineering technologies, and propose schemes to implement to further our understanding of the GI pathology and utility in regenerative and personalized medicine in MNGIE. Conclusion Interstitial cells of Cajal play key roles in the physiology of the gastrointestinal motility. Evaluation of their status in the GI dysmotility related to MNGIE would be valuable for diagnosis of MNGIE. Understanding the underlying pathological and molecular mechanisms affecting ICC is an asset for the development of targeted prevention and treatment strategies for the GI dysmotility related to MNGIE.

Published

2019

16. Biallelic variants in LIG3 cause a novel mitochondrial neurogastrointestinal encephalomyopathy.

Author

Bonora, Elena, Chakrabarty, Sanjiban, Kellaris, Georgios, Tsutsumi, Makiko, Bianco, Francesca, Bergamini, Christian, Ullah, Farid, Isidori, Federica, Liparulo, Irene, Diquigiovanni, Chiara, Masin, Luca, Rizzardi, Nicola, Cratere, Mariapia Giuditta, Boschetti, Elisa, Papa, Valentina, Maresca, Alessandra, Cenacchi, Giovanna, Casadio, Rita, Martelli, Pierluigi, and Matera, Ivana

Subjects

*MITOCHONDRIAL pathology, *MITOCHONDRIAL DNA, *MITOCHONDRIA, *DNA ligases, *GENETIC variation, *CYTOCHROME oxidase, *GASTROINTESTINAL motility, *RESEARCH, *GENETIC mutation, *RESEARCH methodology, *GASTROINTESTINAL diseases, *MEDICAL cooperation, *EVALUATION research, *MITOCHONDRIAL encephalomyopathies, *COMPARATIVE studies, *FISHES, *GENETIC techniques, *GENEALOGY

Abstract

Abnormal gut motility is a feature of several mitochondrial encephalomyopathies, and mutations in genes such as TYMP and POLG, have been linked to these rare diseases. The human genome encodes three DNA ligases, of which only one, ligase III (LIG3), has a mitochondrial splice variant and is crucial for mitochondrial health. We investigated the effect of reduced LIG3 activity and resulting mitochondrial dysfunction in seven patients from three independent families, who showed the common occurrence of gut dysmotility and neurological manifestations reminiscent of mitochondrial neurogastrointestinal encephalomyopathy. DNA from these patients was subjected to whole exome sequencing. In all patients, compound heterozygous variants in a new disease gene, LIG3, were identified. All variants were predicted to have a damaging effect on the protein. The LIG3 gene encodes the only mitochondrial DNA (mtDNA) ligase and therefore plays a pivotal role in mtDNA repair and replication. In vitro assays in patient-derived cells showed a decrease in LIG3 protein levels and ligase activity. We demonstrated that the LIG3 gene defects affect mtDNA maintenance, leading to mtDNA depletion without the accumulation of multiple deletions as observed in other mitochondrial disorders. This mitochondrial dysfunction is likely to cause the phenotypes observed in these patients. The most prominent and consistent clinical signs were severe gut dysmotility and neurological abnormalities, including leukoencephalopathy, epilepsy, migraine, stroke-like episodes, and neurogenic bladder. A decrease in the number of myenteric neurons, and increased fibrosis and elastin levels were the most prominent changes in the gut. Cytochrome c oxidase (COX) deficient fibres in skeletal muscle were also observed. Disruption of lig3 in zebrafish reproduced the brain alterations and impaired gut transit in vivo. In conclusion, we identified variants in the LIG3 gene that result in a mitochondrial disease characterized by predominant gut dysmotility, encephalopathy, and neuromuscular abnormalities. [ABSTRACT FROM AUTHOR]

Published

2021

17. Efficacy of adeno-associated virus gene therapy in a MNGIE murine model enhanced by chronic exposure to nucleosides

Author

Ferran Vila-Julià, Raquel Cabrera-Pérez, Yolanda Cámara, Miguel Molina-Berenguer, Silvia Lope-Piedrafita, Michio Hirano, Federico Mingozzi, Javier Torres-Torronteras, and Ramon Martí

Subjects

MNGIE, Gene therapy, Nucleosides, Mitochondrial disease, Thymidine phosphorylase, Medicine, Medicine (General), R5-920

Abstract

Background: Preclinical studies have shown that gene therapy is a feasible approach to treat mitochondrial neurogastrointestinal encephalomyopathy (MNGIE). However, the genetic murine model of the disease (Tymp/Upp1 double knockout, dKO) has a limited functional phenotype beyond the metabolic imbalances, and so the studies showing efficacy of gene therapy have relied almost exclusively on demonstrating correction of the biochemical phenotype. Chronic oral administration of thymidine (dThd) and deoxyuridine (dUrd) to dKO mice deteriorates the phenotype of the animals, providing a better model to test therapy approaches. Methods: dKO mice were treated with both dThd and dUrd in drinking water from weaning until the end of the study. At 8 - 11 weeks of age, mice were treated with several doses of adeno-associated virus (AAV) serotype 8 vector carrying the human TYMP coding sequence under the control of different liver-specific promoters (TBG, AAT, or HLP). The biochemical profile and functional phenotype were studied over the life of the animals. Findings: Nucleoside exposure resulted in 30-fold higher plasma nucleoside levels in dKO mice compared with non-exposed wild type mice. AAV-treatment provided elevated TP activity in liver and lowered systemic nucleoside levels in exposed dKO mice. Exposed dKO mice had enlarged brain ventricles (assessed by magnetic resonance imaging) and motor impairment (rotarod test); both were prevented by AAV treatment. Among all promoters tested, AAT showed the best efficacy. Interpretation: Our results show that AAV-mediated gene therapy restores the biochemical homeostasis in the murine model of MNGIE and, for the first time, demonstrate that this treatment improves the functional phenotype. Funding: This work was funded in part by the Spanish Instituto de Salud Carlos III, and the Generalitat de Catalunya. The disclosed funders had no role in study design, data collection and analysis, decision to publish, or preparation of the manuscript.

Published

2020

18. Preclinical Efficacy and Safety Evaluation of Hematopoietic Stem Cell Gene Therapy in a Mouse Model of MNGIE

Author

Rana Yadak, Raquel Cabrera-Pérez, Javier Torres-Torronteras, Marianna Bugiani, Joost C. Haeck, Marshall W. Huston, Elly Bogaerts, Steffi Goffart, Edwin H. Jacobs, Merel Stok, Lorena Leonardelli, Luca Biasco, Robert M. Verdijk, Monique R. Bernsen, George Ruijter, Ramon Martí, Gerard Wagemaker, Niek P. van Til, and Irenaeus F.M. de Coo

Subjects

MNGIE, thymidine phosphorylase, hematopoietic stem cells, lentiviral vectors, gene therapy, Genetics, QH426-470, Cytology, QH573-671

Abstract

Mitochondrial neurogastrointestinal encephalomyopathy (MNGIE) is an autosomal recessive disorder caused by thymidine phosphorylase (TP) deficiency resulting in systemic accumulation of thymidine (d-Thd) and deoxyuridine (d-Urd) and characterized by early-onset neurological and gastrointestinal symptoms. Long-term effective and safe treatment is not available. Allogeneic bone marrow transplantation may improve clinical manifestations but carries disease and transplant-related risks. In this study, lentiviral vector-based hematopoietic stem cell gene therapy (HSCGT) was performed in Tymp−/−Upp1−/− mice with the human phosphoglycerate kinase (PGK) promoter driving TYMP. Supranormal blood TP activity reduced intestinal nucleoside levels significantly at low vector copy number (median, 1.3; range, 0.2–3.6). Furthermore, we covered two major issues not addressed before. First, we demonstrate aberrant morphology of brain astrocytes in areas of spongy degeneration, which was reversed by HSCGT. Second, long-term follow-up and vector integration site analysis were performed to assess safety of the therapeutic LV vectors in depth. This report confirms and supplements previous work on the efficacy of HSCGT in reducing the toxic metabolites in Tymp−/−Upp1−/− mice, using a clinically applicable gene transfer vector and a highly efficient gene transfer method, and importantly demonstrates phenotypic correction with a favorable risk profile, warranting further development toward clinical implementation.

Published

2018

19. Successful liver transplantation in mitochondrial neurogastrointestinal encephalomyopathy (MNGIE).

Author

Kripps, KimberlyA., Nakayuenyongsuk, Warapan, Shayota, Brian J., Berquist, William, Gomez-Ospina, Natalia, Esquivel, Carlos O., Concepcion, Waldo, Sampson, Jacinda B., Cristin, David J., Jackson, Whitney E., Gilliland, Samuel, Pomfret, Elizabeth A., Kueht, Michael L., Pettit, Rowland W., Sherif, Youmna A., Emrick, Lisa T., Elsea, Sarah H., Himes, Ryan, Hirano, Michio, and Van Hove, Johan L.K.

Subjects

*LIVER transplantation, *HEMATOPOIETIC stem cells, *STEM cell transplantation, *THYMIDINE, *CIRRHOSIS of the liver, *CHOLANGITIS, *NATALIZUMAB

Abstract

Mitochondrial neurogastrointestinal encephalomyopathy (MNGIE) is a fatal disorder characterized by progressive gastrointestinal dysmotility, peripheral neuropathy, leukoencephalopathy, skeletal myopathy, ophthalmoparesis, and ptosis. MNGIE stems from deficient thymidine phosphorylase activity (TP) leading to toxic elevations of plasma thymidine. Hematopoietic stem cell transplant (HSCT) restores TP activity and halts disease progression but has high transplant-related morbidity and mortality. Liver transplant (LT) was reported to restore TP activity in two adult MNGIE patients. We report successful LT in four additional MNGIE patients, including a pediatric patient. Our patients were diagnosed between ages 14 months and 36 years with elevated thymidine levels and biallelic pathogenic variants in TYMP. Two patients presented with progressive gastrointestinal dysmotility, and three demonstrated progressive peripheral neuropathy with two suffering limitations in ambulation. Two patients, including the child, had liver dysfunction and cirrhosis. Following LT, thymidine levels nearly normalized in all four patients and remained low for the duration of follow-up. Disease symptoms stabilized in all patients, with some manifesting improvements, including intestinal function. No patient died, and LT appeared to have a more favorable safety profile than HSCT, especially when liver disease is present. Follow-up studies will need to document the long-term impact of this new approach on disease outcome. Take Home Message: Liver transplantation is effective in stabilizing symptoms and nearly normalizing thymidine levels in patients with mitochondrial neurogastrointestinal encephalomyopathy (MNGIE) and may have an improved safety profile over hematopoietic stem cell transplant. • Four patients underwent liver transplantation for MNGIE and all survived without major complications • All had significant biochemical improvement in thymidine levels • There was clinical stabilization of disease with short term follow up [ABSTRACT FROM AUTHOR]

Published

2020

20. Mitochondrial Disorders

Author

Bai, Renkui, Higgs, Jaimie D., and Leonard, Debra G.B., editor

Published

2016

21. Mitochondrial neurogastrointestinal encephalomyopathy in a Pakistani female: a case report 

Author

Khan, Zaraq Rashid, Karam, Alvina, ul Haq, Mian Ayaz, Aman, Aleena, and Karam, Ahmad Sharjeel

Published

2022

22. Hemodialysis in MNGIE transiently reduces serum and urine levels of thymidine and deoxyuridine, but not CSF levels and neurological function

Author

Benjamin Röeben, Justus Marquetand, Benjamin Bender, Heiko Billing, Tobias B. Haack, Iciar Sanchez-Albisua, Ludger Schöls, Henk J. Blom, and Matthis Synofzik

Subjects

MNGIE, Haemodialysis, Mitochondriopathy, Thymidine phosphorylases, Medicine

Abstract

Abstract Mitochondrial neurogastrointestinal encephalomyopathy (MNGIE) is a rare, autosomal-recessive mitochondrial disorder caused by TYMP mutations presenting with a multisystemic, often lethal syndrome of progressive leukoencephalopathy, ophthalmoparesis, demyelinating neuropathy, cachexia and gastrointestinal dysmotility. Hemodialysis (HMD) has been suggested as a treatment to reduce accumulation of thymidine and deoxyuridine. However, all studies so far have failed to measure the toxic metabolites in cerebrospinal fluid (CSF), which is the crucial compartment for CNS damage. Our study is the first prospective, longitudinal investigation, exploiting detailed serial testing of predefined clinical and molecular outcome parameters (including serial CSF assessments) in a 29-year-old MNGIE patient undergoing 1 year of extensive HMD. We demonstrate that HMD only transiently restores increased serum and urine levels of thymidine and deoxyuridine, but fails to reduce CSF levels of the toxic metabolites and is ineffective to influence neurological function. These findings have direct important implications for clinical practice: They prevent a burdensome, long-term invasive, but ultimately probably ineffective procedure in future MNGIE patients.

Published

2017

23. Mitochondrial diseases: advances and issues

Author

Scarpelli M, Todeschini A, Volonghi I, Padovani A, and Filosto M

Subjects

mitochondrial diseases, therapy, MNGIE, Medicine (General), R5-920, Genetics, QH426-470

Abstract

Mauro Scarpelli,1 Alice Todeschini,2 Irene Volonghi,2 Alessandro Padovani,2 Massimiliano Filosto2 1Department of Neuroscience, Unit of Neurology, Azienda Ospedaliera Universitaria Integrata Verona, Verona, Italy; 2Center for Neuromuscular Diseases and Neuropathies, Unit of Neurology, ASST “Spedali Civili”, University of Brescia, Brescia, Italy Abstract: Mitochondrial diseases (MDs) are a clinically heterogeneous group of disorders caused by a dysfunction of the mitochondrial respiratory chain. They can be related to mutation of genes encoded using either nuclear DNA or mitochondrial DNA. The advent of next generation sequencing and whole exome sequencing in studying the molecular bases of MDs will bring about a revolution in the field of mitochondrial medicine, also opening the possibility of better defining pathogenic mechanisms and developing novel therapeutic approaches for these devastating disorders. The canonical rules of mitochondrial medicine remain milestones, but novel issues have been raised following the use of advanced diagnostic technologies. Rigorous validation of the novel mutations detected using deep sequencing in patients with suspected MD, and a clear definition of the natural history, outcome measures, and biomarkers that could be usefully adopted in clinical trials, are mandatory goals for the scientific community. Today, therapy is often inadequate and mostly palliative. However, important advances have been made in treating some clinical entities, eg, mitochondrial neuro-gastrointestinal encephalomyopathy, for which approaches using allogeneic hematopoietic stem cell transplantation, orthotopic liver transplantation, and carrier erythrocyte entrapped thymidine phosphorylase enzyme therapy have recently been developed. Promising new treatment methods are being identified so that researchers, clinicians, and patients can join forces to change the history of these untreatable disorders. Keywords: mitochondrial diseases, therapy, MNGIE

Published

2017

24. POLG1 variants can at most cause MNGIE-like but not classic MNGIE phenotype.

Author

Finsterer J

Subjects

Humans, DNA Polymerase gamma genetics, Phenotype, DNA, Mitochondrial genetics, Mutation genetics, Intestinal Pseudo-Obstruction genetics, Ophthalmoplegia, Mitochondrial Encephalomyopathies genetics, Muscular Dystrophy, Oculopharyngeal

Abstract

Competing Interests: Declaration of Competing Interest The author declares that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest.

Published

2024

25. Mitochondrial Neurogastrointestinal Encephalomyopathy: Into the Fourth Decade, What We Have Learned So Far

Author

Dario Pacitti, Michelle Levene, Caterina Garone, Niranjanan Nirmalananthan, and Bridget E. Bax

Subjects

MNGIE, thymidine phosphorylase, mitochondrial disease, rare disease, deoxyribonucleoside, TYMP, Genetics, QH426-470

Abstract

Mitochondrial neurogastrointestinal encephalomyopathy (MNGIE) is an ultra-rare metabolic autosomal recessive disease, caused by mutations in the nuclear gene TYMP which encodes the enzyme thymidine phosphorylase. The resulting enzyme deficiency leads to a systemic accumulation of the deoxyribonucleosides thymidine and deoxyuridine, and ultimately mitochondrial failure due to a progressive acquisition of secondary mitochondrial DNA (mtDNA) mutations and mtDNA depletion. Clinically, MNGIE is characterized by gastrointestinal and neurological manifestations, including cachexia, gastrointestinal dysmotility, peripheral neuropathy, leukoencephalopathy, ophthalmoplegia and ptosis. The disease is progressively degenerative and leads to death at an average age of 37.6 years. As with the vast majority of rare diseases, patients with MNGIE face a number of unmet needs related to diagnostic delays, a lack of approved therapies, and non-specific clinical management. We provide here a comprehensive collation of the available knowledge of MNGIE since the disease was first described 42 years ago. This review includes symptomatology, diagnostic procedures and hurdles, in vitro and in vivo disease models that have enhanced our understanding of the disease pathology, and finally experimental therapeutic approaches under development. The ultimate aim of this review is to increase clinical awareness of MNGIE, thereby reducing diagnostic delay and improving patient access to putative treatments under investigation.

Published

2018

26. Alpha-1-Antitrypsin Promoter Improves the Efficacy of an Adeno-Associated Virus Vector for the Treatment of Mitochondrial Neurogastrointestinal Encephalomyopathy.

Author

Cabrera-Pérez, Raquel, Vila-Julià, Ferran, Hirano, Michio, Mingozzi, Federico, Torres-Torronteras, Javier, and Martí, Ramon

Subjects

*ADENO-associated virus, *SINGLE-stranded DNA, *PHOSPHOGLYCERATE kinase, *HEMATOPOIETIC stem cells, *MITOCHONDRIAL DNA, *DNA replication

Abstract

Mitochondrial neurogastrointestinal encephalomyopathy (MNGIE) is a devastating disease caused by mutations in TYMP, which encodes thymidine phosphorylase (TP). In MNGIE patients, TP dysfunction results in systemic thymidine and deoxyuridine overload, which interferes with mitochondrial DNA replication. Preclinical studies have shown that gene therapy using a lentiviral vector targeted to hematopoietic stem cells or an adeno-associated virus (AAV) vector transcriptionally targeted to liver are feasible approaches to treat MNGIE. Here, we studied the effect of various promoters (thyroxine-binding globulin [TBG], phosphoglycerate kinase [PGK], hybrid liver-specific promoter [HLP], and alpha-1-antitrypsin [AAT]) and DNA configuration (single stranded or self complementary) on expression of the TYMP transgene in the AAV8 serotype in a murine model of MNGIE. All vectors restored liver TP activity and normalized nucleoside homeostasis in mice. However, the liver-specific promoters TBG, HLP, and AAT were more effective than the constitutive PGK promoter, and the self-complementary DNA configuration did not provide any therapeutic advantage over the single-stranded configuration. Among all constructs, only AAV-AAT was effective in all mice treated at the lowest dose (5 × 1010 vector genomes/kg). As use of the AAT promoter will likely minimize the dose needed to achieve clinical efficacy as compared to the other promoters tested, we propose using the AAT promoter in the vector eventually designed for clinical use. [ABSTRACT FROM AUTHOR]

Published

2019

27. Gastrointestinal Dysmotility in MNGIE: from thymidine phosphorylase enzyme deficiency to altered interstitial cells of Cajal.

Author

Yadak, Rana, Breur, Marjolein, and Bugiani, Marianna

Subjects

*GASTROINTESTINAL diseases, *MITOCHONDRIAL neurogastrointestinal encephalopathy syndrome, *THYMIDINE, *DEOXYURIDINE triphosphate, *INTERSTITIAL cells

Abstract

Background: MNGIE is a rare and fatal disease in which absence of the enzyme thymidine phosphorylase induces systemic accumulation of thymidine and deoxyuridine and secondary mitochondrial DNA alterations. Gastrointestinal (GI) symptoms are frequently reported in MNGIE patients, however, they are not resolved with the current treatment interventions. Recently, our understanding of the GI pathology has increased, which rationalizes the pursuit of more targeted therapeutic strategies. In particular, interstitial cells of Cajal (ICC) play key roles in GI physiology and are involved in the pathogenesis of the GI dysmotility. However, understanding of the triggers of ICC deficits in MNGIE is lacking. Herein, we review the current knowledge about the pathology of GI dysmotility in MNGIE, discuss potential mechanisms in relation to ICC loss/dysfunction, remark on the limited contribution of the current treatments, and propose intervention strategies to overcome ICC deficits. Finally, we address the advances and new research avenues offered by organoids and tissue engineering technologies, and propose schemes to implement to further our understanding of the GI pathology and utility in regenerative and personalized medicine in MNGIE.Conclusion: Interstitial cells of Cajal play key roles in the physiology of the gastrointestinal motility. Evaluation of their status in the GI dysmotility related to MNGIE would be valuable for diagnosis of MNGIE. Understanding the underlying pathological and molecular mechanisms affecting ICC is an asset for the development of targeted prevention and treatment strategies for the GI dysmotility related to MNGIE. [ABSTRACT FROM AUTHOR]

Published

2019

28. Next generation sequencing in family with MNGIE syndrome associated to optic atrophy: Novel homozygous POLG mutation in the C-terminal sub-domain leading to mtDNA depletion.

Author

Felhi, Rahma, Sfaihi, Lamia, Charif, Majida, Desquiret-Dumas, Valerie, Bris, Céline, Goudenège, David, Ammar-Keskes, Leila, Hachicha, Mongia, Bonneau, Dominique, Procaccio, Vincent, Reynier, Pascal, Amati-Bonneau, Patrizia, Lenaers, Guy, and Fakhfakh, Faiza

Subjects

*MITOCHONDRIAL DNA, *MITOCHONDRIAL neurogastrointestinal encephalopathy syndrome, *LEBER'S hereditary optic atrophy, *THYMIDINE phosphorylase, *GLYCOSYLTRANSFERASES

Abstract

Abstract Introduction Mitochondrial diseases are a group of disorders caused mainly by the impairment of the mitochondrial oxidative phosphorylation process, due to mutations either in the mitochondrial or nuclear genome. Among them, the mitochondrial neuro-gastrointestinal encephalo-myopathy (MNGIE) syndrome affects adolescents or young adults, and is mostly caused by TYMP mutations encoding a cytosolic thymidine phosphorylase (TP). Patients and methods The present study reports the molecular investigation by next-generation re-sequencing of 281 nuclear genes, encoding mitochondrial proteins, of consanguineous family including two individuals with MNGIE syndrome associated to optic atrophy. Bioinformatic analysis was also performed in addition to mtDNA deletion screening and mtDNA copy number quantification in blood of the two patients which were carried out by solf clipping program and qPCR respectively. Results Next-generation re-sequencing revealed a novel homozygous c.2391G > T POLG mutation (p.M797I) co-occurring with the hypomorphic c.1311A > G OPA1 variant (p.I437M). Analysis of the mitochondrial genome in the two patients disclosed mtDNA depletion in blood, but no deletion. Bio-informatics investigations supported the pathogenicity of the novel POLG mutation that is located in the C-terminal subdomain and might change POLG 3D structure, stability and function. Conclusion The novel homozygous p.M797I POLG mutation is responsible for MNGIE combined to optic atrophy and mtDNA depletion in the two patients. Highlights • We reported 2 patients with MNGIE syndrome plus optic atrophy. • Novel homozygous POLG c.2391 G > T variation was reported. • The heterozygous OPA1 c.1311 A > G variation was reported. • mtDNA depletion was revealed in the two patients. [ABSTRACT FROM AUTHOR]

Published

2019

29. Discovery profiling and bioinformatics analysis of serum microRNA in Mitochondrial NeuroGastroIntestinal Encephalomyopathy (MNGIE).

Author

Levene, Michelle, Enguita, Francisco J., and Bax, Bridget E.

Subjects

*BLOOD serum analysis, *MICRORNA, *ENZYME deficiency, *PATHOLOGY, *METABOLIC disorders, *PHOSPHORYLASES

Abstract

Mitochondrial neurogastrointestinal encephalomyopathy (MNGIE) is a rare and fatal inherited metabolic disorder due to mutations in the nuclear TYMP gene and leads to a deficiency in the enzyme thymidine phosphorylase. This results in an accumulation of the deoxynucleosides, thymidine and deoxyuridine in the cellular and extracellular compartments, ultimately leading to mitochondrial failure. The understanding of the precise molecular mechanisms that underlie the disease pathology is limited, being hampered by the rarity of the disorder. Expression profiling of serum based mircoRNAs and subsequent bioinformatical analyses provide an approach to facilitate the identity of dysregulated genes and signalling pathways potentially involved in the pathogenesis of MNGIE. [ABSTRACT FROM AUTHOR]

Published

2018

30. Mitochondrial Neurogastrointestinal Encephalomyopathy Imitating Crohn's Disease: A Rare Cause of Malnutrition.

Author

Kučerová, Lenka, Dolina, Jiří, Dastych, Milan, Bartušek, Daniel, Honzík, Tomáš, Mazanec, Jan, and Kunovský, Lumír

Subjects

*MITOCHONDRIAL neurogastrointestinal encephalopathy syndrome, *MALNUTRITION diagnosis, *GENETIC disorder diagnosis, *THYMIDINE phosphorylase

Abstract

Mitochondrial neurogastrointestinal encephalomyopathy (MNGIE) is a rare autosomal recessive disease caused by a mutation in the TYMP gene encoding thymidine phosphorylase. MNGIE causes gastrointestinal and neurological symptoms in homozygous individuals and is often misdiagnosed as anorexia nervosa, inflammatory bowel disease, or celiac disease. We present the case of a 26-year-old female with MNGIE, who was initially diagnosed with anorexia nervosa and Crohn's disease. The diagnosis of MNGIE was established by biochemical confirmation of elevated serum and urine thymidine and deoxyuridine levels after multiple examinations and several years of disease progression and ineffective treatment. Subsequent molecular genetic testing demonstrated a homozygous TYMP gene mutation. MNGIE should be considered in patients with unexplained malnutrition, intestinal dysmotility, and atypical neurological symptoms. [ABSTRACT FROM AUTHOR]

Published

2018

31. Long-Term Sustained Effect of Liver-Targeted Adeno-Associated Virus Gene Therapy for Mitochondrial Neurogastrointestinal Encephalomyopathy.

Author

Torres-Torronteras, Javier, Cabrera-Pérez, Raquel, Vila-Julià, Ferran, Viscomi, Carlo, Cámara, Yolanda, Hirano, Michio, Zeviani, Massimo, and Martí, Ramon

Subjects

*LIVER disease treatment, *MELAS syndrome, *GENE therapy, *ADENO-associated virus, *THYMIDINE phosphorylase, *LABORATORY mice

Abstract

Mitochondrial neurogastrointestinal encephalomyopathy (MNGIE) is caused by mutations in TYMP, the gene encoding the enzyme thymidine phosphorylase (TP). TP dysfunction results in systemic accumulation of the noxious TP substrates thymidine and deoxyuridine. Gene therapy using either a lentiviral vector or adeno-associated vector (AAV) has proven to be a feasible strategy, as both vectors restore biochemical homeostasis in a murine model of the disease. This study shows that the effect of an AAV containing the TYMP coding sequence transcriptionally targeted to the liver persists long term in mice. Although the vector copy number was diluted and AAV-mediated liver TP activity eventually reduced or lost after 21 months at the lowest vector doses, the effect was sustained (with a negligible decrease in TP activity) and fully effective on nucleoside homeostasis for at least 21 months at a dose of 2 × 1012 vg/kg. Macroscopic visual inspection of the animals' organs at completion of the study showed no adverse effects associated with the treatment. These results further support the feasibility of gene therapy for MNGIE. [ABSTRACT FROM AUTHOR]

Published

2018

32. Preclinical developments of enzyme-loaded red blood cells

Author

Francesca Pierigè, Mauro Magnani, Luigia Rossi, and Alessandro Bregalda

Subjects

Erythrocytes, enzyme-loaded RBCs, hyperammonemia, medicine.medical_treatment, Pharmaceutical Science, 02 engineering and technology, Pharmacology, 030226 pharmacology & pharmacy, 03 medical and health sciences, Drug Delivery Systems, 0302 clinical medicine, In vivo, Alcohol detoxification, medicine, cancer, Tissue Distribution, MNGIE, PKU, bioreactors, red blood cells as drug delivery system, chemistry.chemical_classification, Immunogenicity, Cancer, Hyperammonemia, 021001 nanoscience & nanotechnology, medicine.disease, ANT, Enzyme, Pharmaceutical Preparations, chemistry, 0210 nano-technology

Abstract

Therapeutic enzymes are currently used in the treatment of several diseases. In most cases, the benefits are limited due to poorAmong the delivery systems, we focused on red blood cells for the delivery of therapeutic enzymes. Erythrocytes possess a long circulation time, a reduced immunogenicity, there is no need of chemical modifications and the encapsulated enzyme remains active because it is protected by the cell membrane. Here we discuss some representative applications of the preclinical developments of the field. Some of these are currently in clinic, others are approaching the clinic and others are illustrative of the development process. The selected examples are not always the most recent, but they are the most useful for a comparative approach.The results discussed confirm the central role that red blood cells can play in the treatment of several conditions and suggest the benefit in using a natural cellular carrier in terms of pharmacokinetic, biodistribution, safety, and efficacy.

Published

2020

33. Hemodialysis in MNGIE transiently reduces serum and urine levels of thymidine and deoxyuridine, but not CSF levels and neurological function.

Author

Röeben, Benjamin, Marquetand, Justus, Bender, Benjamin, Billing, Heiko, Haack, Tobias B., Sanchez-Albisua, Iciar, Schöls, Ludger, Blom, Henk J., and Synofzik, Matthis

Subjects

*HEMODIALYSIS, *MITOCHONDRIAL neurogastrointestinal encephalopathy syndrome, *THYMIDINE phosphorylase, *DEOXYURIDINE triphosphate, *CEREBROSPINAL fluid, *CENTRAL nervous system diseases, *BOWEL obstructions, *GENETIC mutation, *TRANSFERASES, *SYMPTOMS, *DEOXYRIBONUCLEOSIDES, *MITOCHONDRIAL encephalomyopathies, *THERAPEUTICS

Abstract

Mitochondrial neurogastrointestinal encephalomyopathy (MNGIE) is a rare, autosomal-recessive mitochondrial disorder caused by TYMP mutations presenting with a multisystemic, often lethal syndrome of progressive leukoencephalopathy, ophthalmoparesis, demyelinating neuropathy, cachexia and gastrointestinal dysmotility. Hemodialysis (HMD) has been suggested as a treatment to reduce accumulation of thymidine and deoxyuridine. However, all studies so far have failed to measure the toxic metabolites in cerebrospinal fluid (CSF), which is the crucial compartment for CNS damage.Our study is the first prospective, longitudinal investigation, exploiting detailed serial testing of predefined clinical and molecular outcome parameters (including serial CSF assessments) in a 29-year-old MNGIE patient undergoing 1 year of extensive HMD. We demonstrate that HMD only transiently restores increased serum and urine levels of thymidine and deoxyuridine, but fails to reduce CSF levels of the toxic metabolites and is ineffective to influence neurological function. These findings have direct important implications for clinical practice: They prevent a burdensome, long-term invasive, but ultimately probably ineffective procedure in future MNGIE patients. [ABSTRACT FROM AUTHOR]

Published

2017

34. Mitochondrial Neurogastrointestinal Encephalomyopathy Caused by Thymidine Phosphorylase Enzyme Deficiency: From Pathogenesis to Emerging Therapeutic Options.

Author

Yadak, Rana, Smitt, Peter Sillevis, van Gisbergen, Marike W., van Til, Niek P., and de Coo, Irenaeus F. M.

Subjects

MITOCHONDRIAL pathology, METABOLIC disorders, THYMIDINE phosphorylase, ENZYME deficiency, DEOXYRIBONUCLEOSIDES, THYMIDINE

Abstract

Mitochondrial neurogastrointestinal encephalomyopathy (MNGIE) is a progressive metabolic disorder caused by thymidine phosphorylase (TP) enzyme deficiency. The lack of TP results in systemic accumulation of deoxyribonucleosides thymidine (dThd) and deoxyuridine (dUrd). In these patients, clinical features include mental regression, ophthalmoplegia, and fatal gastrointestinal complications. The accumulation of nucleosides also causes imbalances in mitochondrial DNA (mtDNA) deoxyribonucleoside triphosphates (dNTPs), which may play a direct or indirect role in the mtDNA depletion/deletion abnormalities, although the exact underlying mechanism remains unknown. The available therapeutic approaches include dialysis and enzyme replacement therapy, both can only transiently reverse the biochemical imbalance. Allogeneic hematopoietic stem cell transplantation is shown to be able to restore normal enzyme activity and improve clinical manifestations in MNGIE patients. However, transplant related complications and disease progression result in a high mortality rate. New therapeutic approaches, such as adeno-associated viral vector and hematopoietic stem cell gene therapy have been tested in Tymp-/-Upp1-/- mice, a murine model for MNGIE. This review provides background information on disease manifestations of MNGIE with a focus on current management and treatment options. It also outlines the pre-clinical approaches toward future treatment of the disease. [ABSTRACT FROM AUTHOR]

Published

2017

35. Hematopoietic stem cell transplantation with reduced toxicity conditioning regimen in mitochondrial neurogastrointestinal encephalopathy syndrome.

Author

Ozek G, Aksoylar S, Uçar SK, Canda E, Akcan M, Cartı O, Siviş ZO, Oymak Y, Yazıcı H, Bax B, Bulut FD, Yoldaş Çelik M, Erdem F, Çoker M, and Kansoy S

Subjects

Humans, Retrospective Studies, Transplantation, Homologous methods, Transplantation Conditioning methods, Hematopoietic Stem Cell Transplantation adverse effects, Graft vs Host Disease etiology

Abstract

Background: Mitochondrial neurogastrointestinal encephalomyopathy (MNGIE) is a rare autosomal recessive disorder due to mutations in the TYMP gene. Clinical findings are characterized by neurologic manifestations and severe gastrointestinal dysfunction. The syndrome is usually fatal, the most effective treatment appears to be hematopoietic stem cell transplantation (HSCT)., Procedure: In this retrospective study, we evaluated HSCT that was performed using a reduced toxicity myeloablative conditioning regimen in patients with MNGIE at our center., Results: A total of six allogeneic transplant procedures were performed in four patients. Three patients had fully matched donors, and one patient had a haploidentical donor. Treosulfan-based myeloablative conditioning regimen was applied in five of six transplants. Bone marrow was used as a stem cell source. One patient is being followed up in the 4th year of posttransplant with full chimeric and without graft versus host disease (GVHD). One patient died of acute stage IV gastrointestinal system GVHD. Two patients underwent second transplantation due to engraftment failure, one of which was the patient who had a haploidentical transplant., Conclusions: Treosulfan-based regimen is well tolerated, although engraftment failure with this conditioning regimen can be a significant problem. We share our haploidentical transplant experience, which will be the first reported case in the literature., (© 2023 The Authors. Pediatric Blood & Cancer published by Wiley Periodicals LLC.)

Published

2023

36. Leukoencephalopathy with a case of heterozygous POLG mutation mimicking mitochondrial neurogastrointestinal encephalomyopathy (MNGIE).

Author

Yasuda, Ken, Murase, Nagako, Yoshinaga, Kenji, Ohtani, Ryo, Goto, Yu-ichi, Takahashi, Ryosuke, and Nakamura, Michikazu

Abstract

Highlights • Several studies have been reported on POLG1 mutations MNGIE-like phenotype. • POLG1 mutations mimicking MNGIE usually lack leukoencephalopathy or demyelinating neuropathy. • We report POLG1 mutation mimicking MNGIE with leukoencephalopathy and demyelinating neuropathy. Abstract Diseases due to mutations of polymerase γ (POLG) usually present with progressive external ophthalmoplegia. However, a few studies have been reported on POLG1 mutations with the mitochondrial neurogastrointestinal encephalomyopathy (MNGIE)-like phenotype. All cases with POLG1 mutations mimicking MNGIE have never shown leukoencephalopathy on brain magnetic resonance imaging (MRI) or demyelinating polyneuropathy. We present a 26-year-old male with gait disturbance, recurrent bowel obstruction, peripheral neuropathy, ophthalmoplegia or ptosis, which represented MNGIE phenotype. Though he displayed demyelinating peripheral neuropathy or leukoencephalopathy on brain MRI, genetic analysis revealed heterozygous mutation in POLG1 gene. We report for the first time two newly characteristics in our patient with heterozygous POLG1 mutations with the MNGIE-like phenotype: leukoencephalopathy and demyelinating polyneuropathy. [ABSTRACT FROM AUTHOR]

Published

2019

37. Mitochondrial Medicine in the COVID-19 Era

Author

Daniele Orsucci

Subjects

Mitochondrial DNA, 2019-20 coronavirus outbreak, Coronavirus disease 2019 (COVID-19), Mitochondrial disease, Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), NARP, MERRF, CPEO, Mitochondrial myopathy, medicine, Leber, business.industry, mtDNA, mitochondrial myopathy, General Medicine, medicine.disease, Electron transport chain, Virology, Leigh syndrome, Mitochondrial respiratory chain, Editorial, PEO, MNGIE, MELAS, Medicine, business

Abstract

Mitochondrial disorders are a remarkably complex group of diseases caused by impairment of the mitochondrial respiratory chain (or electron transport chain) [...]

Published

2021

38. Mitochondrial neurogastrointestinal encephalomyopathy: Clinical and biochemical impact of allogeneic stem cell transplantation in a Greek patient with one novel

Author

A. Paisiou, M. Rogalidou, R. Pons, E. Ioannidou, K. Dimakou, A. Papadopoulou, F.M. Vaz, G. Vessalas, S.M.I. Goorden, J. Roelofsen, A. Zoetekouw, M.M. Nieman, E. Dimitriou, M. Moraitou, I. Peristeri, H. Michelakakis, and A.B.P. van Kuilenburg

Subjects

Medicine (General), QH301-705.5, dThd, thymidine, HSCT, hematopoietic stem cell transplantation, Endocrinology, R5-920, CSF, cerebrospinal fluid, Genetics, AHSCT, allogeneic hematopoietic stem cell transplantation, Biology (General), Molecular Biology, dUrd, 2′-deoxyuridine, MNGIE, mitochondrial neurogastrointestinal encephalomyopathy, PB, peripheral blood, TP, thymidine phosphorylase, TPN, total parenteral nutrition, TYMP, thymidine phosphorylase gene, VLCFA, very long chain fatty acids, Mutation analysis, mtDNA, mitochondrial DNA, GVHD, Graft Versus Host Disease, OLT, orthotopic liver transplantation, MNGIE, Allogeneic hematopoietic stem cell transplantation, AHSCT, Mitochondrial neurogastrointestinal encephalomyopathy, PLT, platelet, Research Paper

Abstract

We describe the case of a Greek female patient with the Classic form of the ultra- rare and fatal autosomal recessive disorder Mitochondrial neurogastrointestinal encephalomyopathy (MNGIE) and the impact of allogeneic hematopoietic stem cell transplantation on the biochemical and clinical aspects of the disease. The patient presented at the age of 15 years with severe gastrointestinal symptoms, cachexia, peripheral neuropathy and diffuse leukoencephalopathy. The diagnosis of MNGIE disease was established by the increased levels of thymidine and deoxyuridine in plasma and the complete deficiency of thymidine phosphorylase activity. The novel c.[978dup] (p.Ala327Argfs*?) variant and the previously described variant c.[417 + 1G > A] were identified in TYMP. The donor for the allogeneic hematopoietic stem cell transplantation was her fully compatible sister, a carrier of the disease. The patient had a completely uneventful post- transplant period and satisfactory PB chimerism levels. A marked and rapid decrease in thymidine and deoxyuridine plasma levels and an increase of the thymidine phosphorylase activity to the levels measured in her donor sister was observed and is still present sixteen months post-transplant. Disease symptoms stabilized and some improvement was also observed both in her neurological and gastrointestinal symptoms. Follow up studies will be essential for determining the long term impact of allogeneic hematopoietic stem cell transplantation in our patient.

Published

2021

39. A Novel Mutation in an MNGIE Patient Presenting with More Prominent Neurological Symptoms than GI Symptoms.

Author

Chen X, Xiong X, Liu S, Duan C, Xu R, and Yang Q

Subjects

Humans, Female, Adult, Thymidine Phosphorylase genetics, Mutation genetics, Genetic Testing, Mitochondrial Encephalomyopathies complications, Mitochondrial Encephalomyopathies diagnosis, Mitochondrial Encephalomyopathies genetics

Abstract

Mitochondrial neurogastrointestinal encephalopathy (MNGIE) is an autosomal recessive disease associated with the mutation of the TYMP gene. MNGIE causes gastrointestinal and neurological symptoms, and the gastrointestinal symptoms are usually notable, which may lead to misdiagnosis. However, we herein report a 29-year-old female who presented with prominent neurological symptoms, while her gastrointestinal symptoms were mild. Brain MRI revealed prominent diffused leukoencephalopathy and peripheral neuropathy was confirmed by the nerve conduction velocity test. Biochemical tests showed elevated plasma thymidine, deoxyuridine, and lactate levels. Molecular genetic testing demonstrated a novel homozygous TYMP c. 447 dupG mutation and the patient's mother was heterozygous for the mutation but had no clinical features. MNGIE was diagnosed based on the results. Unlike other patients who had notable gastrointestinal symptoms, this patient presented with more prominent neurological symptoms than gastrointestinal symptoms, which might have been caused by the novel mutation in the TYMP gene., Competing Interests: None

Published

2023

40. A celiac case mimicking mitochondrial neurogastrointestinal encephalomyopathy (MNGIE).

Author

Aksoy, Erhan, Tıraþ-Teber, Serap, and Deda, Gülhis

Abstract

Celiac disease (CD) is a chronic disease involving a number of systems in addition to gastrointestinal tract. Although not clear, it has been supposed that the neurological symptoms of CD develop due to immune-mediated mechanisms. In this paper, we present a rare case diagnosed with CD at 12 years of age, and presented with a clinical picture resembling mitochondrial neurogastrointestinal encephalomyopathy (MNGIE). She had onset of her neurological symptoms at the age of 6 years, they progressed despite various therapies, and she became wheelchair-bound. [ABSTRACT FROM AUTHOR]

Published

2016

41. MITOCHONDRIAL NEUROGASTROINTESTINAL ENCEPHALOMYOPATHY (MNGIE)

Author

P. Ayatollahi and A. Tarazi S. Nafissi

Subjects

MNGIE, mitochondrial encephalomyopathy, cachexia, ophthalmoparesis, Medicine (General), R5-920

Abstract

Mitochondrial neurogastrointestinal encephalo-myopathy (MNGIE) is a rare autosomal recessive disease caused by thymidine phosphorylase (TP) gene mutation. Here we report a patient with MNGIE in whom sensorimotor polyneuropathy was the first presenting symptom and had a fluctuating course. This 26-year-old female patient developed acute-onset demyelinating polyneuropathy from the age of 6 with two relapses later on. In addition, she had gastrointestinal symptoms (diarrhea, recurrent abdominal pain), progressive weight loss and ophthalmoparesis. Brain magnetic resonance imaging showed white matter abnormalities, and muscle biopsy showed ragged red fibers. This constellation of clinical and laboratory findings raised the diagnosis of mitochondrial neurogastrointestinal encephalomyopathy (MNGIE). This report highlights the uncommon clinical characteristics of this rare disease.

Published

2006

42. Peripheral neuropathy is a common manifestation of mitochondrial diseases: a single-centre experience.

Author

Luigetti, M., Sauchelli, D., Primiano, G., Cuccagna, C., Bernardo, D., Lo Monaco, M., and Servidei, S.

Subjects

*PERIPHERAL neuropathy, *MITOCHONDRIA, *MITOCHONDRIAL pathology, *PERIPHERAL nervous system, *MERRF syndrome

Abstract

Background and purpose Peripheral neuropathy in mitochondrial diseases ( MDs) may vary from a subclinical finding in a multisystem syndrome to a severe, even isolated, manifestation in some patients. Methods To investigate the involvement of the peripheral nervous system in MDs extensive electrophysiological studies were performed in 109 patients with morphological, biochemical and genetic diagnosis of MD [12 A3243G progressive external ophthalmoplegia ( PEO)/mitochondrial encephalomyopathy, lactic acidosis and stroke-like episodes ( MELAS), 16 myoclonic epilepsy with ragged-red fibres ( MERRF), four mitochondrial neurogastrointestinal encephalomyopathy ( MNGIE), 67 PEO with single or multiple deletions of mitochondrial DNA, 10 others]. Results A neuropathy was found in 49 patients (45%). The incidence was very high in MNGIE (100%), MELAS (92%) and MERRF (69%), whilst 28% of PEO patients had evidence of peripheral involvement. The most frequent abnormality was a sensory axonal neuropathy found in 32/49 patients (65%). A sensory-motor axonal neuropathy was instead detected in 16% of the patients and sensory-motor axonal demyelinating neuropathy in 16%. Finally one Leigh patient had a motor axonal neuropathy. It is interesting to note that the great majority had preserved tendon reflexes and no sensory disturbances. Conclusions In conclusion, peripheral involvement in MD is frequent even if often mild or asymptomatic. The correct identification and characterization of peripheral neuropathy through electrophysiological studies represents another tile in the challenge of MD diagnosis. [ABSTRACT FROM AUTHOR]

Published

2016

43. Next generation sequencing in family with MNGIE syndrome associated to optic atrophy: Novel homozygous POLG mutation in the C-terminal sub-domain leading to mtDNA depletion

Author

David Goudenège, Pascal Reynier, Majida Charif, Rahma Felhi, Dominique Bonneau, Mongia Hachicha, Lamia Sfaihi, Céline Bris, Leila Ammar-Keskes, Guy Lenaers, Patrizia Amati-Bonneau, Valérie Desquiret-Dumas, Vincent Procaccio, Faiza Fakhfakh, Physiopathologie Cardiovasculaire et Mitochondriale (MITOVASC), Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS)-Université d'Angers (UA), Hedi Chaker Hospital [Sfax], Biologie Neurovasculaire et Mitochondriale Intégrée (BNMI), Université d'Angers (UA)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS), Department of Pediatrics, Mitochondrie : Régulations et Pathologie, Université d'Angers (UA)-Institut National de la Santé et de la Recherche Médicale (INSERM), Physiopathologie et thérapie des déficits sensoriels et moteurs, Université Montpellier 2 - Sciences et Techniques (UM2)-IFR76-Institut National de la Santé et de la Recherche Médicale (INSERM), Laboratoire de Génétique Moléculaire Humaine, Faculté de Médecine de Sfax, This work was supported by the Ministry of Higher Education and Scientific Research in Tunisia, University of Sfax. We acknowledge the support from the Institut National de la Santé et de la Recherche Médicale (INSERM), France, Centre National de la Recherche Scientifique (CNRS), France, the Université d'Angers, the University Hospital of Angers, the Région Pays de Loire and Angers Loire Métropole, France., and We would like to thank all the member of the family for their cooperation in the present study.

Subjects

Male, 0301 basic medicine, Mitochondrial DNA, Nuclear gene, Adolescent, [SDV]Life Sciences [q-bio], Clinical Biochemistry, MtDNA depletion, Oxidative phosphorylation, Biology, OPA1, DNA, Mitochondrial, Biochemistry, DNA sequencing, 03 medical and health sciences, 0302 clinical medicine, Atrophy, Muscular Dystrophy, Oculopharyngeal, Mitochondrial Encephalomyopathies, medicine, Humans, Thymidine phosphorylase, Child, ComputingMilieux_MISCELLANEOUS, Genetics, Ophthalmoplegia, mtDNA depletion, Intestinal Pseudo-Obstruction, Biochemistry (medical), Pathogenic variants, General Medicine, medicine.disease, DNA Polymerase gamma, 3. Good health, Optic Atrophy, Cytosol, 030104 developmental biology, POLG, 030220 oncology & carcinogenesis, MNGIE, Mutation

Abstract

Introduction Mitochondrial diseases are a group of disorders caused mainly by the impairment of the mitochondrial oxidative phosphorylation process, due to mutations either in the mitochondrial or nuclear genome. Among them, the mitochondrial neuro-gastrointestinal encephalo-myopathy (MNGIE) syndrome affects adolescents or young adults, and is mostly caused by TYMP mutations encoding a cytosolic thymidine phosphorylase (TP). Patients and methods The present study reports the molecular investigation by next-generation re-sequencing of 281 nuclear genes, encoding mitochondrial proteins, of consanguineous family including two individuals with MNGIE syndrome associated to optic atrophy. Bioinformatic analysis was also performed in addition to mtDNA deletion screening and mtDNA copy number quantification in blood of the two patients which were carried out by solf clipping program and qPCR respectively. Results Next-generation re-sequencing revealed a novel homozygous c.2391G > T POLG mutation (p.M797I) co-occurring with the hypomorphic c.1311A > G OPA1 variant (p.I437M). Analysis of the mitochondrial genome in the two patients disclosed mtDNA depletion in blood, but no deletion. Bio-informatics investigations supported the pathogenicity of the novel POLG mutation that is located in the C-terminal subdomain and might change POLG 3D structure, stability and function. Conclusion The novel homozygous p.M797I POLG mutation is responsible for MNGIE combined to optic atrophy and mtDNA depletion in the two patients.

Published

2019

44. Anatomical Laser Microdissection of the Ileum Reveals mtDNA Depletion Recovery in A Mitochondrial Neuro-Gastrointestinal Encephalomyopathy (MNGIE) Patient Receiving Liver Transplant

Author

Elisa Boschetti, Leonardo Caporali, Roberto D’Angelo, Carolina Malagelada, Anna Accarino, Maria Teresa Dotti, Roberta Costa, Giovanna Cenacchi, Loris Pironi, Rita Rinaldi, Vincenzo Stanghellini, Stefano Ratti, Lucia Manzoli, Valerio Carelli, Roberto De Giorgio, Institut Català de la Salut, [Boschetti E] Department of Biomedical and Neuromotor Sciences (DIBINEM), University of Bologna, Bologna, Italy. IRCCS Azienda Ospedaliero-Universitaria di Bologna, Bologna, Italy. [Caporali L] IRCCS Istituto delle Scienze Neurologiche di Bologna, Bologna, Italy. [D'Angelo R] IRCCS Azienda Ospedaliero-Universitaria di Bologna, Bologna, Italy. [Malagelada C, Accarino A] Centro de Investigacion Biomedica en Red de Enfermedades Hepáticas y Digestivas (CIBEREHD), Barcelona, Spain. Vall d’Hebron Hospital Universitari, Barcelona, Spain. Departament de Medicina, Universitat Autònoma de Barcelona, Bellaterra, Spain. [Dotti MT] Department of Medical, Surgical and Neurological Sciences, University of Siena, Siena, Italy, Vall d'Hebron Barcelona Hospital Campus, Boschetti, Elisa, Caporali, Leonardo, D'Angelo, Roberto, Malagelada, Carolina, Accarino, Anna, Dotti, Maria Teresa, Costa, Roberta, Cenacchi, Giovanna, Pironi, Lori, Rinaldi, Rita, Stanghellini, Vincenzo, Ratti, Stefano, Manzoli, Lucia, Carelli, Valerio, and De Giorgio, Roberto

Subjects

gastrointestinal degeneration, Investigative Techniques::Investigative Techniques::Micromanipulation::Microdissection::Laser Capture Microdissection [ANALYTICAL, DIAGNOSTIC AND THERAPEUTIC TECHNIQUES, AND EQUIPMENT], Laser, Fetge - Trasplantació, ADN mitocondrial, Laser Capture Microdissection, Encefalomielitis, DNA, Mitochondrial, Catalysis, Inorganic Chemistry, Nucleic Acids, Nucleotides, and Nucleosides::Nucleic Acids::DNA::DNA, Circular::DNA, Mitochondrial [CHEMICALS AND DRUGS], Ileum, Mitochondrial Encephalomyopathies, nucleótidos y nucleósidos de ácidos nucleicos::ácidos nucleicos::ADN::ADN circular::ADN mitocondrial [COMPUESTOS QUÍMICOS Y DROGAS], mitochondrial disorder, Humans, Physical and Theoretical Chemistry, Molecular Biology, Spectroscopy, enfermedades del sistema nervioso::enfermedades del sistema nervioso central::enfermedades cerebrales::enfermedades cerebrales metabólicas::enfermedades del sistema nervioso::encefalomiopatías mitocondriales [ENFERMEDADES], terapéutica::terapia biológica::tratamientos basados en células y tejidos::trasplante de tejidos::trasplante de hígado [TÉCNICAS Y EQUIPOS ANALÍTICOS, DIAGNÓSTICOS Y TERAPÉUTICOS], microanatomical dissection, mtDNA depletion, Nervous System Diseases::Central Nervous System Diseases::Brain Diseases::Brain Diseases, Metabolic::Nervous System Diseases::Mitochondrial Encephalomyopathies [DISEASES], Lasers, Organic Chemistry, General Medicine, mitochondrial disorders, MNGIE, Liver Transplantation, Computer Science Applications, técnicas de investigación::técnicas de investigación::micromanipulación::microdisección::microdisección por láser [TÉCNICAS Y EQUIPOS ANALÍTICOS, DIAGNÓSTICOS Y TERAPÉUTICOS], Therapeutics::Biological Therapy::Cell- and Tissue-Based Therapy::Tissue Transplantation::Liver Transplantation [ANALYTICAL, DIAGNOSTIC AND THERAPEUTIC TECHNIQUES, AND EQUIPMENT], Mitocondris - Malalties, Metabolism, Inborn Error, Metabolism, Inborn Errors, Human

Abstract

Microanatomical dissection; Mitochondrial disorders; MtDNA depletion Disección microanatómica; Trastornos mitocondriales; Agotamiento del ADNmt Dissecció microanatòmica; Trastorns mitocondrials; Esgotament de l'ADNmt Mitochondrial neuro-gastrointestinal encephalomyopathy (MNGIE) is a rare genetic disorder characterized by thymidine phosphorylase (TP) enzyme defect. The absence of TP activity induces the imbalance of mitochondrial nucleotide pool, leading to impaired mitochondrial DNA (mtDNA) replication and depletion. Since mtDNA is required to ensure oxidative phosphorylation, metabolically active tissues may not achieve sufficient energy production. The only effective life-saving approach in MNGIE has been the permanent replacement of TP via allogeneic hematopoietic stem cell or liver transplantation. However, the follow-up of transplanted patients showed that gut tissue changes do not revert and fatal complications, such as massive gastrointestinal bleeding, can occur. The purpose of this study was to clarify whether the reintroduction of TP after transplant can recover mtDNA copy number in a normal range. Using laser capture microdissection and droplet-digital-PCR, we assessed the mtDNA copy number in each layer of full-thickness ileal samples of a naive MNGIE cohort vs. controls and in a patient pre- and post-TP replacement. The treatment led to a significant recovery of gut tissue mtDNA amount, thus showing its efficacy. Our results indicate that a timely TP replacement is needed to maximize therapeutic success before irreversible degenerative tissue changes occur in MNGIE. The work was supported by Ministero dell’Istruzione, dell’Università e della Ricerca-Dipartimenti eccellenti on the Project Personalized medicine. LC and VC are supported by the Italian Ministry of Health (Ricerca Corrente 2021 funding). RDG is supported by funds from the University of Ferrara.

Published

2022

45. Validation of an Immunoassay for Anti-thymidine Phosphorylase Antibodies in Patients with MNGIE Treated with Enzyme Replacement Therapy

Author

Jamie Hall, Marcia Sellos-Moura, Charlotte Gasson, Bridget E. Bax, Dario Pacitti, and Michelle Levene

Subjects

0301 basic medicine, lcsh:QH426-470, Pharmacology, thymidine phosphorylase, Article, 03 medical and health sciences, Glycogen phosphorylase, 0302 clinical medicine, Drug tolerance, Genetics, medicine, Thymidine phosphorylase, lcsh:QH573-671, Molecular Biology, medicine.diagnostic_test, biology, Chemistry, lcsh:Cytology, Immunogenicity, Assay sensitivity, Enzyme replacement therapy, assay validation, 3. Good health, bridging immunoassay, lcsh:Genetics, 030104 developmental biology, Immunoassay, MNGIE, biology.protein, Molecular Medicine, Antibody, 030217 neurology & neurosurgery, enzyme replacement therapy

Abstract

Erythrocyte encapsulated thymidine phosphorylase is recombinant Escherichia coli thymidine phosphorylase encapsulated within human autologous erythrocytes and is under development as an enzyme replacement therapy for the ultra-rare inherited metabolic disorder mitochondrial neurogastrointestinal encephalomyopathy. This study describes the method validation of a two-step bridging electrochemiluminescence immunoassay for the detection of anti-thymidine phosphorylase antibodies in human serum according to current industry practice and regulatory guidelines. The analytical method was assessed for screening cut point, specificity, selectivity, precision, prozone effect, drug tolerance, and stability. Key findings were a correction factor of 129 relative light units for the cut-point determination; a specificity cut point of 93% inhibition; confirmed intra-assay and inter-assay precision; assay sensitivity of 356 ng/mL; no matrix or prozone effects up to 25,900 ng/mL; a drug tolerance of 156 ng/mL; and stability at room temperature for 24 hr and up to five freeze-thaws. Immunogenicity evaluations of serum from three patients who received erythrocyte encapsulated thymidine phosphorylase under a compassionate treatment program showed specific anti-thymidine phosphorylase antibodies in one patient. To conclude, a sensitive, specific, and selective immunoassay has been validated for the measurement of anti-thymidine phosphorylase antibodies; this will be utilized in a phase II pivotal clinical trial of erythrocyte encapsulated thymidine phosphorylase. Keywords: assay validation, bridging immunoassay, enzyme replacement therapy, MNGIE, thymidine phosphorylase

Published

2018

46. Circulating miRNAs as Biomarkers for Mitochondrial Neuro-Gastrointestinal Encephalomyopathy

Author

Mark Mencias, Michelle Levene, Kevin Blighe, Bridget E. Bax, and on behalf of the Project Group

Subjects

Oncology, medicine.medical_specialty, Mitochondrial disease, miR-34a-5p, Disease, thymidine phosphorylase, Catalysis, Article, Inorganic Chemistry, lcsh:Chemistry, erythrocyte encapsulated thymidine phosphorylase, outcome measures, Muscular Dystrophy, Oculopharyngeal, Internal medicine, microRNA, medicine, Humans, Physical and Theoretical Chemistry, Thymidine phosphorylase, Molecular Biology, lcsh:QH301-705.5, Spectroscopy, miRNA, Ophthalmoplegia, business.industry, Gene Expression Profiling, Organic Chemistry, Intestinal Pseudo-Obstruction, Outcome measures, General Medicine, medicine.disease, Computer Science Applications, Clinical trial, MicroRNAs, mitochondrial disease, Real-time polymerase chain reaction, lcsh:Biology (General), lcsh:QD1-999, Case-Control Studies, MNGIE, Biomarker (medicine), biomarker, Mitochondrial neurogastrointestinal encephalomyopathy, business, Biomarkers

Abstract

Mitochondrial neurogastrointestinal encephalomyopathy (MNGIE) is an ultra-rare disease for which there are currently no validated outcome measures for assessing therapeutic intervention efficacy. The aim of this study was to identify a plasma and/or serum microRNA (miRNA) biomarker panel for MNGIE. Sixty-five patients and 65 age and sex matched healthy controls were recruited and assigned to one of four study phases: (i) discovery for sample size determination, (ii) candidate screening, (iii) candidate validation, and (iv) verifying the performance of the validated miRNA panel in four patients treated with erythrocyte-encapsulated thymidine phosphorylase (EE-TP), an enzyme replacement under development for MNGIE. Quantitative PCR (qPCR) was used to profile miRNAs in serum and/or plasma samples collected for the discovery, validation and performance phases, and next generation sequencing (NGS) analysis was applied to serum samples assigned to the candidate screening phase. Forty-one differentially expressed candidate miRNAs were identified in the sera of patients (p &lt, 0.05, log2 fold change &gt, 1). The validation cohort revealed that of those, 27 miRNAs were upregulated in plasma and three miRNAs were upregulated in sera (p &lt, 0.05). Through binary logistic regression analyses, five plasma miRNAs (miR-192-5p, miR-193a-5p, miR-194-5p, miR-215-5p and miR-34a-5p) and three serum miRNAs (miR-192-5p, miR-194-5p and miR-34a-5p) were shown to robustly distinguish MNGIE from healthy controls. Reduced longitudinal miRNA expression of miR-34a-5p was observed in all four patients treated with EE-TP and coincided with biochemical and clinical improvements. We recommend the inclusion of the plasma exploratory miRNA biomarker panel in future clinical trials of investigational therapies for MNGIE, it may have prognostic value for assessing clinical status.

Published

2021

47. Mitochondrial Syndromes Revisited

Author

Elena Caldarazzo Ienco, Daniele Orsucci, Andrea Rossi, Michelangelo Mancuso, and Gabriele Siciliano

Subjects

Mitochondrial DNA, Future studies, leber, Mitochondrial disease, lcsh:Medicine, Review, Bioinformatics, NARP, MERRF, 03 medical and health sciences, CPEO, 0302 clinical medicine, Mitochondrial myopathy, medicine, 030304 developmental biology, 0303 health sciences, business.industry, mtDNA, lcsh:R, mitochondrial myopathy, General Medicine, medicine.disease, Phenotype, Leigh syndrome, Clinical trial, Natural history, Homogeneous, PEO, MELAS, MNGIE, business, 030217 neurology & neurosurgery

Abstract

In the last ten years, the knowledge of the genetic basis of mitochondrial diseases has significantly advanced. However, the vast phenotypic variability linked to mitochondrial disorders and the peculiar characteristics of their genetics make mitochondrial disorders a complex group of disorders. Although specific genetic alterations have been associated with some syndromic presentations, the genotype–phenotype relationship in mitochondrial disorders is complex (a single mutation can cause several clinical syndromes, while different genetic alterations can cause similar phenotypes). This review will revisit the most common syndromic pictures of mitochondrial disorders, from a clinical rather than a molecular perspective. We believe that the new phenotype definitions implemented by recent large multicenter studies, and revised here, may contribute to a more homogeneous patient categorization, which will be useful in future studies on natural history and clinical trials.

Published

2021

48. Progressive external ophthalmoplegia.

Author

Hirano M and Pitceathly RDS

Subjects

Humans, DNA, Mitochondrial genetics, Muscle, Skeletal pathology, Syndrome, Ophthalmoplegia, Chronic Progressive External complications, Ophthalmoplegia, Chronic Progressive External genetics, Ophthalmoplegia, Chronic Progressive External pathology, Ophthalmoplegia genetics, Ophthalmoplegia pathology

Abstract

Progressive external ophthalmoplegia (PEO), characterized by ptosis and impaired eye movements, is a clinical syndrome with an expanding number of etiologically distinct subtypes. Advances in molecular genetics have revealed numerous pathogenic causes of PEO, originally heralded in 1988 by the detection of single large-scale deletions of mitochondrial DNA (mtDNA) in skeletal muscle of people with PEO and Kearns-Sayre syndrome. Since then, multiple point variants of mtDNA and nuclear genes have been identified to cause mitochondrial PEO and PEO-plus syndromes, including mitochondrial neurogastrointestinal encephalomyopathy (MNGIE) and sensory ataxic neuropathy dysarthria ophthalmoplegia (SANDO). Intriguingly, many of those nuclear DNA pathogenic variants impair maintenance of the mitochondrial genome causing downstream mtDNA multiple deletions and depletion. In addition, numerous genetic causes of nonmitochondrial PEO have been identified., Competing Interests: Declaration of interests MH is a paid consultant to Modis Therapeutics, a wholly owned subsidiary of Zogenix/UCB, and Entrada Therapeutics. These relationships are de minimus for Columbia University Medical Center. Columbia University has patents for deoxynucleotide and deoxynucleoside therapies for mitochondrial DNA depletion syndrome, which is licensed by Modis Therapeutics; this relationship is monitored by an unconflicted external academic researcher. Received honoraria from the AAN and PlatformQ for speaking activities and research support from Modis Therapeutics and Entrada Therapeutics., (Copyright © 2023 Elsevier B.V. All rights reserved.)

Published

2023

49. Avenços en la teràpia gènica per al MNGIE amb vectors adenoassociats: validació en un model millorat de la malaltia i optimització de seqüència del gen terapèutic

Author

Vila Julià, Ferran, Martí Seves, Ramon, Torres Torronteras, Javier, Messeguer Navarro, Anna, and Martí, Ramon A.

Subjects

Teràpia gènica, Gene therapy, MNGIE, Vectors adenoassociats, Adenoassociated virus vector, Vectores adenoasociados, Ciències de la Salut, Terapia génica

Abstract

El MNGIE és una malaltia mitocondrial d’herència autosòmica recessiva causada per mutacions en el gen TYMP, que codifica l’enzim timidina fosforilasa (TP). La TP catalitza la degradació de timidina (dThd) i desoxiuridina (dUrd), i la seva absència en pacients causa l’acumulació sistèmica d’aquests metabòlits, tòxica per la funció mitocondrial. A dia d’avui les úniques teràpies efectives són el transplantament de cèl·lules mare hematopoètiques i el transplantament de fetge. No obstant, els transplantaments estan limitats per la necessitat d’un donant compatible i tenen una taxa de mortalitat i morbiditat associada especialment elevada en pacients de MNGIE. Per a superar aquests inconvenients, fa temps vam proposar la teràpia gènica mitjançant vectors adenoassociats (rAAV) dirigits al fetge com a alternativa terapèutica, i vam demostrar la seva viabilitat en el model animal de MNGIE, el ratolí doble knockout (dKO) Tymp-/-Upp1-/-. Però aquest model només presenta fenotip bioquímic, de manera que només vam poder demostrar la correcció d’aquest fenotip. Al 2014 es va descriure que augmentant el desequilibri metabòlic mitjançant l’administració oral de dThd i dUrd al model dKO durant tota la seva vida provocava l’aparició d’alguns trets que reproduïen la simptomatologia clínica dels pacients. En aquesta tesi hem estudiat l’ús de la teràpia gènica en aquest model millorat, mitjançant el tractament amb tres rAAVs que expressaven la seqüència codificant de TYMP sota el control de 3 promotors hepàtics a diferents dosis. El tractament amb rAAV va incrementar l’activitat TP en fetge i va disminuir la concentració sistèmica de nucleòsids dels ratolins dKO, que sense tractament eren 30 vegades superiors als valors normals. A nivell fenotípic, en la majoria dels ratolins, el tractament també va prevenir l’increment del volum dels ventricles cerebrals i el deteriorament motor observats en els ratolins no tractats. Quan vam comparar els tres vectors utilitzats, el rAAV amb el promotor de l’alfa-1-antitripsina (AAT) va ser el més eficaç. Aquests resultats confirmen que la teràpia gènica mediada per rAAV dirigida al fetge restaura l’homeòstasi bioquímica i demostren la prevenció de l’aparició del fenotip clínic del model animal millorat de MNGIE. Un altre aspecte important per a la translació de la teràpia a la pràctica clínica és optimitzar el vector per tal de reduir-ne la dosi efectiva. En aquest sentit, hem testat dues aproximacions: la modificació de la seqüència codificant (ADNc) del gen segons la freqüència d’ús de codó per a incrementar la seva expressió, i l’eliminació dels dinucleòtids CpG de l’ADNc del gen per a reduir la immunogenicitat del vector. Vam dissenyar quatre seqüències optimitzades de l’ADNc de TYMP amb 4 algoritmes diferents. Vam generar vectors lentivirals per transduir 4 línies cel·lulars humanes i determinar l’eficiència d’expressió de cada seqüència comparada amb la seqüència salvatge, tenint en compte el grau d’activitat TP, el número de còpies del vector i els nivells relatius d’ARNm. De tots els experiments, només una seqüència optimitzada va millorar el grau d’expressió de TYMP respecte el de la seqüència salvatge en la línia cel·lular hepàtica Huh7. Pel que fa a la reducció de la immunogenicitat del vector, vam eliminar els dinucleòtids CpG de les seqüències dissenyades i vam analitzar el grau d’expressió de TYMP. Només la seqüència salvatge sense dinucleòtids CpG es va acostar a l’expressió de la seqüència natural. Tot i que s’hi observa una reducció d’expressió aproximada del 20%, es compensa per l’avantatge que aporta en termes de reducció de la resposta immunològica de cara a l’ús clínic del vector. En conclusió recomanem aquesta versió sota la regulació del promotor AAT per a ús eventual en la pràctica clínica. El MNGIE (Mitochondrial NeuroGastroIntestinal Encephalomyopathy) es una enfermedad mitocondrial de herencia autosómica recesiva causada por mutaciones en el gen TYMP, que codifica la enzima timidina fosforilasa (TP). La TP cataliza la degradación de timidina (dThd) y desoxiuridina (dUrd), y su ausencia en pacientes causa la acumulación sistémica de estos metabolitos, tóxica para la función mitocondrial. Hoy en día, las únicas terapias efectives son el trasplante de células madre hematopoyéticas y el trasplante de hígado. No obstante, los trasplantes están limitados por la necesidad de un donante compatible y tienen una tasa de mortalidad y morbididad asociada especialmente elevada en pacientes de MNGIE. Para superar estos inconvenientes, hace tiempo propusimos la terapia génica mediante vectores adenoasociados (rAAV) dirigidos al hígado como alternativa terapéutica, y demostramos su viabilidad en el modelo animal de MNGIE, el ratón doble knockout (dKO) Tymp-/-Upp1-/-. Pero este modelo solo presenta fenotipo bioquímico, de forma que solo pudimos demostrar la corrección de este fenotipo. En 2014 se describió que aumentando el desequilibrio metabólico mediante la administración oral de dThd y dUrd al modelo dKO durante toda su vida provocaba la aparición de algunos rasgos que reproducían la sintomatología clínica de los pacientes. En esta tesis hemos estudiado el uso de la terapia génica en este modelo mejorado, mediante el tratamiento con tres rAAVs que expresan la secuencia codificante de TYMP bajo el control de tres promotores hepáticos a distintas dosis. El tratamiento con rAAV incrementó la actividad TP hepática y disminuyo la concentración sistémica de nucleósidos de los ratones dKO, (sin tratamiento eren 30 veces superiores a los valores normales). A nivel fenotípico, en la mayoría de los ratones, el tratamiento también previno el aumento del volumen de los ventrículos cerebrales y el deterioro motor observados en los ratones no tratados. Cuando comparamos los tres vectores utilitzados, el rAAV con el promotor de la alfa-1-antitripsina (AAT) fue el más eficaz. Estos resultados confirman que la terapia génica por rAAV dirigida al hígado restaura la homeóstasis bioquímica y demuestran la prevención de la aparición del fenotipo clínico del modelo animal mejorado de MNGIE. Otro aspecto importante para la translación de la terapia a la práctica clínica es optimizar el vector para reducir la dosis efectiva. En este sentido, hemos testado dos aproximaciones: la modificación de la secuencia codificante (ADNc) del gen según la frecuencia de uso de codón para aumentar su expresión, y la eliminación de los dinucleótidos CpG del ADNc del gen para reducir la immunogenicidad del vector. Diseñamos cuatro secuencies optimizadas del ADNc de TYMP utilitzando 4 algoritmos diferentes. Generamos vectores lentivirales para transducir 4 líneas celulares humanas y determinar la eficiencia de expresión de cada secuencia comparada con la secuencia natural, teniendo en cuenta el grado de actividad TP, el número de copias del vector y los niveles relativos de ARNm. De todos los experimentos, solo una secuencia optimizada mejoró el grado de expresión de TYMP comparado con el de la secuencia natural, en la línea celular hepática Huh7. En cuanto a la reducción de la immunogenicidad del vector, eliminamos los dinucleótidos CpG de las secuencias diseñadas y analizamos el nivel de expresión de TYMP. Solo la secuencia natural sin dinucleótidos CpG se acercó a la expresión de la secuencia natural. Aunque se observa una reducción de expresión aproximada del 20%, se compensa con la ventaja que aporta en términos de reducción de la respuesta inmunológica de cara al uso clínico del vector. En conclusión, entre las opciones testadas, recomendamos el rAAV que contiene el ADNc natural de TYMP sin dinucleótidos CpG bajo el control del promotor AAT para un uso eventual en la práctica clínica. MNGIE (Mitochondrial NeuroGastroIntestinal Encephalomyopathy) is an autosomal recessive disease caused by mutations in TYMP, which encodes for the enzyme thymidine phosphorylase (TP). TP catalyses the first step of the catabolism of the nucleosides thymidine (dThd) and deoxyuridine (dUrd). The lack of TP activity causes systemic nucleoside accumulation which is toxic for mitochondrial function. Nowadays, the only available therapies for MNGIE are allogeneic hematopoetic stem cell transplantation or liver transplantation. However, these treatments are limited by the need of a compatible donor and are associated to high mortality and morbidity rates in MNGIE patients. To overcome these limitations, our laboratory proposed adenoassociated virus (rAAV) mediated gene therapy targeted to the liver for MNGIE and demonstrated its feasibility in the Tymp-/- Upp1-/- (dKO) mouse model of the disease. However, dKO mice show biochemical phenotype only, therefore we could only demonstrate the efficacy of our approach at the biochemical level. In 2014 it was reported that increasing the biochemical imbalances of the dKO model by chronic oral administration of dThd and dUrd to dKO mice over their entire life induced some features that recapitulate part of the clinical manifestations observed in patients. In this thesis we have studied the effect of gene therapy in this enhanced model, by treating the animals with three rAAVs expressing the human TYMP coding sequence under the control of three different liver-specific promoters. rAAV treatment increased liver TP activity and limited the systemic nucleoside concentration present in the dKO enhanced model, which was 30-fold higher as compared with non-exposed wild-type mice. AAV-treatment also prevented, in most animals, the enlarged brain ventricles and the motor impairment observed in the exposed dKO mice. When we compared the three promoters tested, the rAAV containing the AAT promoter showed the best efficacy. These results confirm that AAV-mediated gene therapy restores the biochemical homeostasis and demonstrate that this treatment prevents the clinical phenotype developed by the enhanced murine model of MNGIE. Another key point for the clinical translation of gene therapy is the optimization of the therapeutic gene expression to reduce the vector dose. For this reason, we tested two approaches: modification of the coding sequence of TYMP based on the codon use frequency to increase the expression of the gene, and CpG dinucleotide removal from the coding sequence to reduce immunogenicity of the vector. We designed four different codon-optimized sequences of the TYMP coding sequence, using four different algorithms. We cloned each optimized sequence in a lentiviral vector and transduced 4 different human cell lines. We analysed the degree of expression achieved with each sequence, as compared with the non-optimized wild-type TYMP sequence through evaluation of TP activity, vector copy number, and mRNA levels in the cell lines. Among all the sequences studied, only one optimized sequence resulted in higher TP activity when expressed per vector copy number in the hepatic cell line Huh7. To reduce the immunogenicity of the vector we removed the CpG dinucleotides from the wild-type coding TYMP sequence and two codon-optimized TYMP sequences. The wild-type sequence without CpG was the only one showing expression levels similar to those of the wild-type sequence. Even though the CpG free sequence shows a reduced expression of about 20% of that observed in the wild-type sequence, it is compensated by the advantages associated to the absence of CpG sites in terms of reduction of the immunological response when considering the vector for clinical use. In conclusion, among the different options tested, we recommend the rAAV vector containing the wild-type coding TYMP CpG-free sequence under the control of the AAT promoter for its use in the clinical practice. Universitat Autònoma de Barcelona. Programa de Doctorat en Bioquímica, Biologia Molecular i Biomedicina

Published

2021

50. Biallelic variants in LIG3 cause a novel mitochondrial neurogastrointestinal encephalomyopathy

Author

Pierluigi Martelli, Tom J. de Koning, Takema Kato, Irene Liparulo, Mariko Taniguchi-Ikeda, Tatsushi Toda, Hisayoshi Nakamura, Wilfred F. A. den Dunnen, Giovanna Cenacchi, Sanjiban Chakrabarty, Yu Sheng Yeh, Sushil Kumar Mishra, Rita Casadio, Akira Ohtake, Ichizo Nishino, Roberto De Giorgio, Paolo Picco, Pasquale Striano, Chiara Fiorillo, Isabella Ceccherini, Tsuyoshi Goto, Elisa Boschetti, Makiko Tsutsumi, Eleonora Aronica, Georgios Kellaris, Mariel Alders, Gabor E. Linthorst, Jantima Tanboon, Angela Rita Sementa, Floor A. M. Duijkers, Yu Ichi Goto, Hiroki Kurahashi, Masakazu Mimaki, Gerard Dijkstra, Dik C. van Gent, Mariasavina Severino, Yoshinobu Oyazato, Christian Bergamini, Ikuya Nonaka, Yoshiki Yamaguchi, Ivana Matera, Giuseppe Raiola, Karin Van Spaendonck, Nicholas Katsanis, Luca Masin, Shumpei Uchino, Kenjiro Kosaki, Sara Signa, Anja Raams, Federica Isidori, Elena Bonora, Serena Arrigo, Kandai Nozu, Marc Engelen, Farid Ullah, Ichiro Morioka, Chiara Diquigiovanni, Marco Seri, Valerio Carelli, Francesca Bianco, Mariapia Giuditta Cratere, Nicola Rizzardi, Romana Fato, Alessandra Maresca, Alyson W. MacInnes, Valentina Papa, Kazumoto Iijima, Movement Disorder (MD), Molecular Neuroscience and Ageing Research (MOLAR), Groningen Institute for Organ Transplantation (GIOT), Translational Immunology Groningen (TRIGR), Groningen Institute for Gastro Intestinal Genetics and Immunology (3GI), Human Genetics, ACS - Pulmonary hypertension & thrombosis, ARD - Amsterdam Reproduction and Development, Neurology, Paediatric Neurology, ANS - Cellular & Molecular Mechanisms, AGEM - Amsterdam Gastroenterology Endocrinology Metabolism, Endocrinology, Pathology, Bonora, Elena, Chakrabarty, Sanjiban, Kellaris, Georgio, Tsutsumi, Makiko, Bianco, Francesca, Bergamini, Christian, Ullah, Farid, Isidori, Federica, Liparulo, Irene, Diquigiovanni, Chiara, Masin, Luca, Rizzardi, Nicola, Cratere, Mariapia Giuditta, Boschetti, Elisa, Papa, Valentina, Maresca, Alessandra, Cenacchi, Giovanna, Casadio, Rita, Martelli, Pierluigi, Matera, Ivana, Ceccherini, Isabella, Fato, Romana, Raiola, Giuseppe, Arrigo, Serena, Signa, Sara, Sementa, Angela Rita, Severino, Mariasavina, Striano, Pasquale, Fiorillo, Chiara, Goto, Tsuyoshi, Uchino, Shumpei, Oyazato, Yoshinobu, Nakamura, Hisayoshi, Mishra, Sushil K, Yeh, Yu-Sheng, Kato, Takema, Nozu, Kandai, Tanboon, Jantima, Morioka, Ichiro, Nishino, Ichizo, Toda, Tatsushi, Goto, Yu-Ichi, Ohtake, Akira, Kosaki, Kenjiro, Yamaguchi, Yoshiki, Nonaka, Ikuya, Iijima, Kazumoto, Mimaki, Masakazu, Kurahashi, Hiroki, Raams, Anja, MacInnes, Alyson, Alders, Mariel, Engelen, Marc, Linthorst, Gabor, de Koning, Tom, den Dunnen, Wilfred, Dijkstra, Gerard, van Spaendonck, Karin, van Gent, Dik C, Aronica, Eleonora M, Picco, Paolo, Carelli, Valerio, Seri, Marco, Katsanis, Nichola, Duijkers, Floor A M, Taniguchi-Ikeda, Mariko, De Giorgio, Roberto, and Molecular Genetics

Subjects

Male, 0301 basic medicine, Mitochondrial DNA, Gastrointestinal Disease, Mitochondrial disease, LIG3, mtDNA replication, mtDNA repair, MNGIE, CIPO, LIG3, Biology, Mitochondrion, CIPO, MNGIE, mtDNA repair, mtDNA replication, LS3_11, Mitochondrial Encephalomyopathie, NO, DNA Ligase ATP, 03 medical and health sciences, 0302 clinical medicine, SDG 3 - Good Health and Well-being, LS5_1, LS4_1, medicine, LS2_6, Ligase activity, LS5_2, Poly-ADP-Ribose Binding Protein, Zebrafish, Exome sequencing, Mitochondrial Encephalomyopathies, Animal, medicine.disease, Molecular biology, Pedigree, 030104 developmental biology, Mitochondrial DNA repair, 030220 oncology & carcinogenesis, Mutation, Female, Neurology (clinical), Gastrointestinal Motility, Human

Abstract

Abnormal gut motility is a feature of several mitochondrial encephalomyopathies, and mutations in genes such as TYMP and POLG, have been linked to these rare diseases. The human genome encodes three DNA ligases, of which only one, ligase III (LIG3), has a mitochondrial splice variant and is crucial for mitochondrial health. We investigated the effect of reduced LIG3 activity and resulting mitochondrial dysfunction in seven patients from three independent families, who showed the common occurrence of gut dysmotility and neurological manifestations reminiscent of mitochondrial neurogastrointestinal encephalomyopathy. DNA from these patients was subjected to whole exome sequencing. In all patients, compound heterozygous variants in a new disease gene, LIG3, were identified. All variants were predicted to have a damaging effect on the protein. The LIG3 gene encodes the only mitochondrial DNA (mtDNA) ligase and therefore plays a pivotal role in mtDNA repair and replication. In vitro assays in patient-derived cells showed a decrease in LIG3 protein levels and ligase activity. We demonstrated that the LIG3 gene defects affect mtDNA maintenance, leading to mtDNA depletion without the accumulation of multiple deletions as observed in other mitochondrial disorders. This mitochondrial dysfunction is likely to cause the phenotypes observed in these patients. The most prominent and consistent clinical signs were severe gut dysmotility and neurological abnormalities, including leukoencephalopathy, epilepsy, migraine, stroke-like episodes, and neurogenic bladder. A decrease in the number of myenteric neurons, and increased fibrosis and elastin levels were the most prominent changes in the gut. Cytochrome c oxidase (COX) deficient fibres in skeletal muscle were also observed. Disruption of lig3 in zebrafish reproduced the brain alterations and impaired gut transit in vivo. In conclusion, we identified variants in the LIG3 gene that result in a mitochondrial disease characterized by predominant gut dysmotility, encephalopathy, and neuromuscular abnormalities. Bonora et al. identify a new mitochondrial recessive disorder caused by biallelic variants in the LIG3 gene encoding DNA ligase III, which is responsible for mitochondrial DNA repair. Clinical signs include gut dysmotility and neurological features such as leucoencephalopathy, epilepsy and stroke-like episodes.

Published

2021