208 results on '"Un Kyung Kim"'
Search Results
2. Mitochondrial redox system: A key target of antioxidant therapy to prevent acquired sensorineural hearing loss
- Author
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Jeong-In Baek, Ye-Ri Kim, Kyu-Yup Lee, and Un-Kyung Kim
- Subjects
acquired hearing loss ,noise ,ototoxic drugs ,ROS ,mitochondria ,drug development ,Therapeutics. Pharmacology ,RM1-950 - Abstract
Noise (noise-induced hearing loss), and ototoxic drugs (drug-induced ototoxicity), and aging (age-related hearing loss) are the major environmental factors that lead to acquired sensorineural hearing loss. So far, there have been numerous efforts to develop protective or therapeutic agents for acquired hearing loss by investigating the pathological mechanisms of each types of hearing loss, especially in cochlear hair cells and auditory nerves. Although there is still a lack of information on the underlying mechanisms of redox homeostasis and molecular redox networks in hair cells, an imbalance in mitochondrial reactive oxygen species (ROS) levels that enhance oxidative stress has been suggested as a key pathological factor eventually causing acquired sensorineural hearing loss. Thus, various types of antioxidants have been investigated for their abilities to support auditory cells in maintenance of the hearing function against ototoxic stimuli. In this review, we will discuss the scientific possibility of developing drugs that target particular key elements of the mitochondrial redox network in prevention or treatment of noise- and ototoxic drug-induced hearing loss.
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- 2023
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3. An autosomal dominant ERLIN2 mutation leads to a pure HSP phenotype distinct from the autosomal recessive ERLIN2 mutations (SPG18)
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Jin-Mo Park, Byeonghyeon Lee, Jong-Heun Kim, Seong-Yong Park, Jinhoon Yu, Un-Kyung Kim, and Jin-Sung Park
- Subjects
Medicine ,Science - Abstract
Abstract Hereditary spastic paraplegia (HSP) is a heterogeneous inherited disorder that manifests with lower extremity weakness and spasticity. HSP can be inherited by autosomal dominant, autosomal recessive, and X-linked inheritance patterns. Recent studies have shown that, although rare, mutations in a single gene can lead to multiple patterns of inheritance of HSP. We enrolled the HSP family showing autosomal dominant inheritance and performed genetic study to find the cause of phenotype in this family. We recruited five members of a Korean family as study participants. Four of the five family members had pure HSP. Part of the family members underwent whole-exome sequencing (WES) to identify the causative mutation. As the result of WES and Sanger sequencing analysis, a novel missense mutation (c.452 C > T, p.Ala151Val) of ERLIN2 gene was identified as the cause of the autosomal dominant HSP in the family. Our study suggests that the ERLIN2 gene leads to both autosomal recessive and autosomal dominant patterns of inheritance in HSP. Moreover, autosomal dominant HSP caused by ERLIN2 appears to cause pure HSP in contrast to autosomal recessive ERLIN2 related complicated HSP (SPG18).
- Published
- 2020
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- View/download PDF
4. Berberine chloride protects cochlear hair cells from aminoglycoside-induced ototoxicity by reducing the accumulation of mitochondrial reactive oxygen species
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Ye-Ri Kim, Jeong-In Baek, Kyu-Yup Lee, and Un-Kyung Kim
- Subjects
Physiology (medical) ,Biochemistry - Published
- 2023
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5. Targeted Gene Delivery into the Mammalian Inner Ear Using Synthetic Serotypes of Adeno-Associated Virus Vectors
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Min-A Kim, Nari Ryu, Hye-Min Kim, Ye-Ri Kim, Byeonghyeon Lee, Tae-Jun Kwon, Jinwoong Bok, and Un-Kyung Kim
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Genetics ,QH426-470 ,Cytology ,QH573-671 - Abstract
Targeting specific cell types in the mammalian inner ear is important for treating genetic hearing loss due to the different cell type-specific functions. Adeno-associated virus (AAV) is an efficient in vivo gene transfer vector, and it has demonstrated promise for treating genetic hearing loss. Although more than 100 AAV serotypes have been identified, few studies have investigated whether AAV can be distributed to specific inner ear cell types. Here we screened three EGFP-AAV reporter constructs (serotypes DJ, DJ8, and PHP.B) in the neonatal mammalian inner ear by injection via the round window membrane to determine the cellular specificity of the AAV vectors. Sensory hair cells, supporting cells, cells in Reissner’s membrane, interdental cells, and root cells were successfully transduced. Hair cells in the cochlear sensory epithelial region were the most frequently transduced cell type by all tested AAV serotypes. The recombinant DJ serotype most effectively transduced a range of cell types at a high rate. Our findings provide a basis for improving treatment of hereditary hearing loss using targeted AAV-mediated gene therapy. Keywords: gene therapy, genetic hearing loss, inner ear, adeno-associated virus, serotype
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- 2019
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6. Therapeutic potential of the mitochondria-targeted antioxidant MitoQ in mitochondrial-ROS induced sensorineural hearing loss caused by Idh2 deficiency
- Author
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Ye-Ri Kim, Jeong-In Baek, Sung Hwan Kim, Min-A Kim, Byeonghyeon Lee, Nari Ryu, Kyung-Hee Kim, Deok-Gyun Choi, Hye-Min Kim, Michael P. Murphy, Greg Macpherson, Yeon-Sik Choo, Jinwoong Bok, Kyu-Yup Lee, Jeen-Woo Park, and Un-Kyung Kim
- Subjects
Medicine (General) ,R5-920 ,Biology (General) ,QH301-705.5 - Abstract
Mitochondrial NADP+-dependent isocitrate dehydrogenase 2 (IDH2) is a major NADPH-producing enzyme which is essential for maintaining the mitochondrial redox balance in cells. We sought to determine whether IDH2 deficiency induces mitochondrial dysfunction and modulates auditory function, and investigated the protective potential of an antioxidant agent against reactive oxygen species (ROS)-induced cochlear damage in Idh2 knockout (Idh2−/−) mice. Idh2 deficiency leads to damages to hair cells and spiral ganglion neurons (SGNs) in the cochlea and ultimately to apoptotic cell death and progressive sensorineural hearing loss in Idh2−/− mice. Loss of IDH2 activity led to decreased levels of NADPH and glutathione causing abnormal ROS accumulation and oxidative damage, which might trigger apoptosis signal in hair cells and SGNs in Idh2−/− mice. We performed ex vivo experiments to determine whether administration of mitochondria-targeted antioxidants might protect or induce recovery of cells from ROS-induced apoptosis in Idh2-deficient mouse cochlea. MitoQ almost completely neutralized the H2O2-induced ototoxicity, as the survival rate of Idh2−/− hair cells were restored to normal levels. In addition, the lack of IDH2 led to the accumulation of mitochondrial ROS and the depolarization of ΔΨm, resulting in hair cell loss. In the present study, we identified that IDH2 is indispensable for the functional maintenance and survival of hair cells and SGNs. Moreover, the hair cell degeneration caused by IDH2 deficiency can be prevented by MitoQ, which suggests that Idh2−/− mice could be a valuable animal model for evaluating the therapeutic effects of various antioxidant candidates to overcome ROS-induced hearing loss. Keywords: Idh2, NADP+, ROS, Hearing loss, Antioxidant, MitoQ
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- 2019
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7. Identification of novel missense mutation related with non-syndromic sensorineural deafness, DFNA11 in korean family by NGS
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Ye-Ri Kim, Hye-Min Kim, Byeonghyeon Lee, Jeong-In Baek, Kyu-Yup Lee, Hong-Joon Park, and Un-Kyung Kim
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Genetics ,Molecular Biology ,Biochemistry - Published
- 2023
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8. Fursultiamine Prevents Drug-Induced Ototoxicity by Reducing Accumulation of Reactive Oxygen Species in Mouse Cochlea
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Ye-Ri Kim, Tae-Jun Kwon, Un-Kyung Kim, In-Kyu Lee, Kyu-Yup Lee, and Jeong-In Baek
- Subjects
cisplatin ,kanamycin ,ototoxicity ,reactive oxygen species ,fursultiamine ,Therapeutics. Pharmacology ,RM1-950 - Abstract
Drug-induced hearing loss is a major type of acquired sensorineural hearing loss. Cisplatin and aminoglycoside antibiotics have been known to cause ototoxicity, and excessive accumulation of intracellular reactive oxygen species (ROS) are suggested as the common major pathology of cisplatin- and aminoglycoside antibiotics-induced ototoxicity. Fursultiamine, also called thiamine tetrahydrofurfuryl disulfide, is a thiamine disulfide derivative that may have antioxidant effects. To evaluate whether fursultiamine can prevent cisplatin- and kanamycin-induced ototoxicity, we investigated their preventive potential using mouse cochlear explant culture system. Immunofluorescence staining of mouse cochlear hair cells showed that fursultiamine pretreatment reduced cisplatin- and kanamycin-induced damage to both inner and outer hair cells. Fursultiamine attenuated mitochondrial ROS accumulation as evidenced by MitoSOX Red staining and restored mitochondrial membrane potential in a JC-1 assay. In addition, fursultiamine pretreatment reduced active caspase-3 and TUNEL signals after cisplatin or kanamycin treatment, indicating that fursultiamine decreased apoptotic hair cell death. This study is the first to show a protective effect of fursultiamine against cisplatin- and aminoglycoside antibiotics-induced ototoxicity. Our results suggest that fursultiamine could act as an antioxidant and anti-apoptotic agent against mitochondrial oxidative stress.in cochlear hair cells.
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- 2021
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9. A Novel Frameshift Mutation of in a Korean Family With Nonsyndromic Hearing Loss and Enlarged Vestibular Aqueduct
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Borum Sagong, Jeong-In Baek, Kyu-Yup Lee, and Un-Kyung Kim
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DFNB4 ,Hearing Loss ,Enlarged Vestibular Aqueduct ,Novel Mutation ,Medicine ,Otorhinolaryngology ,RF1-547 - Abstract
Objectives We aimed to identify the causative mutation for siblings in a Korean family with nonsyndromic hearing loss (HL) and enlarged vestibular aqueduct (EVA). The siblings were a 19-year-old female with bilateral profound HL and an 11-year-old male with bilateral moderately severe HL. Methods We extracted genomic DNA from blood samples of the siblings with HL, their parents, and 100 controls. We performed mutation analysis for SLC26A4 using direct sequencing. Results The two siblings were compound heterozygotes with the novel mutation p.I713LfsX8 and the previously described mutation p.H723R. Their parents had heterozygous mono-allelic mutations. Father had p.I713LfsX8 mutation as heterozygous, and mother had p.H723R mutation as heterozygous. However, novel mutation p.I713LfsX8 was not detected in 100 unrelated controls. Conclusion Both mutations identified in this study were located in the sulfate transporter and anti-sigma factor antagonist domain, the core region for membrane targeting of SulP/SLC26 anion transporters, which strongly suggests that failure in membrane trafficking by SLC26A4 is a direct cause of HL in this family. Our study could therefore provide a foundation for further investigations elucidating the SLC26A4-related mechanisms of HL.
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- 2017
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10. Phenotype of the Aging-Dependent Spontaneous Onset of Hearing Loss in DBA/2 Mice
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Min-Soo Seo, Byeonghyeon Lee, Kyung-Ku Kang, Soo-Eun Sung, Joo-Hee Choi, Si-Joon Lee, Young-In Kim, Young-Suk Jung, Un-Kyung Kim, and Kil Soo Kim
- Subjects
hearing loss ,laboratory animals ,aging ,DBA/2 mice ,Veterinary medicine ,SF600-1100 - Abstract
DBA/2 mice are a well-known animal model for hearing loss developed due to intrinsic properties of these animals. However, results on the phenotype of hearing loss in DBA/2 mice have been mainly reported at an early stage in mice aged ≤7 weeks. Instead, the present study evaluated the hearing ability at 5, 13, and 34 weeks of age using DBA/2korl mice. Auditory brainstem response test was performed at 8–32 KHz at 5, 13, and 34 weeks of age, and hearing loss was confirmed to be induced in a time-dependent manner. In addition, histopathological evaluation at the same age confirmed the morphological damage of the cochlea. The findings presented herein are the results of the long-term observation of the phenotype of hearing loss in DBA/2 mice and can be useful in studies related to aging-dependent hearing loss.
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- 2021
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11. Role of the TAS2R38 Bitter Taste Receptor Gene Single Nucleotide Polymorphism in Patients With Taste Disorders
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Sang-Yen Geum, Jin-Woo Park, Seung-Heon Shin, Un-Kyung Kim, Byung-Jun Kang, and Mi-Kyung Ye
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Genetics ,TAS2R38 ,Otorhinolaryngology ,Taste disorder ,business.industry ,Medicine ,Surgery ,Single-nucleotide polymorphism ,In patient ,business ,Receptor ,Bitter taste ,Gene - Abstract
Background and Objectives Several studies have shown that three single nucleotide polymorphisms (SNPs) in the TAS2R38 gene demonstrate a strong association with the ability to sense the bitter taste of phenylthiocarbamide (PTC) in. We have previously reported about TAS2R38 genotypes in normal volunteers. The aim of this study was to investigate the role TAS2R38 gene plays in taste disorder by examining SNPs in the TAS2R38 gene in taste disorder patients.Subjects and Method Ninety-four patients with taste dysfunction from multiple etiologies were enrolled. The genotypes were defined by identifying SNPs on the TAS2R38 gene. The proportion of different TAS2R38 genotypes in the group was compared with that in the normal volunteers of our previous study. The whole mouth taste threshold tests were performed and the thresholds were compared among the three different genotypic groups.Results The proportion of each diplotype in taste disorder patients were as follows: PAV/ PAV 36.2% (34/94), PAV/AVI 34.0% (32/94), and AVI/AVI 29.8% (28/94). The proportion of AVI/AVI type was higher in the group than in the normal volunteers (p=0.031). The detection and recognition thresholds of all four basic tastes were increased in the order of PAV/PAV, PAV/AVI, and AVI/AVI genotypes.Conclusion The proportion of AVI/AVI homozygous was significantly higher in taste disorder patients than in the normal volunteers. Our findings suggest that the genotypes of TAS2R38 may represent one of the risk factors responsible for the development of taste disorders.
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- 2021
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12. Protective effect of berberine chloride against cisplatin-induced ototoxicity
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Jeong-In Baek, Ye-Ri Kim, Jong-Heun Kim, Un-Kyung Kim, Kyu-Yup Lee, and Inkyu Lee
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Berberine ,Antineoplastic Agents ,Apoptosis ,Pharmacology ,Mitochondrion ,Biology ,Protective Agents ,medicine.disease_cause ,Biochemistry ,Mice ,chemistry.chemical_compound ,Chlorides ,Ototoxicity ,Hair Cells, Auditory ,In Situ Nick-End Labeling ,Genetics ,medicine ,Animals ,Inner mitochondrial membrane ,Organ of Corti ,Molecular Biology ,Cells, Cultured ,Membrane Potential, Mitochondrial ,Berberine chloride ,Caspase 3 ,ROS ,medicine.disease ,Cochlea ,medicine.anatomical_structure ,chemistry ,Berberine Chloride ,Cisplatin ,Antioxidant ,Reactive Oxygen Species ,Oxidative stress ,Research Article - Abstract
Background Cisplatin (CP) is an effective anticancer drug broadly used for various types of cancers, but it has shown ototoxicity that results from oxidative stress. Berberine has been reported for its anti-oxidative stress suggesting its therapeutic potential for many diseases such as colitis, diabetes, and vascular dementia. Objective Organ of Corti of postnatal day 3 mouse cochlear explants were used to compare hair cells after the treatment with cisplatin alone or with berberine chloride (BC) followed by CP. Methods We investigated the potential of the anti-oxidative effect of BC against the cisplatin-induced ototoxicity. We observed a reduced aberrant bundle of stereocilia in hair cells in CP with BC pre-treated group. Caspase-3 immunofluorescence and TUNEL assay supported the hypothesis that BC attenuates the apoptotic signals induced by CP. Reactive oxygen species level in the mitochondria were investigated by MitoSOX Red staining and the mitochondrial membrane potentials were compared by JC-1 assay. Results BC decreased ROS generation with preserved mitochondrial membrane potentials in mitochondria as well as reduced DNA fragmentation in hair cells. In summary, our data indicate that BC might act as antioxidant against CP by reducing the stress in mitochondria resulting in cell survival. Conclusion Our result suggests the therapeutic potential of BC for prevention of the detrimental effect of CP-induced ototoxicity.
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- 2021
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13. Follistatin regulates the specification of the apical cochlea responsible for low-frequency hearing in mammals
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Hei Yeun Koo, Min-A Kim, Hyehyun Min, Jae Yeon Hwang, Meenakshi Prajapati-DiNubila, Kwan Soo Kim, Martin M. Matzuk, Juw Won Park, Angelika Doetzlhofer, Un-Kyung Kim, and Jinwoong Bok
- Subjects
Mammals ,Mice ,Follistatin ,Multidisciplinary ,Hearing ,Animals ,Hedgehog Proteins ,Cochlea - Abstract
The cochlea’s ability to discriminate sound frequencies is facilitated by a special topography along its longitudinal axis known as tonotopy. Auditory hair cells located at the base of the cochlea respond to high-frequency sounds, whereas hair cells at the apex respond to lower frequencies. Gradual changes in morphological and physiological features along the length of the cochlea determine each region’s frequency selectivity, but it remains unclear how tonotopy is established during cochlear development. Recently, sonic hedgehog (SHH) was proposed to initiate the establishment of tonotopy by conferring regional identity to the primordial cochlea. Here, using mouse genetics, we provide in vivo evidence that regional identity in the embryonic cochlea acts as a framework upon which tonotopy-specific properties essential for frequency selectivity in the mature cochlea develop. We found that follistatin (FST) is required for the maintenance of apical cochlear identity, but dispensable for its initial induction. In a fate-mapping analysis, we found that FST promotes expansion of apical cochlear cells, contributing to the formation of the apical cochlear domain. SHH, in contrast, is required both for the induction and maintenance of apical identity. In the absence of FST or SHH, mice produce a short cochlea lacking its apical domain. This results in the loss of apex-specific anatomical and molecular properties and low-frequency-specific hearing loss.
- Published
- 2022
14. C-phycocyanin from Limnothrix Species KNUA002 Alleviates Cisplatin-Induced Ototoxicity by Blocking the Mitochondrial Apoptotic Pathway in Auditory Cells
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Ye-Ri Kim, Jeong-Mi Do, Kyung Hee Kim, Alexandra R. Stoica, Seung-Woo Jo, Un-Kyung Kim, and Ho-Sung Yoon
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ototoxicity ,cisplatin ,C-phycocyanin ,Limnothrix ,HEI-OC1 ,Biology (General) ,QH301-705.5 - Abstract
Ototoxicity, or adverse pharmacological effects on the inner ear or auditory nerve, is a common side effect of cisplatin, a platinum-based drug widely used in anticancer chemotherapy. Although the incidence of ototoxicity is high among patients that receive cisplatin therapy, there is currently no effective treatment for it. The generation of excessive reactive oxygen species (ROS) is considered to be the major cause of cisplatin-induced ototoxicity. C-phycocyanin (C-PC), a blue phycobiliprotein found in cyanobacteria and red algae, has antioxidant and anticancer activities in different experimental models in vitro and in vivo. Thus, we tested the ability of C-PC from Limnothrix sp. KNUA002 to protect auditory cells from cisplatin-induced ototoxicity in vitro. Pretreatment with C-PC from Limnothrix sp. KNUA002 inhibited apoptosis and protected mitochondrial function by preventing ROS accumulation in cisplatin-treated House Ear Institute-Organ of Corti 1 (HEI-OC1) cells, a mouse auditory cell line. Cisplatin increased the expression of Bax and reduced the expression of Bcl-2, which activate and inhibit, respectively, the mitochondrial apoptotic pathway in response to oxidative stress. Pretreatment with C-PC prior to cisplatin treatment caused the Bax and Bcl-2 levels to stay close to the levels in untreated control cells. Our results suggest that C-PC from Limnothrix sp. KNUA002 protects cells against cisplatin-induced cytotoxicity by inhibiting the mitochondrial apoptotic pathway.
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- 2019
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15. Identification of an in-frame homozygous KIF1A variant causing a mild SPG30 phenotype in a Korean family
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Byeonghyeon Lee, Ha Hyun Song, Ye-Ri Kim, Jong-Heun Kim, Seong Tae Cho, Jeong Ho Lee, Un-Kyung Kim, and Jin-Sung Park
- Subjects
Genetics ,General Medicine - Published
- 2023
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16. Disease-specific ACMG/AMP guidelines improve sequence variant interpretation for hearing loss
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Mayher J. Patel, Marina T. DiStefano, Andrea M. Oza, Madeline Y. Hughes, Emma H. Wilcox, Sarah E. Hemphill, Brandon J. Cushman, Andrew R. Grant, Rebecca K. Siegert, Jun Shen, Alex Chapin, Nicole J. Boczek, Lisa A. Schimmenti, Kiyomitsu Nara, Margaret Kenna, Hela Azaiez, Kevin T. Booth, Karen B. Avraham, Hannie Kremer, Andrew J. Griffith, Heidi L. Rehm, Sami S. Amr, Ahmad N. Abou Tayoun, Sonia Abdelhak, John Alexander, Zippora Brownstein, Rachel Burt, Byung Yoon Choi, Lilian Downie, Thomas Friedman, Anne Giersch, John Greinwald, Jeffrey Holt, Makoto Hosoya, Un-Kyung Kim, Ian Krantz, Suzanne Leal, Saber Masmoudi, Tatsuo Matsunaga, Matías Morín, Cynthia Morton, Hideki Mutai, Arti Pandya, Richard Smith, Mustafa Tekin, Shin-Ichi Usami, Guy Van Camp, Kazuki Yamazawa, Hui-Jun Yuan, Elizabeth Black-Zeigelbein, and Kejian Zhang
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Disease specific ,medicine.medical_specialty ,Hearing loss ,Molecular pathology ,business.industry ,Genome, Human ,Genetic Variation ,Computational biology ,Sensory disorders Donders Center for Medical Neuroscience [Radboudumc 12] ,Human genetics ,Article ,medicine ,Medical genetics ,Humans ,Genetic Testing ,medicine.symptom ,business ,Hearing Loss ,Uncertain significance ,Genetics (clinical) ,Likely pathogenic ,Sequence (medicine) - Abstract
Contains fulltext : 243959.pdf (Publisher’s version ) (Closed access) PURPOSE: The ClinGen Variant Curation Expert Panels (VCEPs) provide disease-specific rules for accurate variant interpretation. Using the hearing loss-specific American College of Medical Genetics and Genomics/Association for Molecular Pathology (ACMG/AMP) guidelines, the Hearing Loss VCEP (HL VCEP) illustrates the utility of expert specifications in variant interpretation. METHODS: A total of 157 variants across nine HL genes, previously submitted to ClinVar, were curated by the HL VCEP. The curation process involved collecting published and unpublished data for each variant by biocurators, followed by bimonthly meetings of an expert curation subgroup that reviewed all evidence and applied the HL-specific ACMG/AMP guidelines to reach a final classification. RESULTS: Before expert curation, 75% (117/157) of variants had single or multiple variants of uncertain significance (VUS) submissions (17/157) or had conflicting interpretations in ClinVar (100/157). After applying the HL-specific ACMG/AMP guidelines, 24% (4/17) of VUS and 69% (69/100) of discordant variants were resolved into benign (B), likely benign (LB), likely pathogenic (LP), or pathogenic (P). Overall, 70% (109/157) variants had unambiguous classifications (B, LB, LP, P). We quantify the contribution of the HL-specified ACMG/AMP codes to variant classification. CONCLUSION: Expert specification and application of the HL-specific ACMG/AMP guidelines effectively resolved discordant interpretations in ClinVar. This study highlights the utility of ClinGen VCEPs in supporting more consistent clinical variant interpretation.
- Published
- 2021
17. An autosomal dominant ERLIN2 mutation leads to a pure HSP phenotype distinct from the autosomal recessive ERLIN2 mutations (SPG18)
- Author
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Byeonghyeon Lee, Jong-Heun Kim, Jinhoon Yu, Un-Kyung Kim, Jin-Sung Park, Jin-Mo Park, and Seong-Yong Park
- Subjects
0301 basic medicine ,Male ,lcsh:Medicine ,030105 genetics & heredity ,medicine.disease_cause ,Inheritance Patterns ,Missense mutation ,Exome ,lcsh:Science ,Genes, Dominant ,Genetics ,Sanger sequencing ,Mutation ,Multidisciplinary ,Middle Aged ,Phenotype ,Magnetic Resonance Imaging ,Pedigree ,symbols ,Medicine ,Female ,Hereditary spastic paraplegia ,Science ,Mutation, Missense ,Single gene ,Genes, Recessive ,Biology ,Article ,03 medical and health sciences ,symbols.namesake ,Republic of Korea ,Exome Sequencing ,medicine ,Humans ,Motor neuron disease ,Gene ,Gait Disorders, Neurologic ,Aged ,Spastic Paraplegia, Hereditary ,lcsh:R ,Membrane Proteins ,Sequence Analysis, DNA ,medicine.disease ,030104 developmental biology ,lcsh:Q - Abstract
Hereditary spastic paraplegia (HSP) is a heterogeneous inherited disorder that manifests with lower extremity weakness and spasticity. HSP can be inherited by autosomal dominant, autosomal recessive, and X-linked inheritance patterns. Recent studies have shown that, although rare, mutations in a single gene can lead to multiple patterns of inheritance of HSP. We enrolled the HSP family showing autosomal dominant inheritance and performed genetic study to find the cause of phenotype in this family. We recruited five members of a Korean family as study participants. Four of the five family members had pure HSP. Part of the family members underwent whole-exome sequencing (WES) to identify the causative mutation. As the result of WES and Sanger sequencing analysis, a novel missense mutation (c.452 C > T, p.Ala151Val) of ERLIN2 gene was identified as the cause of the autosomal dominant HSP in the family. Our study suggests that the ERLIN2 gene leads to both autosomal recessive and autosomal dominant patterns of inheritance in HSP. Moreover, autosomal dominant HSP caused by ERLIN2 appears to cause pure HSP in contrast to autosomal recessive ERLIN2 related complicated HSP (SPG18).
- Published
- 2020
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18. Construction of a DNA Chip for Screening of Genetic Hearing Loss
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Soo-Young Choi, Young-Eun Kim, Dong-bin Ahn, Tae-Hoon Kim, Jae-Hyuk Choi, Hye-Ryung Lee, Sang-Joon Hwang, Un-Kyung Kim, and Sang-Heun Lee
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Hearing loss ,DNA chip ,Gene ,Medicine ,Otorhinolaryngology ,RF1-547 - Abstract
ObjectivesHearing loss is the most common sensory disorder in humans and genetic causes are estimated to cause more than 50% of all incidents of congenital hearing loss. To develop an efficient method for a genetic diagnosis of hearing loss, we have developed and validated a genetic hearing loss DNA chip that allows the simultaneous analysis of 7 different mutations in the GJB2, SLC26A4, and the mtDNA 12S rRNA genes in Koreans.MethodsA genotyping microarray, based on the allele-specific primer extension (ASPE) method, was used and preliminary validation was examined from the five patients and five controls that were already known their genotypes by DNA sequencing analysis.ResultsThe cutoff Genotyping index (GI) of genotyping for each mutation was set up and validated to discriminate among the genotypes. The result of the DNA chip assay was identical to those of previous results.ConclusionWe successfully designed the genetic hearing loss DNA chip for the first time in Korea and it would be useful for a clinical genetic diagnosis of hearing loss. Further consideration will be needed in order to examine the accuracy of this DNA chip with much larger patient sample numbers.
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- 2009
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19. Evaluation of the contribution of the EYA4 and GRHL2 genes in Korean patients with autosomal dominant non-syndromic hearing loss.
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Ye-Ri Kim, Min-A Kim, Borum Sagong, Seung-Hyun Bae, Hyo-Jeong Lee, Hyung-Jong Kim, Jae Young Choi, Kyu-Yup Lee, and Un-Kyung Kim
- Subjects
Medicine ,Science - Abstract
EYA4 and GRHL2 encode transcription factors that play an important role in regulating many developmental stages. Since EYA4 and GRHL2 were identified as the transcription factors for the DFNA10 and DFNA28, 8 EYA4 mutations and 2 GRHL2 mutations have been reported worldwide. However, these genes have been reported in few studies of the Korean population. In this study, we performed a genetic analysis of EYA4 and GRHL2 in 87 unrelated Korean patients with autosomal dominant non-syndromic hearing loss (NSHL). A total of 4 genetic variants in the EYA4 gene were identified, including the 2 nonsense mutations p.S288X and p.Q393X. The novel mutation p.Q393X (c.1177C>T) resulted in a change in the codon at amino acid position 393 from a glutamine to a stop codon. The p.Q393X allele was predicted to encode a truncated protein lacking the entire C-terminal Eya homolog region (Eya HR), which is essential for the interaction with the transcription factor SIX3. The p.S288X (c.863C>A) mutation was found in a Korean family from a previous study. We analyzed p.S288X-linked microsatellite markers and determined that p.S288X might be a founder mutation and a hotspot mutation in Koreans. In GRHL2, a total of 4 genetic variants were identified, but none were associated with hearing loss in Korean patients. This suggests that GRHL2 may not be a main causal gene for autosomal dominant NSHL in Korean patients. In conclusion, our data provide fundamental information to predict the genotypes of Korean patients diagnosed with autosomal dominant NSHL.
- Published
- 2015
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20. Follistatin regulates the specification of the apical cochlea responsible for low-frequency hearing in mammals.
- Author
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Hei Yeun Koo, Min-A Kim, Hyehyun Min, Jae Yeon Hwang, Prajapati-DiNubila, Meenakshi, Kwan Soo Kim, Matzuk, Martin M., Juw Won Park, Doetzlhofer, Angelika, Un-Kyung Kim, and Jinwoong Bok
- Subjects
COCHLEA ,FOLLISTATIN ,HAIR cells ,MICE genetics ,AUDIO frequency - Abstract
The cochlea's ability to discriminate sound frequencies is facilitated by a special topography along its longitudinal axis known as tonotopy. Auditory hair cells located at the base of the cochlea respond to high-frequency sounds, whereas hair cells at the apex respond to lower frequencies. Gradual changes in morphological and physiological features along the length of the cochlea determine each region's frequency selectivity, but it remains unclear how tonotopy is established during cochlear development. Recently, sonic hedgehog (SHH) was proposed to initiate the establishment of tonotopy by conferring regional identity to the primordial cochlea. Here, using mouse genetics, we provide in vivo evidence that regional identity in the embryonic cochlea acts as a framework upon which tonotopy-specific properties essential for frequency selectivity in the mature cochlea develop. We found that follistatin (FST) is required for the maintenance of apical cochlear identity, but dispensable for its initial induction. In a fate-mapping analysis, we found that FST promotes expansion of apical cochlear cells, contributing to the formation of the apical cochlear domain. SHH, in contrast, is required both for the induction and maintenance of apical identity. In the absence of FST or SHH, mice produce a short cochlea lacking its apical domain. This results in the loss of apex-specific anatomical and molecular properties and low-frequency-specific hearing loss. [ABSTRACT FROM AUTHOR]
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- 2023
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21. Fursultiamine Prevents Drug-Induced Ototoxicity by Reducing Accumulation of Reactive Oxygen Species in Mouse Cochlea
- Author
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Inkyu Lee, Ye-Ri Kim, Tae-Jun Kwon, Jeong-In Baek, Kyu-Yup Lee, and Un-Kyung Kim
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Mitochondrial ROS ,kanamycin ,Physiology ,Clinical Biochemistry ,cisplatin ,RM1-950 ,Oxidative phosphorylation ,Pharmacology ,Biochemistry ,Article ,Ototoxicity ,medicine ,otorhinolaryngologic diseases ,Molecular Biology ,Cisplatin ,chemistry.chemical_classification ,reactive oxygen species ,Reactive oxygen species ,Aminoglycoside ,fursultiamine ,Cell Biology ,medicine.disease ,medicine.anatomical_structure ,ototoxicity ,chemistry ,Apoptosis ,Therapeutics. Pharmacology ,Hair cell ,medicine.drug - Abstract
Drug-induced hearing loss is a major type of acquired sensorineural hearing loss. Cisplatin and aminoglycoside antibiotics have been known to cause ototoxicity, and excessive accumulation of intracellular reactive oxygen species (ROS) are suggested as the common major pathology of cisplatin- and aminoglycoside antibiotics-induced ototoxicity. Fursultiamine, also called thiamine tetrahydrofurfuryl disulfide, is a thiamine disulfide derivative that may have antioxidant effects. To evaluate whether fursultiamine can prevent cisplatin- and kanamycin-induced ototoxicity, we investigated their preventive potential using mouse cochlear explant culture system. Immunofluorescence staining of mouse cochlear hair cells showed that fursultiamine pretreatment reduced cisplatin- and kanamycin-induced damage to both inner and outer hair cells. Fursultiamine attenuated mitochondrial ROS accumulation as evidenced by MitoSOX Red staining and restored mitochondrial membrane potential in a JC-1 assay. In addition, fursultiamine pretreatment reduced active caspase-3 and TUNEL signals after cisplatin or kanamycin treatment, indicating that fursultiamine decreased apoptotic hair cell death. This study is the first to show a protective effect of fursultiamine against cisplatin- and aminoglycoside antibiotics-induced ototoxicity. Our results suggest that fursultiamine could act as an antioxidant and anti-apoptotic agent against mitochondrial oxidative stress.in cochlear hair cells.
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- 2021
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22. CRISPR/Cas9-mediated genome editing of splicing mutation causing congenital hearing loss
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Nari Ryu, Kyu-Yup Lee, Min-A Kim, Jong Kyung Sonn, Ye-Ri Kim, Deok-Gyun Choi, and Un-Kyung Kim
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0301 basic medicine ,Silent mutation ,Staphylococcus aureus ,Biology ,Cell Line ,Mice ,03 medical and health sciences ,Exon ,0302 clinical medicine ,Bacterial Proteins ,Genome editing ,CRISPR-Associated Protein 9 ,otorhinolaryngologic diseases ,Genetics ,Animals ,Humans ,CRISPR ,Hearing Loss ,Gene Editing ,Cas9 ,Intron ,Gene targeting ,Exons ,Genetic Therapy ,General Medicine ,030104 developmental biology ,Sulfate Transporters ,030220 oncology & carcinogenesis ,Gene Targeting ,RNA splicing ,CRISPR-Cas Systems - Abstract
Clustered regularly interspaced short palindromic repeats (CRISPR)/Cas9 system has ushered in a new era of gene therapy. In this study, we aimed to demonstrate precise CRISPR/Cas9-mediated genome editing of the splicing mutation c.919-2A > G in intron 7 of the SLC26A4 gene, which is the second most common causative gene of congenital hearing loss. We designed candidate single-guide RNAs (sgRNAs) aimed to direct the targeting of Staphylococcus aureus Cas9 to either exon 7 or exon 8 of SLC26A4. Several of the designed sgRNAs showed targeting activity, with average indel efficiencies ranging from approximately 14% to 25%. The usage of dual sgRNAs delivered both into Neuro2a cells and primary mouse embryonic fibroblasts resulted in the successful removal of large genomic fragments within the target locus. We subsequently evaluated genome editing in the presence of artificial donor templates to induce precise target modification via homology-directed repair. Using this approach, two different donor plasmids successfully introduced silent mutations within the c.919-2A region of Slc26a4 without evident off-target activities. Overall, these results indicate that CRISPR/Cas9-mediated correction of mutations in the Slc26a4 gene is a feasible therapeutic option for restoration of hearing loss.
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- 2019
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23. Targeted Gene Delivery into the Mammalian Inner Ear Using Synthetic Serotypes of Adeno-Associated Virus Vectors
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Un-Kyung Kim, Nari Ryu, Tae-Jun Kwon, Min-A Kim, Byeonghyeon Lee, Jinwoong Bok, Hye-Min Kim, and Ye-Ri Kim
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0301 basic medicine ,inner ear ,Cell type ,lcsh:QH426-470 ,Genetic enhancement ,viruses ,Cell ,adeno-associated virus ,Gene delivery ,Biology ,medicine.disease_cause ,Article ,03 medical and health sciences ,0302 clinical medicine ,Genetics ,medicine ,otorhinolaryngologic diseases ,Inner ear ,Vector (molecular biology) ,serotype ,lcsh:QH573-671 ,Molecular Biology ,Adeno-associated virus ,Round window ,lcsh:Cytology ,genetic hearing loss ,gene therapy ,Cell biology ,lcsh:Genetics ,030104 developmental biology ,medicine.anatomical_structure ,030220 oncology & carcinogenesis ,Molecular Medicine ,sense organs - Abstract
Targeting specific cell types in the mammalian inner ear is important for treating genetic hearing loss due to the different cell type-specific functions. Adeno-associated virus (AAV) is an efficient in vivo gene transfer vector, and it has demonstrated promise for treating genetic hearing loss. Although more than 100 AAV serotypes have been identified, few studies have investigated whether AAV can be distributed to specific inner ear cell types. Here we screened three EGFP-AAV reporter constructs (serotypes DJ, DJ8, and PHP.B) in the neonatal mammalian inner ear by injection via the round window membrane to determine the cellular specificity of the AAV vectors. Sensory hair cells, supporting cells, cells in Reissner’s membrane, interdental cells, and root cells were successfully transduced. Hair cells in the cochlear sensory epithelial region were the most frequently transduced cell type by all tested AAV serotypes. The recombinant DJ serotype most effectively transduced a range of cell types at a high rate. Our findings provide a basis for improving treatment of hereditary hearing loss using targeted AAV-mediated gene therapy. Keywords: gene therapy, genetic hearing loss, inner ear, adeno-associated virus, serotype
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- 2019
24. Gene therapy for hereditary hearing loss by SLC26A4 mutations in mice reveals distinct functional roles of pendrin in normal hearing
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Jinwoong Bok, Ji-Hyun Ma, Kyu-Yup Lee, Jae Young Choi, Jinsei Jung, Min-A Kim, Ye-Ri Kim, Philine Wangemann, Nari Ryu, Sung Huhn Kim, Un-Kyung Kim, and Chuan-Jen Hsu
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0301 basic medicine ,Pathology ,Transcription, Genetic ,Pendred syndrome ,Membranous labyrinth ,Medicine (miscellaneous) ,0302 clinical medicine ,Hearing ,Pharmacology, Toxicology and Pharmaceutics (miscellaneous) ,Mice, Knockout ,In-utero ,biology ,Stria Vascularis ,Dependovirus ,Hydrogen-Ion Concentration ,Cochlea ,Phenotype ,medicine.anatomical_structure ,Sulfate Transporters ,Enlarged vestibular aqueduct ,Sensorineural hearing loss ,medicine.symptom ,Research Paper ,medicine.medical_specialty ,Recombinant adeno-associated virus ,Hearing loss ,Solute carrier family 26 member 4 ,Hearing Loss, Sensorineural ,Otolithic Membrane ,03 medical and health sciences ,Gene therapy ,Hair Cells, Auditory ,otorhinolaryngologic diseases ,medicine ,Animals ,Inner ear ,RNA, Messenger ,business.industry ,Epithelial Cells ,Genetic Therapy ,Pendrin ,medicine.disease ,Mice, Inbred C57BL ,030104 developmental biology ,Ear, Inner ,Mutation ,biology.protein ,sense organs ,Endolymphatic Sac ,business ,030217 neurology & neurosurgery - Abstract
Rationale: Mutations of SLC26A4 that abrogate pendrin, expressed in endolymphatic sac, cochlea and vestibule, are known to cause autosomal recessive sensorineural hearing loss with enlargement of the membranous labyrinth. This is the first study to demonstrate the feasibility of gene therapy for pendrin-related hearing loss. Methods: We used a recombinant viral vector to transfect Slc26a4 cDNA into embryonic day 12.5 otocysts of pendrin-deficient knock-out (Slc26a4∆/∆ ) and pendrin-deficient knock-in (Slc26a4tm1Dontuh/tm1Dontuh ) mice. Results: Local gene-delivery resulted in spatially and temporally limited pendrin expression, prevented enlargement, failed to restore vestibular function, but succeeded in the restoration of hearing. Restored hearing phenotypes included normal hearing as well as sudden, fluctuating, and progressive hearing loss. Conclusion: Our study illustrates the feasibility of gene therapy for pendrin-related hearing loss, suggests differences in the requirement of pendrin between the cochlea and the vestibular labyrinth, and documents that insufficient pendrin expression during late embryonal and early postnatal development of the inner ear can cause sudden, fluctuating and progressive hearing loss without obligatory enlargement of the membranous labyrinth.
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- 2019
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25. Genetic analysis of genes related to tight junction function in the Korean population with non-syndromic hearing loss.
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Min-A Kim, Ye-Ri Kim, Borum Sagong, Hyun-Ju Cho, Jae Woong Bae, Jeongho Kim, Jinwook Lee, Hong-Joon Park, Jae Young Choi, Kyu-Yup Lee, and Un-Kyung Kim
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Medicine ,Science - Abstract
Tight junctions (TJs) are essential components of eukaryotic cells, and serve as paracellular barriers and zippers between adjacent tissues. TJs are critical for normal functioning of the organ of Corti, a part of the inner ear that causes loss of sensorineural hearing when damaged. To investigate the relation between genes involved in TJ function and hereditary loss of sensorineural hearing in the Korean population, we selected the TJP2 and CLDN14 genes as candidates for gene screening of 135 Korean individuals. The TJP2 gene, mutation of which causes autosomal dominant non-syndromic hearing loss (ADNSHL), lies at the DFNA51 locus on chromosome 9. The CLDN14 gene, mutation of which causes autosomal recessive non-syndromic hearing loss (ARNSHL), lies at the DFNB29 locus on chromosome 21. In the present study, we conducted genetic analyses of the TJP2 and CLDN14 genes in 87 unrelated patients with ADNSHL and 48 unrelated patients with either ARNSHL or potentially sporadic hearing loss. We identified two pathogenic variations, c.334G>A (p.A112T) and c.3562A>G (p.T1188A), and ten single nucleotide polymorphisms (SNPs) in the TJP2 gene. We found eight non-pathogenic variations in the CLDN14 gene. These findings indicate that, whereas mutation of the TJP2 gene might cause ADNSHL, CLDN14 is not a major causative gene for ARNSHL in the Korean population studied. Our findings may improve the understanding of the genetic cause of non-syndromic hearing loss in the Korean population.
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- 2014
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26. The effect of novel mutations on the structure and enzymatic activity of unconventional myosins associated with autosomal dominant non-syndromic hearing loss
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Tae-Jun Kwon, Se-Kyung Oh, Hong-Joon Park, Osamu Sato, Hanka Venselaar, Soo Young Choi, SungHee Kim, Kyu-Yup Lee, Jinwoong Bok, Sang-Heun Lee, Gert Vriend, Mitsuo Ikebe, Un-Kyung Kim, and Jae Young Choi
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myosin ,mutation ,atpase ,protein structure ,gene ,Biology (General) ,QH301-705.5 - Abstract
Mutations in five unconventional myosin genes have been associated with genetic hearing loss (HL). These genes encode the motor proteins myosin IA, IIIA, VI, VIIA and XVA. To date, most mutations in myosin genes have been found in the Caucasian population. In addition, only a few functional studies have been performed on the previously reported myosin mutations. We performed screening and functional studies for mutations in the MYO1A and MYO6 genes in Korean cases of autosomal dominant non-syndromic HL. We identified four novel heterozygous mutations in MYO6. Three mutations (p.R825X, p.R991X and Q918fsX941) produce a premature truncation of the myosin VI protein. Another mutation, p.R205Q, was associated with diminished actin-activated ATPase activity and actin gliding velocity of myosin VI in an in vitro analysis. This finding is consistent with the results of protein modelling studies and corroborates the pathogenicity of this mutation in the MYO6 gene. One missense variant, p.R544W, was found in the MYO1A gene, and in silico analysis suggested that this variant has deleterious effects on protein function. This finding is consistent with the results of protein modelling studies and corroborates the pathogenic effect of this mutation in the MYO6 gene.
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- 2014
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27. A nonsense
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Minwoo Wendy, Jang, Doo-Yi, Oh, Eunyoung, Yi, Xuezhong, Liu, Jie, Ling, Nayoung, Kim, Kushal, Sharma, Tai Young, Kim, Seungmin, Lee, Ah-Reum, Kim, Min Young, Kim, Min-A, Kim, Mingyu, Lee, Jin-Hee, Han, Jae Joon, Han, Hye-Rim, Park, Bong Jik, Kim, Sang-Yeon, Lee, Dong Ho, Woo, Jayoung, Oh, Soo-Jin, Oh, Tingting, Du, Ja-Won, Koo, Seung-Ha, Oh, Hyun-Woo, Shin, Moon-Woo, Seong, Kyu-Yup, Lee, Un-Kyung, Kim, Jung Bum, Shin, Shushan, Sang, Xinzhang, Cai, Lingyun, Mei, Chufeng, He, Susan H, Blanton, Zheng-Yi, Chen, Hongsheng, Chen, Xianlin, Liu, Aida, Nourbakhsh, Zaohua, Huang, Kwon-Woo, Kang, Woong-Yang, Park, Yong, Feng, C Justin, Lee, and Byung Yoon, Choi
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Male ,cochlea ,Membrane Proteins ,glia-like supporting cells ,Biological Sciences ,Cochlear Implantation ,Connexins ,Pedigree ,Mice, Inbred C57BL ,Mice ,Codon, Nonsense ,otorhinolaryngologic diseases ,Speech Perception ,auditory neuropathy spectrum disorder ,Animals ,Humans ,Female ,Hearing Loss, Central ,Genes, Dominant ,Neuroscience - Abstract
Significance Auditory neuropathy spectrum disorder (ANSD) is a confounding auditory disease in which the subjects respond to sound but have difficulties in speech discrimination. Herein, we examined two Asian families with hereditary late-age–onset ANSD. By linkage analysis and exome sequencing, we identified the TMEM43-p.(Arg372Ter) variant as the etiology of the disease. To examine the mechanism of TMEM43 on ANSD, we generated a knock-in mouse with the p.(Arg372Ter) variant that recapitulated the progressive hearing loss phenotype of the two families. We discovered that variation in TMEM43 impairs the connexin-linked function of mediating passive conductance current in cochlear glial cells. Based on the pathology involving cochlear glial cells, we performed cochlear implant on the human patients, and their speech discrimination ability was restored., Genes that are primarily expressed in cochlear glia-like supporting cells (GLSs) have not been clearly associated with progressive deafness. Herein, we present a deafness locus mapped to chromosome 3p25.1 and an auditory neuropathy spectrum disorder (ANSD) gene, TMEM43, mainly expressed in GLSs. We identify p.(Arg372Ter) of TMEM43 by linkage analysis and exome sequencing in two large Asian families segregating ANSD, which is characterized by inability to discriminate speech despite preserved sensitivity to sound. The knock-in mouse with the p.(Arg372Ter) variant recapitulates a progressive hearing loss with histological abnormalities in GLSs. Mechanistically, TMEM43 interacts with the Connexin26 and Connexin30 gap junction channels, disrupting the passive conductance current in GLSs in a dominant-negative fashion when the p.(Arg372Ter) variant is introduced. Based on these mechanistic insights, cochlear implant was performed on three subjects, and speech discrimination was successfully restored. Our study highlights a pathological role of cochlear GLSs by identifying a deafness gene and its causal relationship with ANSD.
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- 2021
28. A nonsense TMEM43 variant leads to disruption of connexin-linked function and autosomal dominant auditory neuropathy spectrum disorder
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Minwoo Wendy Jang, C. Justin Lee, Nayoung K.D. Kim, Aida Nourbakhsh, Seungmin Lee, Yong Feng, Jayoung Oh, Dong Ho Woo, Bong Jik Kim, Eunyoung Yi, Sang Yeon Lee, Lingyun Mei, Kyu Yup Lee, Doo Yi Oh, Zaohua Huang, Jie Ling, Shushan Sang, Tai Young Kim, Jae Joon Han, Min Young Kim, Byung Yoon Choi, Mingyu Lee, Hongsheng Chen, Min-A Kim, Kushal Sharma, Tingting Du, Xinzhang Cai, Soo Jin Oh, Hyun Woo Shin, Woong-Yang Park, Jin Hee Han, Susan H. Blanton, Jung-Bum Shin, Kwon Woo Kang, Ja Won Koo, Un Kyung Kim, Zheng-Yi Chen, Xianlin Liu, Ah Reum Kim, Moon Woo Seong, Chufeng He, Hye Rim Park, Seung Ha Oh, and Xuezhong Liu
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Multidisciplinary ,medicine.medical_treatment ,media_common.quotation_subject ,Nonsense ,Connexin ,Locus (genetics) ,Biology ,medicine.disease ,Auditory neuropathy spectrum disorder ,Genetic linkage ,Cochlear implant ,otorhinolaryngologic diseases ,medicine ,Neuroscience ,Cochlea ,Exome sequencing ,media_common - Abstract
Genes that are primarily expressed in cochlear glia-like supporting cells (GLSs) have not been clearly associated with progressive deafness. Herein, we present a deafness locus mapped to chromosome 3p25.1 and an auditory neuropathy spectrum disorder (ANSD) gene, TMEM43, mainly expressed in GLSs. We identify p.(Arg372Ter) of TMEM43 by linkage analysis and exome sequencing in two large Asian families segregating ANSD, which is characterized by inability to discriminate speech despite preserved sensitivity to sound. The knock-in mouse with the p.(Arg372Ter) variant recapitulates a progressive hearing loss with histological abnormalities in GLSs. Mechanistically, TMEM43 interacts with the Connexin26 and Connexin30 gap junction channels, disrupting the passive conductance current in GLSs in a dominant-negative fashion when the p.(Arg372Ter) variant is introduced. Based on these mechanistic insights, cochlear implant was performed on three subjects, and speech discrimination was successfully restored. Our study highlights a pathological role of cochlear GLSs by identifying a deafness gene and its causal relationship with ANSD.
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- 2021
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29. A Family of H723R Mutation for Associated with Enlarged Vestibular Aqueduct Syndrome
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SungHee Kim, Dae Gun Song, Jae Woong Bae, Soo-Young Choi, Un-Kyung Kim, Young Jun Choi, Kyu Yup Lee, Sang Heun Lee, and Jung Rae Lee
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Sensorineural hearing loss ,protein ,Human ,Medicine ,Otorhinolaryngology ,RF1-547 - Abstract
Recessive mutations of the SLC26A4 (PDS) gene on chromosome 7q31 can cause sensorineural deafness with goiter (Pendred syndrome, OMIM 274600) or NSRD with goiter (at the DFNB4 locus, OMIM 600791). H723R (2168A>G) is the most commonly reported SLC26A4 mutations in Korean and Japanese and known as founder mutation. We recently experienced one patient with enlarged vestibular aqueduct syndrome. The genetic study showed H723R homozygous in the proband and H723R heterozygous mutation in his family members. The identification of a disease-causing mutation can be used to establish a genotypic diagnosis and provide important information to both families and their physicians.
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- 2009
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30. Phenotype of the Aging-Dependent Spontaneous Onset of Hearing Loss in DBA/2 Mice
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Un-Kyung Kim, Byeonghyeon Lee, Young-In Kim, Kil Soo Kim, Joo-Hee Choi, Young-Suk Jung, Kyung-Ku Kang, Sijoon Lee, Min-Soo Seo, and Soo-Eun Sung
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medicine.medical_specialty ,Hearing loss ,Audiology ,03 medical and health sciences ,0302 clinical medicine ,Animal model ,medicine ,otorhinolaryngologic diseases ,DBA/2 mice ,Dba 2 mice ,Cochlea ,laboratory animals ,030304 developmental biology ,hearing loss ,0303 health sciences ,Hearing ability ,lcsh:Veterinary medicine ,General Veterinary ,business.industry ,Communication ,aging ,Phenotype ,Auditory brainstem response ,lcsh:SF600-1100 ,medicine.symptom ,business ,030217 neurology & neurosurgery - Abstract
Simple Summary In this study, we confirmed the changes in hearing function and inner ear structure over a long period of time in DBA/2 mice, a laboratory animal model suitable for studying hearing loss. We believe that our study is the first to report findings regarding hearing function and structural changes in DBA/2 mice aged ≥34 weeks. These results are of significance for researchers and the scientific community using laboratory animal models. Abstract DBA/2 mice are a well-known animal model for hearing loss developed due to intrinsic properties of these animals. However, results on the phenotype of hearing loss in DBA/2 mice have been mainly reported at an early stage in mice aged ≤7 weeks. Instead, the present study evaluated the hearing ability at 5, 13, and 34 weeks of age using DBA/2korl mice. Auditory brainstem response test was performed at 8–32 KHz at 5, 13, and 34 weeks of age, and hearing loss was confirmed to be induced in a time-dependent manner. In addition, histopathological evaluation at the same age confirmed the morphological damage of the cochlea. The findings presented herein are the results of the long-term observation of the phenotype of hearing loss in DBA/2 mice and can be useful in studies related to aging-dependent hearing loss.
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- 2021
31. A rapid method for simultaneous screening of multi-gene mutations associated with hearing loss in the Korean population.
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Borum Sagong, Jeong-In Baek, Se-Kyung Oh, Kyung Jin Na, Jae Woong Bae, Soo Young Choi, Ji Yun Jeong, Jae Young Choi, Sang-Heun Lee, Kyu-Yup Lee, and Un-Kyung Kim
- Subjects
Medicine ,Science - Abstract
Hearing loss (HL) is a congenital disease with a high prevalence, and patients with hearing loss need early diagnosis for treatment and prevention. The GJB2, MT-RNR1, and SLC26A4 genes have been reported as common causative genes of hearing loss in the Korean population and some mutations of these genes are the most common mutations associated with hearing loss. Accordingly, we developed a method for the simultaneous detection of seven mutations (c.235delC of GJB2, c.439A>G, c.919-2A>G, c.1149+3A>G, c.1229C>T, c.2168A>G of SLC26A4, and m.1555A>G of the MT-RNR1 gene) using multiplex SNaPshot minisequencing to enable rapid diagnosis of hereditary hearing loss. This method was confirmed in patients with hearing loss and used for genetic diagnosis of controls with normal hearing and neonates. We found that 4.06% of individuals with normal hearing and 4.32% of neonates were heterozygous carriers. In addition, we detected that an individual is heterozygous for two different mutations of GJB2 and SLC26A4 gene, respectively and one normal hearing showing the heteroplasmy of m.1555A>G. These genotypes corresponded to those determined by direct sequencing. Overall, we successfully developed a robust and cost-effective diagnosis method that detects common causative mutations of hearing loss in the Korean population. This method will be possible to detect up to 40% causative mutations associated with prelingual HL in the Korean population and serve as a useful genetic technique for diagnosis of hearing loss for patients, carriers, neonates, and fetuses.
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- 2013
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32. Mutational analysis of EYA1, SIX1 and SIX5 genes and strategies for management of hearing loss in patients with BOR/BO syndrome.
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Mee Hyun Song, Tae-Jun Kwon, Hui Ram Kim, Ju Hyun Jeon, Jeong-In Baek, Won-Sang Lee, Un-Kyung Kim, and Jae Young Choi
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Medicine ,Science - Abstract
BACKGROUND: Branchio-oto-renal (BOR) or branchio-otic (BO) syndrome is one of the most common forms of autosomal dominant syndromic hearing loss. Mutations in EYA1, SIX1 and SIX5 genes have been associated with BOR syndrome. In this study, clinical and genetic analyses were performed in patients with BOR/BO syndrome focusing on auditory manifestations and rehabilitation. METHODS: The audiologic manifestations were reviewed in 10 patients with BOR/BO syndrome. The operative findings and hearing outcome were analyzed in patients who underwent middle ear surgeries. The modality and outcome of auditory rehabilitation were evaluated. Genetic analysis was performed for EYA1, SIX1, and SIX5 genes. RESULTS: All patients presented with mixed hearing loss. Five patients underwent middle ear surgeries without successful hearing gain. Cochlear implantation performed in two patients resulted in significant hearing improvement. Genetic analysis revealed four novel EYA1 mutations and a large deletion encompassing the EYA1 gene. CONCLUSIONS: Auditory rehabilitation in BOR/BO syndrome should be individually tailored keeping in mind the high failure rate after middle ear surgeries. Successful outcome can be expected with cochlear implantations in patients with BOR/BO syndrome who cannot benefit from hearing aids. The novel EYA1 mutations may add to the genotypic and phenotypic spectrum of BOR syndrome in the East Asian population.
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- 2013
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33. Mutations in TMEM43 cause autosomal dominant auditory neuropathy spectrum disorder via interaction with connexin-mediated passive conductance channels
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Min Young Kim, Xianlin Liu, Seungmin Lee, Byung Yoon Choi, Yong Feng, Lingyun Mei, Jin Hee Han, Jayoung Oh, Minwoo Wendy Jang, Moon Woo Seong, Kyu Yup Lee, Zaohua Huang, Dong Ho Woo, Bong Jik Kim, Aida Nourbakhsh, Nayoung K.D. Kim, Hongsheng Chen, Min-A Kim, Eunyoung Yi, C. Justin Lee, Jie Ling, Jae Joon Han, Tai Young Kim, Woong-Yang Park, Kushal Sharma, Mingyu Lee, Xinzhang Cai, Doo-Yi Oh, Un-Kyung Kim, Ja Won Koo, Sang-Yeon Lee, Chufeng He, Ting-Ting Du, Hye-Rim Park, Shushan Sang, Seung Ha Oh, Ah Reum Kim, Zheng-Yi Chen, Susan H. Blanton, Jung-Bum Shin, Soo Jin Oh, Hyun Woo Shin, and Xuezhong Liu
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medicine.medical_treatment ,Gap junction ,Connexin ,Locus (genetics) ,Biology ,medicine.disease ,Auditory neuropathy spectrum disorder ,Genetic linkage ,Cochlear implant ,otorhinolaryngologic diseases ,medicine ,Gene ,Neuroscience ,Exome sequencing - Abstract
Genes that are primarily expressed in cochlear glia-like supporting cells (GLSs) have never been clearly associated with progressive deafness. Herein, we present a novel deafness locus mapped to chromosome 3p25.1 and a new auditory neuropathy spectrum disorder (ANSD) gene TMEM43 mainly expressed in GLSs. We identify p.R372X of TMEM43 by linkage analysis and exome sequencing in two large Asian families. The knock-in (KI) mouse with p.R372X mutation recapitulates a progressive hearing loss with histological abnormalities exclusively in GLSs. Mechanistically, TMEM43 interacts with Cx26 and Cx30 gap junction channels, disrupting the passive conductance current in GLSs in a dominant-negative fashion when the p.R372X mutation is introduced. Based on the mechanistic insights, cochlear implant was performed on two patients and speech discrimination was successfully restored. Our study highlights a pathological role of cochlear GLSs by identifying a novel deafness gene and its causal relationship with ANSD.
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- 2020
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34. KL1333, a derivative of β-lapachone, protects against cisplatin-induced ototoxicity in mouse cochlear cultures
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Un-Kyung Kim, Ye-Ri Kim, Inkyu Lee, Kyu-Yup Lee, Jeong-In Baek, and Han-Sol Lee
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0301 basic medicine ,Mitochondrial ROS ,Apoptosis ,RM1-950 ,Pharmacology ,Mitochondrion ,medicine.disease_cause ,Protective Agents ,Antioxidants ,Tissue Culture Techniques ,03 medical and health sciences ,Mice ,0302 clinical medicine ,Ototoxicity ,Hair Cells, Auditory ,medicine ,Animals ,Cochlea ,chemistry.chemical_classification ,Membrane Potential, Mitochondrial ,Cochlear explant ,Reactive oxygen species ,Chemistry ,ROS ,General Medicine ,medicine.disease ,Immunohistochemistry ,Mitochondria ,Oxidative Stress ,030104 developmental biology ,medicine.anatomical_structure ,Organ of Corti ,KL1333 ,030220 oncology & carcinogenesis ,Hair cell ,Therapeutics. Pharmacology ,Cisplatin ,Reactive Oxygen Species ,Oxidative stress ,Naphthoquinones - Abstract
Cisplatin (CP) is a chemotherapeutic drug used to treat cancerous solid tumors, but it causes serious side effects, including ototoxicity. The major cause of CP-induced ototoxicity is increased levels of mitochondrial reactive oxygen species (ROS). In this study, we examined the effect of 2-Isopropyl-3H-naphtho(1,2-d)imidazole-4,5-dione (KL1333), a β-lapachone derivative, on CP-induced ototoxicity using ex vivo organotypic culture system of cochlea. Hair cell damages in CP-treated cochlear explants with or without KL1333 were compared by immunohistochemistry. CP-induced oxidative stress and the preventive effect of KL1333 were analyzed by measuring intracellular ROS levels and depolarization of mitochondrial membrane potential. Activation of apoptosis signaling pathway was detected using TUNEL assay and immunostaining of cleaved caspase-3. As the results, it was found that KL1333 pretreatment significantly decreased stereocilia degeneration and hair cell loss, and prevented an increase in mitochondrial ROS levels in response to CP. Immunohistochemical examinations of cochlear explants revealed greater caspase-3 immunopositivity in the CP group than in controls, while the KL1333 + CP group showed significantly less immunopositivity than the CP group (P < 0.05). Thus, it appeared that KL1333 protected hair cells in the organ of Corti from CP-induced apoptosis by decreasing mitochondrial damages due to the production of mitochondrial ROS. This study is the first report showed the preventive effect of KL1333 against CP-induced ototoxicity. Although further studies should be performed to determine if KL1333 could maintain anticancer effect of CP, our data cautiously suggests that the antioxidant KL1333 can be used as an effective anti-apoptotic agent to prevent ototoxicity caused by CP-induced oxidative stress, and may prove useful in preventing hearing loss caused by CP.
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- 2020
35. Distinct roles of stereociliary links in the nonlinear sound processing and noise resistance of cochlear outer hair cells
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Seok Jun Moon, Jinu Lee, Un-Kyung Kim, Dae Won Moon, Jinwoong Bok, Chul Hoon Kim, Hyehyun Min, Jeong Oh Shin, Jinsei Jung, Ji-Hyun Ma, Jae Young Choi, and Woongsu Han
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Tectorial Membrane ,Hearing loss ,Stereocilia (inner ear) ,Otoacoustic Emissions, Spontaneous ,Biology ,computer.software_genre ,Noise stress ,Stereocilia ,Mice ,medicine ,otorhinolaryngologic diseases ,Animals ,Cochlear Outer Hair Cells ,Audio signal processing ,Outer hair cells ,Hearing Loss ,Cochlea ,Mice, Knockout ,Multidisciplinary ,Biological Sciences ,Mice, Inbred C57BL ,Noise ,Hair Cells, Auditory, Outer ,Sound ,Acoustic Stimulation ,Models, Animal ,Intercellular Signaling Peptides and Proteins ,sense organs ,medicine.symptom ,computer ,Neuroscience ,Microtubule-Associated Proteins - Abstract
Outer hair cells (OHCs) play an essential role in hearing by acting as a nonlinear amplifier which helps the cochlea detect sounds with high sensitivity and accuracy. This nonlinear sound processing generates distortion products, which can be measured as distortion-product otoacoustic emissions (DPOAEs). The OHC stereocilia that respond to sound vibrations are connected by three kinds of extracellular links: tip links that connect the taller stereocilia to shorter ones and convey force to the mechanoelectrical transduction channels, tectorial membrane-attachment crowns (TM-ACs) that connect the tallest stereocilia to one another and to the overlying TM, and horizontal top connectors (HTCs) that link adjacent stereocilia. While the tip links have been extensively studied, the roles that the other two types of links play in hearing are much less clear, largely because of a lack of suitable animal models. Here, while analyzing genetic combinations of tubby mice, we encountered models missing both HTCs and TM-ACs or HTCs alone. We found that the tubby mutation causes loss of both HTCs and TM-ACs due to a mislocalization of stereocilin, which results in OHC dysfunction leading to severe hearing loss. Intriguingly, the addition of the modifier allele modifier of tubby hearing 1 in tubby mice selectively rescues the TM-ACs but not the HTCs. Hearing is significantly rescued in these mice with robust DPOAE production, indicating an essential role of the TM-ACs but not the HTCs in normal OHC function. In contrast, the HTCs are required for the resistance of hearing to damage caused by noise stress.
- Published
- 2020
36. Molecular and clinical characterization of the variable phenotype in Korean families with hearing loss associated with the mitochondrial A1555G mutation.
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Jae Woong Bae, Dong-Bin Kim, Jae Young Choi, Hong-Joon Park, Jong Dae Lee, Dong Gu Hur, Seung-Hyun Bae, Da Jung Jung, Sang Heun Lee, Un-Kyung Kim, and Kyu Yup Lee
- Subjects
Medicine ,Science - Abstract
Hearing loss, which is genetically heterogeneous, can be caused by mutations in the mitochondrial DNA (mtDNA). The A1555G mutation of the 12S ribosomal RNA (rRNA) gene in the mtDNA has been associated with both aminoglycoside-induced and non-syndromic hearing loss in many ethnic populations. Here, we report for the first time the clinical and genetic characterization of nine Korean pedigrees with aminoglycoside-induced and non-syndromic hearing loss. These Korean families carry in the A1555G mutation of 12S rRNA gene and exhibit variable penetrance and expressivity of hearing loss. Specifically, the penetrance of hearing loss in these families ranged between 28.6% and 75%, with an average of 60.8%. These results were higher than the 29.8% penetrance that was previously reported in a Chinese population but similar to the 65.4% and 54.1% penetrance observed in a large Arab-Israeli population and nineteen Spanish pedigrees, respectively. The mutational analysis of the complete mtDNA genome in these families showed that the haplogroups of the Korean population, which belongs to the eastern Asian population, were similar to those of the Chinese population but different from the Spanish population, which belongs to the European-Caucasian population. The mtDNA variants that may act as modifier factors were also found to be similar to the Chinese population. Although the mtDNA haplogroups and variants were similar to the eastern Asian population, we did find some differing phenotypes, although some subjects had the same variants. This result suggests that both the ethnic background and environmental factors lead to a variable phenotype of the A1555G mutation.
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- 2012
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37. Genetic and epigenetic alterations of the NF2 gene in sporadic vestibular schwannomas.
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Jong Dae Lee, Tae Jun Kwon, Un-Kyung Kim, and Won-Sang Lee
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Medicine ,Science - Abstract
BACKGROUND: Mutations in the neurofibromatosis type 2 (NF2) tumor-suppressor gene have been identified in not only NF2-related tumors but also sporadic vestibular schwannomas (VS). This study investigated the genetic and epigenetic alterations in tumors and blood from 30 Korean patients with sporadic VS and correlated these alterations with tumor behavior. METHODOLOGY/PRINCIPAL FINDINGS: NF2 gene mutations were detected using PCR and direct DNA sequencing and three highly polymorphic microsatellite DNA markers were used to assess the loss of heterozygosity (LOH) from chromosome 22. Aberrant hypermethylation of the CpG island of the NF2 gene was also analyzed. The tumor size, the clinical growth index, and the proliferative activity assessed using the Ki-67 labeling index were evaluated. We found 18 mutations in 16 cases of 30 schwannomas (53%). The mutations included eight frameshift mutations, seven nonsense mutations, one in-frame deletion, one splicing donor site, and one missense mutation. Nine patients (30%) showed allelic loss. No patient had aberrant hypermethylation of the NF2 gene and correlation between NF2 genetic alterations and tumor behavior was not observed in this study. CONCLUSIONS/SIGNIFICANCE: The molecular genetic changes in sporadic VS identified here included mutations and allelic loss, but no aberrant hypermethylation of the NF2 gene was detected. In addition, no clear genotype/phenotype correlation was identified. Therefore, it is likely that other factors contribute to tumor formation and growth.
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- 2012
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38. Effective PEI-mediated delivery of CRISPR-Cas9 complex for targeted gene therapy
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Byeonghyeon Lee, Jeong-In Baek, Kyu-Yup Lee, Won Jong Kim, Dongsik Park, Min-A Kim, Kyung-Hee Kim, Ye-Ri Kim, Un-Kyung Kim, and Nari Ryu
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0301 basic medicine ,Genetic enhancement ,Biomedical Engineering ,Pharmaceutical Science ,Medicine (miscellaneous) ,Bioengineering ,Locus (genetics) ,02 engineering and technology ,Computational biology ,Biology ,Mice ,Neuroblastoma ,03 medical and health sciences ,Drug Delivery Systems ,Plasmid ,Genome editing ,Tumor Cells, Cultured ,Animals ,Polyethyleneimine ,CRISPR ,General Materials Science ,Guide RNA ,Gene ,Cell Proliferation ,Cas9 ,Genetic Therapy ,021001 nanoscience & nanotechnology ,030104 developmental biology ,Sulfate Transporters ,Molecular Medicine ,CRISPR-Cas Systems ,0210 nano-technology ,Plasmids - Abstract
The-state-of-art CRISPR/Cas9 is one of the most powerful among the approaches being developed to rescue fundamental causes of gene-based inheritable diseases. Several strategies for delivering such genome editing materials have been developed, but the safety, efficacy over time, cost of production, and gene size limitations are still under debate and must be addressed to further improve applications. In this study, we evaluated branched forms of the polyethylenimine (PEI) - branched PEI 25 kDa (BPEI-25K) - and found that it could efficiently deliver CRISPR/Cas9 plasmids. Plasmid DNA expressing both guide RNA and Cas9 to target the Slc26a4 locus was successfully delivered into Neuro2a cells and meditated genome editing within the targeted locus. Our results demonstrated that BPEI-25K is a promising non-viral vector to deliver the CRISPR/Cas9 system in vitro to mediate targeted gene therapy, and these findings contribute to an understanding of CRISPR/Cas9 delivery that may enable development of successful in vivo techniques.
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- 2018
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39. CHD7 mutational analysis and clinical considerations for auditory rehabilitation in deaf patients with CHARGE syndrome.
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Mee Hyun Song, Hyun-Ju Cho, Hee Keun Lee, Tae Jun Kwon, Won-Sang Lee, Sanghee Oh, Jinwoong Bok, Jae Young Choi, and Un-Kyung Kim
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Medicine ,Science - Abstract
BACKGROUND: Otologic manifestations are one of the most consistent findings of CHARGE syndrome found in more than 90%. Since genetic analysis of the CHD7 gene has rarely been performed in previous reports dealing with ear abnormalities, the genotypic spectrum of CHD7 mutations was analyzed in deaf patients with CHARGE syndrome, and the clinical considerations concerning auditory rehabilitation were investigated. METHODS: Nine Korean patients with CHARGE syndrome showing profound hearing loss and semicircular canal aplasia were included. All 38 exons of CHD7 were analyzed by direct sequencing. For splice site variations, in silico and exon-trapping analyses were performed to verify the pathogenicity of nucleotide variations. Clinical features and the outcome of auditory rehabilitation were also analyzed. RESULTS: Eight of 9 patients revealed alterations of the CHD7 gene including 3 frameshift, 2 nonsense, 2 splice site, and 1 missense mutations. Five of 9 patients were clinically diagnosed as atypical CHARGE syndrome but demonstrated various mutations of the CHD7 gene. One familial case showed intra-familial variability. Radiologic findings suggesting cochleovestibular nerve deficiency were identified in most of the patients. Of the 8 patients who underwent cochlear implantation, 5 patients demonstrated favorable outcome. Larger diameter of the cochleovestibular nerve on imaging and absence of severe mental retardation were factors related to better outcome after cochlear implantation rather than the type of CHD7 mutations. Auditory brainstem implantation was performed in two patients who did not benefit from cochlear implantation. CONCLUSIONS: Genetic analysis of the CHD7 gene should be performed in cases with semicircular canal aplasia even when other typical features of CHARGE syndrome are absent. For auditory rehabilitation in CHARGE syndrome, cochlear implantation should be strongly recommended in selected cases with favorable prognostic factors. Auditory brainstem implantation may be a viable option in patients with CHARGE syndrome who have failed to benefit from cochlear implantation.
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- 2011
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40. Microneedle array with a pH-responsive polymer coating and its application in smart drug delivery for wound healing
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Gyu Man Kim, Haroon Khan, Dongseon Kim, Asad Ullah, Ye-Ri Kim, Mijin Jang, Sanghyun An, Un-Kyung Kim, and Hye Jin Choi
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food.ingredient ,integumentary system ,Chemistry ,Metals and Alloys ,Biofilm ,Penetration (firestop) ,engineering.material ,Condensed Matter Physics ,Gelatin ,Surfaces, Coatings and Films ,Electronic, Optical and Magnetic Materials ,food ,Coating ,Targeted drug delivery ,In vivo ,Materials Chemistry ,engineering ,Electrical and Electronic Engineering ,Wound healing ,Instrumentation ,Layer (electronics) ,Biomedical engineering - Abstract
For successful wound treatment, therapeutics must be delivered directly to the wound. Various issues restrict the delivery of antibiotics to wounds, including the barrier mannered by necrotic tissue and biofilms, which create an extracellular polymeric layer that impedes the efficient administration of therapeutics. For achieving break of the necrotic tissue barrier and biofilm, in addition, improving antibiotics penetration through a painless administration, we fabricated porous polymer coatings on microneedles (MNs) which had the ability of automatic “release” therapeutics in response to wound pH conditions. In the pores of the porous polymer film, the model drug was packed using aqueous gelatin porogen, and the porous layer was coated with a Eudragit S100 film to cap the pores to prevent drug leakage and provide a wound pH-responsive drug release. By combining the advantages of porous and pH-responsive polymer coatings, the coated MNs exhibited remarkably enhanced therapeutic results. This formulation showed both in vivo (in rats) and in vitro (in phosphate-buffered saline and in porcine skin) wound pH-sensitive drug release with rapid responsiveness. At healthy skin pH (pH 4.5), an insignificant release was noticed for MNs in the test media. However, drug release considerably increased when MNs were exposed to wound pH conditions (pH 7.5). The present study provides proof-of-concept evidence that developed MNs have the potential of enhanced treatment protocol for wound infections with the flexibility of coating materials and antimicrobials and offers significant scope for further variations and advancement.
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- 2021
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41. Identification of a novel splicing mutation within SLC17A8 in a Korean family with hearing loss by whole-exome sequencing
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Hong-Joon Park, Jinwoong Bok, Byeonghyeon Lee, Seokwon Lee, Chan Ik Park, Tae-Jun Kwon, Kyu-Yup Lee, Jeong-In Baek, Un-Kyung Kim, and Nari Ryu
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Adult ,Male ,0301 basic medicine ,Hearing loss ,RNA Splicing ,Biology ,DNA sequencing ,03 medical and health sciences ,symbols.namesake ,0302 clinical medicine ,Republic of Korea ,Vesicular Glutamate Transport Proteins ,Genetics ,medicine ,Humans ,Exome ,Hearing Loss ,Exome sequencing ,Aged ,Sanger sequencing ,Massive parallel sequencing ,Genetic heterogeneity ,General Medicine ,Pedigree ,030104 developmental biology ,SLC17A8 ,Mutation ,Mutation (genetic algorithm) ,symbols ,Female ,medicine.symptom ,030217 neurology & neurosurgery - Abstract
Hereditary hearing loss (HHL) is a common genetically heterogeneous disorder, which follows Mendelian inheritance in humans. Because of this heterogeneity, the identification of the causative gene of HHL by linkage analysis or Sanger sequencing have shown economic and temporal limitations. With recent advances in next-generation sequencing (NGS) techniques, rapid identification of a causative gene via massively parallel sequencing is now possible. We recruited a Korean family with three generations exhibiting autosomal dominant inheritance of hearing loss (HL), and the clinical information about this family revealed that there are no other symptoms accompanied with HL. To identify a causative mutation of HL in this family, we performed whole-exome sequencing of 4 family members, 3 affected and an unaffected. As the result, A novel splicing mutation, c.763+1G>T, in the solute carrier family 17, member 8 (SLC17A8) gene was identified in the patients, and the genotypes of the mutation were co-segregated with the phenotype of HL. Additionally, this mutation was not detected in 100 Koreans with normal hearing. Via NGS, we detected a novel splicing mutation that might influence the hearing ability within the patients with autosomal dominant non-syndromic HL. Our data suggests that this technique is a powerful tool to discover causative genetic factors of HL and facilitate diagnoses of the primary cause of HHL.
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- 2017
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42. Spatiotemporal expression patterns of clusterin in the mouse inner ear
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Jeong Oh Shin, Seokwon Lee, Jinwoong Bok, Borum Sagong, and Un-Kyung Kim
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0301 basic medicine ,Pathology ,medicine.medical_specialty ,Histology ,Fluorescent Antibody Technique ,Gene Expression ,In situ hybridization ,Pathology and Forensic Medicine ,Mice ,03 medical and health sciences ,0302 clinical medicine ,Downregulation and upregulation ,otorhinolaryngologic diseases ,medicine ,Animals ,Inner ear ,RNA, Messenger ,Cochlea ,Messenger RNA ,biology ,Clusterin ,Gene Expression Regulation, Developmental ,Cell Biology ,Cell biology ,Mice, Inbred C57BL ,030104 developmental biology ,medicine.anatomical_structure ,Organ of Corti ,Ear, Inner ,Chaperone (protein) ,biology.protein ,Female ,sense organs ,030217 neurology & neurosurgery - Abstract
Clusterin (CLU) is an extracellular chaperone protein that is implicated in diverse physiological and pathophysiological cellular processes. CLU expression is upregulated in response to cellular stress and under certain conditions, such as neurodegenerative disease and cancer. CLU primarily functions as a chaperone that exerts cytoprotective effects by removing cellular debris and misfolded proteins and also acts as a signaling molecule that regulates pro-survival pathways. Deafness is caused by genetic factors and various extrinsic insults, including ototoxic drugs, exposure to loud sounds and aging. Considering its cytoprotectivity, CLU may also mediate cellular defense mechanisms against hearing loss due to cellular stresses. To understand the function of CLU in the inner ear, we analyze CLU expression patterns in the mouse inner ear during development and in the adult stage. Results of quantitative real-time polymerase chain reaction analysis showed that Clu mRNA levels in the inner ear were increased during embryogenesis and were constantly expressed in the adult. Detailed spatial expression patterns of Clu both in the mRNA and protein levels were analyzed throughout various developmental stages via in situ hybridization and immunofluorescence staining. Clu expression was found in specific domains of developing inner ear starting from the otocyst stage, mainly adjacent to the prosensory domain of the cochlear epithelium. In the mature inner ear, Clu expression was observed in Deiter's cells and pillar cells of the organ of Corti, outer sulcus and in basal cells of the stria vascularis in the cochlea. These specific spatiotemporal expression patterns suggest the possible roles of CLU in inner ear development and in maintaining proper hearing function.
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- 2017
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43. Protective effects of 1,2,3-triazole derivative KPR-A020 against cisplatin-induced ototoxicity in murine cochlear cultures
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Sekyung Oh, Tae-Ho Lee, Kyu-Yup Lee, Da Jung Jung, Inkyu Lee, Un-Kyung Kim, and Ye-Ri Kim
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0301 basic medicine ,Mitochondrial ROS ,medicine.medical_specialty ,Antioxidant ,Cell Survival ,medicine.medical_treatment ,Antineoplastic Agents ,Apoptosis ,Pharmacology ,Antioxidants ,Mice ,03 medical and health sciences ,0302 clinical medicine ,Ototoxicity ,medicine ,Animals ,Hearing Loss ,Cisplatin ,chemistry.chemical_classification ,Reactive oxygen species ,business.industry ,General Medicine ,Triazoles ,medicine.disease ,Immunohistochemistry ,Cochlea ,Surgery ,Oxidative Stress ,030104 developmental biology ,medicine.anatomical_structure ,Otorhinolaryngology ,chemistry ,Organ of Corti ,030220 oncology & carcinogenesis ,Pediatrics, Perinatology and Child Health ,Toxicity ,Hair cell ,Reactive Oxygen Species ,business ,medicine.drug - Abstract
Cisplatin (cis-diaminedichloridoplatinum(II), cis-[PtCl2(NH3)2]) is an effective chemotherapeutic agent in the treatment of several types of malignant solid tumors but its clinical use is associated with ototoxicity. Several studies have investigated the effect of antioxidants on cisplatin-induced ototoxicity in mice. The triazole KPR-A020 has been shown to play a protective role against mitochondrial dysfunction by reducing the production of mitochondrial reactive oxygen species (ROS). The effect of KPR-A020 on cisplatin-induced ototoxicity was examined using cultures of cochlear explants. Healthy mice were randomly divided into 4 groups: control, treated with cisplatin alone (CP), treated with cisplatin and KPR-A020 (CP + KPR-A020), and treated with KPR-A020 alone (KPR-A020). The cochlear explants were harvested for histological and immunohistochemical examinations. Biochemical analyses of the explants revealed that pre-treatment with KPR-A020 prevented an increase in mitochondrial ROS levels. Moreover, the CP + KPR-A020 group showed better hair cell survival than the CP group. Immunohistochemical examinations of cochlear explants stained with anti-caspase-3 revealed greater immunopositivity in the CP group. The CP + KPR-A020 group showed significantly less immunopositivity than the CP group (P < 0.05). Thus, it appears that KPR-A020 protects hair cells in the organ of Corti from cisplatin-induced toxicity by decreasing the production of mitochondrial ROS. The results of this study suggest that KPR-A020 can be used as an antioxidant and antiapoptotic agent to prevent hearing loss caused by cisplatin induced-oxidative stress.
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- 2017
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44. A Novel Frameshift Mutation of SLC26A4 in a Korean Family With Nonsyndromic Hearing Loss and Enlarged Vestibular Aqueduct
- Author
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Un-Kyung Kim, Borum Sagong, Jeong-In Baek, and Kyu-Yup Lee
- Subjects
0301 basic medicine ,Genetics ,medicine.medical_specialty ,business.industry ,Hearing loss ,Audiology ,Compound heterozygosity ,medicine.disease ,Frameshift mutation ,03 medical and health sciences ,genomic DNA ,030104 developmental biology ,0302 clinical medicine ,Otorhinolaryngology ,030220 oncology & carcinogenesis ,Mutation (genetic algorithm) ,otorhinolaryngologic diseases ,Mutation testing ,medicine ,Surgery ,medicine.symptom ,business ,Novel mutation ,DFNB4 ,Hearing Loss ,Enlarged Vestibular Aqueduct ,SLC26A4 ,NovelMutation ,Enlarged vestibular aqueduct - Abstract
Objectives We aimed to identify the causative mutation for siblings in a Korean family with nonsyndromic hearing loss (HL) and enlarged vestibular aqueduct (EVA). The siblings were a 19-year-old female with bilateral profound HL and an 11-year-old male with bilateral moderately severe HL. Methods We extracted genomic DNA from blood samples of the siblings with HL, their parents, and 100 controls. We performed mutation analysis for SLC26A4 using direct sequencing. Results The two siblings were compound heterozygotes with the novel mutation p.I713LfsX8 and the previously described mutation p.H723R. Their parents had heterozygous mono-allelic mutations. Father had p.I713LfsX8 mutation as heterozygous, and mother had p.H723R mutation as heterozygous. However, novel mutation p.I713LfsX8 was not detected in 100 unrelated controls. Conclusion Both mutations identified in this study were located in the sulfate transporter and anti-sigma factor antagonist domain, the core region for membrane targeting of SulP/SLC26 anion transporters, which strongly suggests that failure in membrane trafficking by SLC26A4 is a direct cause of HL in this family. Our study could therefore provide a foundation for further investigations elucidating the SLC26A4-related mechanisms of HL.
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- 2017
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45. Temporal and spatial expression patterns of Hedgehog receptors in the developing inner and middle ear
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Harinarayana Ankamreddy, Seokwon Lee, Naga Mahesh Jakka, Jinwoong Bok, Un Kyung Kim, and Jeong Oh Shin
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0301 basic medicine ,Patched ,Embryology ,Neurogenesis ,Ear, Middle ,Cell Cycle Proteins ,Receptors, Cell Surface ,Biology ,GPI-Linked Proteins ,Mice ,03 medical and health sciences ,Pregnancy ,otorhinolaryngologic diseases ,medicine ,Animals ,Hedgehog Proteins ,Inner ear ,Sonic hedgehog ,Hedgehog ,Mice, Inbred ICR ,Hair cell differentiation ,Anatomy ,Embryonic stem cell ,Cell biology ,Patched-1 Receptor ,030104 developmental biology ,medicine.anatomical_structure ,PTCH1 ,Ear, Inner ,Immunoglobulin G ,Middle ear ,biology.protein ,Female ,sense organs ,Cell Adhesion Molecules ,Signal Transduction ,Developmental Biology - Abstract
The mammalian inner ear is a complex organ responsible for balance and hearing. Sonic hedgehog (Shh), a member of the Hedgehog (Hh) family of secreted proteins, has been shown to play important roles in several aspects of inner ear development, including dorsoventral axial specification, cochlear elongation, tonotopic patterning, and hair cell differentiation. Hh proteins initiate a downstream signaling cascade by binding to the Patched 1 (Ptch1) receptor. Recent studies have revealed that other types of co-receptors can also mediate Hh signaling, including growth arrest-specific 1 (Gas1), cell-adhesion molecules-related/down-regulated by oncogenes (Cdon), and biregional Cdon binding protein (Boc). However, little is known about the role of these Hh co-receptors in inner ear development. In this study, we examined the expression patterns of Gas1, Cdon, and Boc, as well as that of Ptch1, in the developing mouse inner ear from otocyst (embryonic day (E) 9.5) until birth and in the developing middle ear at E15.5. Ptch1, a readout of Hh signaling, was expressed in a graded pattern in response to Shh signaling throughout development. Expression patterns of Gas1, Cdon, and Boc differed from that of Ptch1, and each Hh co-receptor was expressed in specific cells and domains in the developing inner and middle ear. These unique and differential expression patterns of Hh co-receptors suggest their roles in mediating various time- and space-specific functions of Shh during ear development.
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- 2017
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46. Modified U1 snRNA and antisense oligonucleotides rescue splice mutations in SLC26A4 that cause hereditary hearing loss
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Sekyung Oh, Sang-Joo Kim, Jeong-In Baek, Sung-Ho Goh, Ye-Ri Kim, Jong-Heun Kim, Kyu-Yup Lee, Un-Kyung Kim, and Byeonghyeon Lee
- Subjects
Hearing Loss, Sensorineural ,Biology ,U1 snRNA binding ,Conserved sequence ,03 medical and health sciences ,Transcription (biology) ,RNA, Small Nuclear ,otorhinolaryngologic diseases ,Genetics ,Humans ,splice ,Gene ,Conserved Sequence ,Genetics (clinical) ,030304 developmental biology ,0303 health sciences ,Binding Sites ,Base Sequence ,030305 genetics & heredity ,Oligonucleotides, Antisense ,Introns ,Alternative Splicing ,Sulfate Transporters ,Mutation ,RNA splicing ,RNA Splice Sites ,Small nuclear RNA ,HeLa Cells ,Minigene - Abstract
One of most important factors for messenger RNA (mRNA) transcription is the spliceosomal component U1 small nuclear RNA (snRNA), which recognizes 5' splicing donor sites at specific regions in pre-mRNA. Mutations in these sites disrupt U1 snRNA binding and cause abnormal splicing. In this study, we investigated mutations at splice sites in SLC26A4 (HGNC 8818), one of the major causative genes of hearing loss, which may result in the synthesis of abnormal pendrin, the channel protein encoded by the gene. Seventeen SLC26A4 variants with mutations in the U1 snRNA binding sites were assessed by minigene splicing assays, and 11 were found to result in abnormal splicing. Interestingly, eight of the 11 pathogenic mutations were intronic, suggesting the importance of conserved sequences at the intronic splice site. The application of modified U1 snRNA effectively rescued the abnormal splicing for most of these mutations. Although three were cryptic mutations, they were rescued by cotransfection of modified U1 snRNA and modified antisense oligonucleotides. Our results demonstrate the important role of snRNA in SLC26A4 mutations, suggesting the therapeutic potential of modified U1 snRNA and antisense oligonucleotides for neutralizing the pathogenic effect of the splice-site mutations that may result in hearing loss.
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- 2019
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47. C-phycocyanin from Limnothrix Species KNUA002 Alleviates Cisplatin-Induced Ototoxicity by Blocking the Mitochondrial Apoptotic Pathway in Auditory Cells
- Author
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Ho-Sung Yoon, Jeong-Mi Do, Kyung Hee Kim, Seung-Woo Jo, Un-Kyung Kim, Ye-Ri Kim, and Alexandra R. Stoica
- Subjects
Limnothrix ,Cell Survival ,Pharmaceutical Science ,cisplatin ,Antineoplastic Agents ,Apoptosis ,Pharmacology ,medicine.disease_cause ,Cyanobacteria ,Protective Agents ,Article ,Cell Line ,03 medical and health sciences ,Mice ,0302 clinical medicine ,Ototoxicity ,In vivo ,Drug Discovery ,Hair Cells, Auditory ,medicine ,Animals ,Cytotoxicity ,Hearing Loss ,lcsh:QH301-705.5 ,Pharmacology, Toxicology and Pharmaceutics (miscellaneous) ,030304 developmental biology ,bcl-2-Associated X Protein ,chemistry.chemical_classification ,Cisplatin ,0303 health sciences ,Reactive oxygen species ,Caspase 3 ,Phycocyanin ,Cell Cycle Checkpoints ,medicine.disease ,C-phycocyanin ,Mitochondria ,ototoxicity ,lcsh:Biology (General) ,chemistry ,Proto-Oncogene Proteins c-bcl-2 ,Cell culture ,HEI-OC1 ,Reactive Oxygen Species ,030217 neurology & neurosurgery ,Oxidative stress ,medicine.drug - Abstract
Ototoxicity, or adverse pharmacological effects on the inner ear or auditory nerve, is a common side effect of cisplatin, a platinum-based drug widely used in anticancer chemotherapy. Although the incidence of ototoxicity is high among patients that receive cisplatin therapy, there is currently no effective treatment for it. The generation of excessive reactive oxygen species (ROS) is considered to be the major cause of cisplatin-induced ototoxicity. C-phycocyanin (C-PC), a blue phycobiliprotein found in cyanobacteria and red algae, has antioxidant and anticancer activities in different experimental models in vitro and in vivo. Thus, we tested the ability of C-PC from Limnothrix sp. KNUA002 to protect auditory cells from cisplatin-induced ototoxicity in vitro. Pretreatment with C-PC from Limnothrix sp. KNUA002 inhibited apoptosis and protected mitochondrial function by preventing ROS accumulation in cisplatin-treated House Ear Institute-Organ of Corti 1 (HEI-OC1) cells, a mouse auditory cell line. Cisplatin increased the expression of Bax and reduced the expression of Bcl-2, which activate and inhibit, respectively, the mitochondrial apoptotic pathway in response to oxidative stress. Pretreatment with C-PC prior to cisplatin treatment caused the Bax and Bcl-2 levels to stay close to the levels in untreated control cells. Our results suggest that C-PC from Limnothrix sp. KNUA002 protects cells against cisplatin-induced cytotoxicity by inhibiting the mitochondrial apoptotic pathway.
- Published
- 2019
48. A family with a mild form of congenital nystagmus and optic disc coloboma caused by a novel PAX6 mutation
- Author
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Deok-Gyun Choi, Un-Kyung Kim, Eun Hye Oh, Byeonghyeon Lee, Bo Young Chun, Jin-Sung Park, and Yun Jeong Lee
- Subjects
0301 basic medicine ,Male ,medicine.medical_specialty ,PAX6 Transcription Factor ,Optic Disk ,Video Recording ,Nystagmus ,Biology ,03 medical and health sciences ,0302 clinical medicine ,Ophthalmology ,Exome Sequencing ,Genetics ,medicine ,Videonystagmography ,Humans ,Point Mutation ,Genetic Predisposition to Disease ,medicine.diagnostic_test ,Point mutation ,Fundus photography ,Optic Nerve ,General Medicine ,medicine.disease ,eye diseases ,Pedigree ,Coloboma ,030104 developmental biology ,Phenotype ,Aniridia ,030220 oncology & carcinogenesis ,Child, Preschool ,Mutation (genetic algorithm) ,Female ,sense organs ,PAX6 ,medicine.symptom ,Nystagmus, Congenital ,Congenital nystagmus - Abstract
Congenital nystagmus (CN) is a heterogeneous disease that shows variable clinical features. There are a few mutations that are known to cause CN. Among them, a PAX6 mutation is known to cause CN with an extremely high frequency of aniridia. Here, we report on a family with an autosomal dominant PAX6 mutation, c.214G > A (p.Gly72Ser.), who presented with CN in the absence of aniridia. This study describes detailed clinical findings, including videonystagmography and fundus photography findings and emphasizes the importance of screening for the PAX6 gene in patients who present with CN in the absence of aniridia, as this will further elucidate the known phenotypes of PAX6-related diseases.
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- 2019
49. ClinGen Expert Clinical Validity Curation of 164 Hearing Loss Gene-Disease Pairs
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Marina T. DiStefano, Sarah E. Hemphill, Andrea M. Oza, Rebecca K. Siegert, Andrew R. Grant, Madeline Y. Hughes, Brandon J. Cushman, Hela Azaiez, Kevin T. Booth, Alex Chapin, Hatice Duzkale, Tatsuo Matsunaga, Jun Shen, Wenying Zhang, Margaret Kenna, Lisa A. Schimmenti, Mustafa Tekin, Heidi L. Rehm, Ahmad N. Abou Tayoun, Sami S. Amr, Sonia Abdelhak, John Alexander, Karen Avraham, Neha Bhatia, Donglin Bai, Nicole Boczek, Zippora Brownstein, Rachel Burt, Yasmin Bylstra, Ignacio del Castillo, Byung Yoon Choi, Lilian Downie, Thomas Friedman, Anne Giersch, Jasmine Goh, John Greinwald, Andrew J. Griffith, Amy Hernandez, Jeffrey Holt, Makoto Hosoya, Lim Jiin Ying, Kanika Jain, Un-Kyung Kim, Hannie Kremer, Ian Krantz, Suzanne Leal, Morag Lewis, Xue Zhong Liu, Wendy Low, Yu Lu, Minjie Luo, Saber Masmoudi, Tan Yuen Ming, Miguel Angel Moreno-Pelayo, Matías Morín, Cynthia Morton, Jaclyn Murray, Hideki Mutai, Kiyomitsu Nara, Arti Pandya, Sylvia Kam Pei-Rong, Richard J.H. Smith, Saumya Shekhar Jamuar, Funda Elif Suer, Shin-Ichi Usami, Guy Van Camp, Kazuki Yamazawa, Hui-Jun Yuan, Elizabeth Black-Zeigelbein, Keijan Zhang, and ClinGen Hearing Loss Clinical Domain Working Group
- Subjects
ClinGen ,Hearing loss ,Medical laboratory ,Computational biology ,Disease ,Deafness ,gene curation ,Genome ,Sensory disorders Donders Center for Medical Neuroscience [Radboudumc 12] ,Article ,genetic diagnosis ,03 medical and health sciences ,0302 clinical medicine ,Databases, Genetic ,Humans ,Medicine ,Genetic Testing ,Hearing Loss ,Biology ,Gene ,Genetics (clinical) ,Data Curation ,030304 developmental biology ,Genetic testing ,0303 health sciences ,medicine.diagnostic_test ,Genome, Human ,business.industry ,Genetic Variation ,Reproducibility of Results ,Genomics ,Medical decision making ,Human genetics ,Mutation ,Clinical validity ,Human medicine ,medicine.symptom ,business ,030217 neurology & neurosurgery - Abstract
PurposeProper interpretation of genomic variants is critical to successful medical decision making based on genetic testing results. A fundamental prerequisite to accurate variant interpretation is the clear understanding of the clinical validity of gene-disease relationships. The Clinical Genome Resource (ClinGen) has developed a semi-quantitative framework to assign clinical validity to gene-disease relationships.MethodsThe ClinGen Hearing Loss Gene Curation Expert Panel (HL GCEP) uses this framework to perform evidence-based curations of genes present on testing panels from 17 clinical laboratories in the Genetic Testing Registry. The HL GCEP curated and reviewed 142 genes and 164 gene-disease pairs, including 105 nonsyndromic and 59 syndromic forms of hearing loss.ResultsThe final outcome included 82 Definitive (50%), 12 Strong (7%), 25 Moderate (15%), 32 Limited (20%), 10 Disputed (6%), and 3 Refuted (2%) classifications. The summary of each curation is date stamped with the HL GCEP approval, is live, and will be kept up-to-date on the ClinGen website (https://search.clinicalgenome.org/kb/gene-validity).ConclusionThis gene curation approach serves to optimize the clinical sensitivity of genetic testing while reducing the rate of uncertain or ambiguous test results caused by the interrogation of genes with insufficient evidence of a disease link.
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- 2019
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50. A novel REEP1 splicing mutation with broad clinical variability in a family with hereditary spastic paraplegia
- Author
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Seong-Yong Park, Un-Kyung Kim, Byeonghyeon Lee, Jin-Mo Park, and Jin-Sung Park
- Subjects
Adult ,Male ,0301 basic medicine ,Heterozygote ,Hereditary spastic paraplegia ,RNA Splicing ,Ankle contracture ,Biology ,Asymptomatic ,03 medical and health sciences ,0302 clinical medicine ,Genetics ,medicine ,Humans ,Family ,Exome sequencing ,Spastic Paraplegia, Hereditary ,Membrane Transport Proteins ,General Medicine ,Middle Aged ,medicine.disease ,Phenotype ,Pedigree ,030104 developmental biology ,030220 oncology & carcinogenesis ,Mutation ,Immunology ,Mutation (genetic algorithm) ,Female ,Restriction fragment length polymorphism ,medicine.symptom ,Asymptomatic carrier - Abstract
Hereditary spastic paraplegia (HSP) is a heterogeneous group of genetic disorders characterized by lower-limb spastic paralysis. We report on a family with three generations of autosomal dominant inheritance of HSP caused by a novel heterozygous splice-site mutation (c.303 + 2 T > C) in REEP1 that was confirmed by RFLP analysis. Carriers of the mutation, including one asymptomatic individual, showed a mild HSP phenotype with a wide range of intrafamilial variation. All symptomatic carriers had ankle contractures in addition to other classical clinical symptoms of HSP. Clinicians should suspect REEP1-related HSP in patients who show ankle contractures with other symptoms of HSP and should consider that these patients have asymptomatic carriers within their family.
- Published
- 2021
- Full Text
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