Your search keyword '"EPIDERMOLYSIS bullosa"' showing total 403 results

1. Gene-edited cells: novel allogeneic gene/cell therapy for epidermolysis bullosa.

Author

Gila, Fatemeh, Alamdari-Palangi, Vahab, Rafiee, Maedeh, Jokar, Arezoo, Ehtiaty, Sajad, Dianatinasab, Aria, Khatami, Seyyed Hossein, Taheri-Anganeh, Mortaza, Movahedpour, Ahmad, and Fallahi, Jafar

Abstract

Epidermolysis bullosa (EB) is a group of rare genetic skin fragility disorders, which are hereditary. These disorders are associated with mutations in at least 16 genes that encode components of the epidermal adhesion complex. Currently, there are no effective treatments for this disorder. All current treatment approaches focus on topical treatments to prevent complications and infections. In recent years, significant progress has been achieved in the treatment of the severe genetic skin blistering condition known as EB through preclinical and clinical advancements. Promising developments have emerged in the areas of protein and cell therapies, such as allogeneic stem cell transplantation; in addition, RNA-based therapies and gene therapy approaches have also become a reality. Stem cells obtained from embryonic or adult tissues, including the skin, are undifferentiated cells with the ability to generate, maintain, and replace fully developed cells and tissues. Recent advancements in preclinical and clinical research have significantly enhanced stem cell therapy, presenting a promising treatment option for various diseases that are not effectively addressed by current medical treatments. Different types of stem cells such as primarily hematopoietic and mesenchymal, obtained from the patient or from a donor, have been utilized to treat severe forms of diseases, each with some beneficial effects. In addition, extensive research has shown that gene transfer methods targeting allogeneic and autologous epidermal stem cells to replace or correct the defective gene are promising. These methods can regenerate and restore the adhesion of primary keratinocytes in EB patients. The long-term treatment of skin lesions in a small number of patients has shown promising results through the transplantation of skin grafts produced from gene-corrected autologous epidermal stem cells. This article attempts to summarize the current situation, potential development prospects, and some of the challenges related to the cell therapy approach for EB treatment. [ABSTRACT FROM AUTHOR]

Published

2024

2. Highlights of Gene and Cell Therapy for Epidermolysis Bullosa and Ichthyosis.

Author

Koutsoukos, Stefanos A. and Bilousova, Ganna

Subjects

*EPIDERMOLYSIS bullosa, *GENE therapy, *ICHTHYOSIS, *CELLULAR therapy, *TECHNOLOGICAL innovations, *SKIN diseases, *MOLECULAR genetics

Abstract

Advancements in the molecular genetics of epidermolysis bullosa (EB) and ichthyosis, two rare inherited skin conditions, have enabled the identification of genetic variants that cause these diseases. Alongside technological advancements in genetic medicine, the identification of variants causal of these rare skin conditions has led to preclinical research and the clinical development of various in vivo and ex vivo gene and cell therapies for their treatment. Gene and cell therapies are considered to be the most advanced forms of personalized medicine, demonstrating safety and efficacy in numerous rare diseases. Although the orphan drug development boom has resulted in regulatory approval of multiple gene and cell therapies for various rare conditions, the application of these modalities to rare inherited skin conditions remains limited. Nonetheless, there are successful examples of both in vivo gene therapy- and ex vivo cell therapy-based approaches developed to treat EB and ichthyosis. This review highlights preclinical research and the clinical development of gene and cell therapies for multiple subtypes of these two devastating congenital skin conditions, including a gene therapy recently approved by the U.S. Food and Drug Administration for the treatment of recessive dystrophic EB. Plain Language Summary: Advances in genetics research for skin diseases such as epidermolysis bullosa and ichthyosis have led to the discovery of many new subtypes of these severe skin conditions. Identifying new subtypes has in turn led to new treatments for these conditions, including gene and cell therapies. Gene and cell therapies aim to address the underlying genetic causes of disease and have already shown success in the clinic. While the development of such treatments for rare skin diseases has been limited, there are notable examples of gene and cell therapies developed for epidermolysis bullosa and ichthyosis. This review highlights recent developments in gene and cell therapy for epidermolysis bullosa and ichthyosis, including a newly approved gene therapy for recessive dystrophic epidermolysis bullosa. [ABSTRACT FROM AUTHOR]

Published

2024

3. Effectiveness and safety of mexiletine versus placebo in patients with myotonia: a systematic review and meta-analysis.

Author

Elettreby, Abdelrahman Mohammed, Elnaga, Ahmed Abdullah Abo, Alsaied, Mohamed Ahmed, Ewis, Dalia Kamal, Sharkawy, Aya Mohammed, Fareed, Rahma, and Alderbi, Gehad Magdy

Subjects

*MEXILETINE, *CLINICAL trials, *PLACEBOS, *PATIENT safety, *EPIDERMOLYSIS bullosa

Abstract

Background: The rare nature of dystrophic and non-dystrophic myotonia has limited the available evidence on the efficacy of mexiletine as a potential treatment. To address this gap, we conducted a systematic review and meta-analysis to evaluate the effectiveness and safety of mexiletine for both dystrophic and non-dystrophic myotonic patients. Methods: The search was conducted on various electronic databases up to March 2023, for randomized clinical trials (RCTs) comparing mexiletine versus placebo in myotonic patients. A risk of bias assessment was carried out, and relevant data was extracted manually into an online sheet. RevMan software (version 5.4) was employed for analysis. Results: A total of five studies, comprising 186 patients, were included in the meta-analysis. Our findings showed that mexiletine was significantly more effective than placebo in improving stiffness score (SMD = − 1.19, 95% CI [− 1.53, − 0.85]), as well as in reducing hand grip myotonia (MD = − 1.36 s, 95% CI [− 1.83, − 0.89]). Mexiletine also significantly improved SF-36 Physical and Mental Component Score in patients with non-dystrophic myotonia only. Regarding safety, mexiletine did not significantly alter ECG parameters but was associated with greater gastrointestinal symptoms (GIT) compared to placebo (RR 3.7, 95% CI [1.79, 7.64]). Other adverse events showed no significant differences. Conclusion: The results support that mexiletine is effective and safe in myotonic patients; however, it is associated with a higher risk of GIT symptoms. Due to the scarcity of published RCTs and the prevalence of GIT symptoms, we recommend further well-designed RCTs testing various drug combinations to reduce GIT symptoms. [ABSTRACT FROM AUTHOR]

Published

2024

4. Treatment of Epidermolysis Bullosa and Future Directions: A Review.

Author

Danescu, Sorina, Negrutiu, Mircea, and Has, Cristina

Subjects

*EPIDERMOLYSIS bullosa, *GENE therapy, *DRUG therapy, *WOUND healing, *DRUG repositioning, *GENETIC disorders

Abstract

Epidermolysis bullosa (EB) comprises rare genetic disorders characterized by skin and mucosal membrane blistering induced by mechanical trauma. Molecularly, pathogenic variants affect genes encoding proteins crucial for epidermal–dermal adhesion and stability. Management of severe EB is multidisciplinary, focusing on wound healing support, ensuring that patients thrive, and complication treatment. Despite extensive research over 30 years, novel therapeutic approaches face challenges. Gene therapy and protein therapy struggle with efficacy, while regenerative cell-based therapies show limited effects. Drug repurposing to target various pathogenic mechanisms has gained attention, as has in vivo gene therapy with drugs for dystrophic and junctional EB that were recently approved by the US Food and Drug Administration (FDA) and European Medicines Agency (EMA). However, their high cost limits global accessibility. This review examines therapeutic advancements made over the past 5 years, exploiting a systematic literature review and clinical trial data. [ABSTRACT FROM AUTHOR]

Published

2024

5. A scalable and cGMP-compatible autologous organotypic cell therapy for Dystrophic Epidermolysis Bullosa.

Author

Neumayer, Gernot, Torkelson, Jessica L., Li, Shengdi, McCarthy, Kelly, Zhen, Hanson H., Vangipuram, Madhuri, Mader, Marius M., Gebeyehu, Gulilat, Jaouni, Taysir M., Jacków-Malinowska, Joanna, Rami, Avina, Hansen, Corey, Guo, Zongyou, Gaddam, Sadhana, Tate, Keri M., Pappalardo, Alberto, Li, Lingjie, Chow, Grace M., Roy, Kevin R., and Nguyen, Thuylinh Michelle

Subjects

EPIDERMOLYSIS bullosa, CELLULAR therapy, INDUCED pluripotent stem cells, SKIN grafting, NUCLEOTIDE sequencing

Abstract

We present Dystrophic Epidermolysis Bullosa Cell Therapy (DEBCT), a scalable platform producing autologous organotypic iPS cell-derived induced skin composite (iSC) grafts for definitive treatment. Clinical-grade manufacturing integrates CRISPR-mediated genetic correction with reprogramming into one step, accelerating derivation of COL7A1-edited iPS cells from patients. Differentiation into epidermal, dermal and melanocyte progenitors is followed by CD49f-enrichment, minimizing maturation heterogeneity. Mouse xenografting of iSCs from four patients with different mutations demonstrates disease modifying activity at 1 month. Next-generation sequencing, biodistribution and tumorigenicity assays establish a favorable safety profile at 1-9 months. Single cell transcriptomics reveals that iSCs are composed of the major skin cell lineages and include prominent holoclone stem cell-like signatures of keratinocytes, and the recently described Gibbin-dependent signature of fibroblasts. The latter correlates with enhanced graftability of iSCs. In conclusion, DEBCT overcomes manufacturing and safety roadblocks and establishes a reproducible, safe, and cGMP-compatible therapeutic approach to heal lesions of DEB patients. Dystrophic Epidermolysis Bullosa is an uncurable monogenetic skin disease. Here, Neumayer et al. develop a cGMP-compatible CRISPR- and iPS cell-based approach that produces gene-corrected, autologous skin composite grafts for definitive treatment. [ABSTRACT FROM AUTHOR]

Published

2024

6. Advances in Treatments for Epidermolysis Bullosa (EB): Emphasis on Stem Cell-Based Therapy.

Author

Raoufinia, Ramin, Rahimi, Hamid reza, Keyhanvar, Neda, Moghbeli, Meysam, Abdyazdani, Nima, Rostami, Mehdi, Naghipoor, Karim, Forouzanfar, Fatemeh, Foroudi, Sara, and Saburi, Ehsan

Subjects

*STEM cell treatment, *EPIDERMOLYSIS bullosa, *THERAPEUTICS, *GENE therapy, *PAIN management

Abstract

Epidermolysis bullosa (EB) is a rare genetic dermatosis characterized by skin fragility and blister formation. With a wide phenotypic spectrum and potential extracutaneous manifestations, EB poses significant morbidity and mortality risks. Currently classified into four main subtypes based on the level of skin cleavage, EB is caused by genetic mutations affecting proteins crucial for maintaining skin integrity. The management of EB primarily focuses on preventing complications and treating symptoms through wound care, pain management, and other supportive measures. However, recent advancements in the fields of stem cell therapy, tissue engineering, and gene therapy have shown promise as potential treatments for EB. Stem cells capable of differentiating into skin cells, have demonstrated positive outcomes in preclinical and early clinical trials by promoting wound healing and reducing inflammation. Gene therapy, on the other hand, aims to correct the underlying genetic defects responsible for EB by introducing functional copies of mutated genes or modifying existing genes to restore protein function. Particularly for severe subtypes like Recessive Dystrophic Epidermolysis Bullosa (RDEB), gene therapy holds significant potential. This review aims to evaluate the role of new therapeutic approaches in the treatment of EB. The review includes findings from studies conducted on humans. While early studies and clinical trials have shown promising results, further research and trials are necessary to establish the safety and efficacy of these innovative approaches for EB treatment. [ABSTRACT FROM AUTHOR]

Published

2024

7. Successful Treatment of Severe Pemphigus Vulgaris with Reduced Side Effects Using a Novel IVIg Preparation.

Author

Wiedenmayer, Nadine, Vollmer, Anastasia S., Winkler, Julia K., and Enk, Alexander H.

Subjects

*PEMPHIGUS vulgaris, *TREATMENT effectiveness, *INTRAVENOUS immunoglobulins, *EPIDERMOLYSIS bullosa, *MANUFACTURING processes, *AUTOANTIBODIES, *BULLOUS pemphigoid

Abstract

Pemphigus vulgaris (PV) is a rare autoimmune bullous dermatosis (AIBD) characterized by painful blistering of the skin and mucosa caused by autoantibodies that lead to loss of adhesion in the epidermis. Standard therapy for PV is corticosteroids, either alone or in combination with steroid-sparing immunosuppressants or infusions with rituximab. According to the published European guideline, high-dose intravenous immunoglobulin (IVIg) therapy with a dosage of 2 g per kg body weight distributed over 2–5 days every 4 weeks is a promising treatment option, especially for severe or refractory disease. This report describes a 73-year-old female patient with severe and recurrent disease who achieved stabilization with IVIg treatment. However, the patient experienced side effects such as headaches, nausea, and vomiting, which affected daily life. Hence, she was transitioned to a new IVIg preparation with a new manufacturing process, resulting in fewer side effects and an improved quality of life. Further follow-up is necessary to fully evaluate the effectiveness and tolerability of this new IVIg product. [ABSTRACT FROM AUTHOR]

Published

2024

8. The Need of Differential Diagnosis Between Vulvar Lichen Sclerosus and Autoimmune Dermatoses in Adolescent Girls.

Author

Dulska, Agnieszka, Bodziony, Jakub, Janik, Marta, and Drosdzol-Cop, Agnieszka

Subjects

*VULVAR diseases, *LICHEN sclerosus et atrophicus, *MEDICAL care, *MEDICAL personnel, *TEENAGE girls, *SKIN diseases, *EPIDERMOLYSIS bullosa

Abstract

Introduction: Vulvar lichen sclerosus (VLS) is a chronic inflammatory condition affecting the anogenital region, which can manifest in prepubertal or adolescent patients. The prevailing theories point to autoimmune and genetic factors. The primary symptoms of VLS typically include vulvar itching, discomfort, dysuria, and constipation. Physical examination often reveals a characteristic figure 8 pattern, involving the labia minora, clitoral hood, and perianal region. However, these symptoms and the age of onset are nonspecific and require differentiation from autoimmune dermatoses such as bullous diseases, pemphigus diseases, epidermolysis bullosa acquisita, and dermatitis herpetiformis. We performed this study to distinguish VLS from autoimmune dermatoses, and in doing so, uncover the underlying causes of chronic vulvar changes. This knowledge will enable healthcare providers to offer appropriate medical care to affected patients. Methods: The study was conducted between July 2020 and February 2021, with a sample of 55 girls aged 2–18 years who did not have any systemic diseases. The study group was composed of 20 girls previously diagnosed with vulvar lichen sclerosus, while the control group included 35 girls without VLS. Questionnaires regarding the medical history of the children were completed by their legal guardians. Blood samples were collected and analyzed biochemically to assess human immunoglobulin A (IgA), IgG, and IgM antibodies against various substrates, including the desmosome of stratum spinosum, basement membrane zone, desmoglein 1 (DSG1), desmoglein 3 (DSG3), BP180-NC16A-4X, BP230gC, pemphigoid antigen, collagen type VII NC1, transitional epithelium, gliadin (GAF-3X), endomysium (EMA), and cellular nucleus (ANA). Results: The analysis of the study group revealed that the most commonly observed signs and symptoms included: itching, soreness, burning sensations, and excoriation, as well as erythema or/and pallor of the skin and perineal mucosa. Among the assessed antibodies, only anti-GAF3x antibodies and ANA antibodies were detected. However, the results did not reach statistical significance (p > 0.5). [ABSTRACT FROM AUTHOR]

Published

2024

9. Oleogel-S10 in Dystrophic Epidermolysis Bullosa: A Case Series Evaluating the Impact on Wound Burden Over Two Years.

Author

Torres Pradilla, Mauricio, Álvarez, Erick, Novoa, Mónica, Lozano, Ivonne, and Trujillo, Maribel

Abstract

Epidermolysis bullosa (EB) is a group of rare, difficult-to-treat, inherited multisystem diseases affecting epithelial integrity. Impaired wound healing is central and can lead to serious clinical complications, deformities, and symptoms with a devastating impact on quality of life (QoL). Dressing changes and wound care are central to the management of EB. Recently Oleogel-S10 (also known as birch bark extract or birch triterpenes) was approved in Europe and the UK for treating EB wounds. This approval was based on data from the EASE phase 3 study, which demonstrated Oleogel-S10 accelerated wound healing, reduced total wound burden, and decreased the frequency of dressing changes in patients with EB. A retrospective analysis of medical records was conducted for up to 24 months in 13 patients with EB treated with Oleogel-S10 through an early access programme in Colombia. Effectiveness was assessed by measuring body surface area percentage (BSAP) and total body wound burden (EBDASI). Tolerability and safety were monitored throughout. This is the first report to evaluate the effectiveness of Oleogel-S10 in clinical practice. The results showed a reduction in percentage of BSA affected, from a mean of 27.3% at baseline to 10.4% at 24-month follow-up, despite treatment interruptions. A reduction in EBDASI skin activity score of − 16.2 (24 months) together with a reduced skin damage index score of − 15.4 (18 months) was also observed. Physicians, patients, and caregivers perceived faster wound closure. Adherence with therapy by patients was good, and patients expressed satisfaction with treatment and reported improvements in self-esteem, productivity, and social interaction. Oleogel-S10 was well tolerated; however, two patients reported worsening wounds related to gauze adherence. Two deaths during treatment interruption were reported and was not considered related to Oleogel-S10. This study supports the effectiveness of Oleogel-S10 in a real-world scenario in a country with scarce resources for the treatment of EB. [ABSTRACT FROM AUTHOR]

Published

2024

10. Roles of dystonin isoforms in the maintenance of neural, muscle, and cutaneous tissues.

Author

Yoshioka, Nozomu

Subjects

*BULLOUS pemphigoid, *EPIDERMOLYSIS bullosa, *CYTOSKELETAL proteins, *TISSUES, *FAMILIAL spastic paraplegia

Abstract

Dystonin (DST), also known as bullous pemphigoid antigen 1 (BPAG1), encodes cytoskeletal linker proteins belonging to the plakin family. The DST gene produces several isoforms, including DST-a, DST-b, and DST-e, which are expressed in neural, muscle, and cutaneous tissues, respectively. Pathogenic DST mutations cause hereditary sensory and autonomic neuropathy type 6 (HSAN-VI) and epidermolysis bullosa simplex (EBS); therefore, it is important to elucidate the roles of DST isoforms in multiple organs. Recently, we have used several Dst mutant mouse strains, in which the expression of Dst isoforms is disrupted in distinct patterns, to gain new insight into how DST functions in multiple tissues. This review provides an overview of the roles played by tissue-specific DST isoforms in neural, muscle, and cutaneous tissues. [ABSTRACT FROM AUTHOR]

Published

2024

11. Recessive dystrophic epidermolysis bullosa caused by a novel COL7A1 variant with isodisomy.

Author

Niida, Yo, Kobayashi, Azusa, Togi, Sumihito, and Ura, Hiroki

Subjects

EPIDERMOLYSIS bullosa, SINGLE nucleotide polymorphisms, GENETIC variation, GENETIC disorders

Abstract

Recessive dystrophic epidermolysis bullosa is a genetic collagen disorder characterized by skin fragility that leads to generalized severe blistering, wounds, and scarring. In this report, we present a patient with a novel COL7A1 homozygous nonsense variant, c.793C>T p.(Gln265*). Although the parents were not consanguineous, both were heterozygous carriers of the variant. Single nucleotide polymorphism (SNP) array analysis revealed an isodisomy area on 3p22.1p21.1, encompassing COL7A1, suggesting that the variant originated from a common ancestor. [ABSTRACT FROM AUTHOR]

Published

2023

12. Birch Bark Extract: A Review in Epidermolysis Bullosa.

Author

Heo, Young-A

Subjects

*WOUND healing, *DRUG efficacy, *DRUG approval, *SUNFLOWER seed oil, *DRUG tolerance, *TRITERPENES, *TREATMENT effectiveness, *BARK, *PHARMACEUTICAL gels, *EPIDERMOLYSIS bullosa, *PLANT extracts, *CUTANEOUS therapeutics, *RARE diseases, *WOUND care, *PATIENT safety, *EVALUATION, *CHILDREN

Abstract

Birch bark extract (Filsuvez®; also known as the developmental name Oleogel-S10), a topical gel consisting of 10% dry birch bark extract and 90% sunflower oil, is the first therapy approved in the EU and UK for the treatment of partial thickness wounds associated with dystrophic and junctional epidermolysis bullosa (EB) in patients aged ≥ 6 months old. In the pivotal double-blind, randomized, vehicle-controlled, phase III EASE trial in patients with EB, the primary endpoint was met, in which birch bark extract relative to control gel significantly increased the proportion of patients with first complete target wound closure within 45 days. Moreover, patients treated with birch bark extract demonstrated several other positive findings in improving wound burden and wound-associated symptoms. The clinical benefits of birch bark extract were maintained in the 24-month open-label extension period of the EASE trial. Birch bark extract was generally well tolerated in patients with EB, with the tolerability profile being similar to that of control gel. Current evidence indicates that birch bark extract is an effective, emerging treatment option for patients with dystrophic and junctional EB. Plain Language Summary: Epidermolysis bullosa (EB) is a rare, heterogenous genetic disorder characterized by extreme skin fragility and trauma-induced blister formation of the skin, mucosa or internal epithelial linings of organs. Due to lack of disease-modifying therapies, the mainstay treatment options for EB remain supportive in nature, such as wound care, skin protection, itch and pain management, infection control and trauma prevention. With various therapies being investigated as a potential treatment option for EB, birch bark extract (Filsuvez®; also known as the developmental name Oleogel-S10) topical gel has been approved in the EU and UK for the treatment of partial thickness wounds associated with dystrophic and junctional EB in patients aged ≥ 6 months old. Birch bark extract has demonstrated anti-inflammatory, antibacterial, antiviral, antimycotic and wound-healing properties. In patients with EB, birch bark extract relative to control gel significantly accelerated wound healing within 45 days, together with other positive findings in improving wound burden and wound-associated symptoms. The clinical benefits of birch bark extract in improving wound burden were maintained for up to 24 months of continued treatment. Birch bark extract was generally well tolerated in patients with EB, with most adverse events being mild to moderate in severity. Current evidence indicates that birch bark extract is an effective, emerging treatment option for patients with dystrophic and junctional EB. [ABSTRACT FROM AUTHOR]

Published

2023

13. Esophageal dilation with EsoFLIP is faster than CRE balloon dilation combined with EndoFLIP in children.

Author

Hoskins, Brett, Almazan, Erik, Hohl, Brenna, and Ng, Kenneth

Subjects

*EOSINOPHILIC esophagitis, *TIME dilation, *EPIDERMOLYSIS bullosa, *RACE, *FLUOROSCOPY, *CHILD patients

Abstract

Background: Controlled radial expansion (CRE) balloon dilators are traditionally used to dilate esophageal strictures during an esophagogastroduodenoscopy (EGD). EndoFLIP is a diagnostic tool used during an EGD to measure important parameters of the gastrointestinal lumen, capable of assessing treatment before and after dilation. EsoFLIP is a related device that combines a balloon dilator with high-resolution impedance planimetry to provide some of the luminal parameters in real time during dilation. We sought to compare procedure time, fluoroscopy time, and safety profile of esophageal dilation using either CRE balloon dilation combined with EndoFLIP (E + CRE) versus EsoFLIP alone. Methods: A single-center retrospective review was performed to identify patients ≤ 21 years of age who underwent an EGD with biopsy and esophageal stricture dilation using E + CRE or EsoFLIP between October 2017 and May 2022. Results: Twenty-nine EGDs with esophageal stricture dilation were performed in 23 patients (19 E + CRE and 10 EsoFLIP). The two groups did not differ in age, gender, race, chief complaint, type of esophageal stricture, or history of prior gastrointestinal procedures (all p > 0.05). The most common medical history in the E + CRE and EsoFLIP groups were eosinophilic esophagitis and epidermolysis bullosa, respectively. Median procedures times were shorter in the EsoFLIP cohort compared to E + CRE balloon dilation (40.5 min [IQR 23–57 min] for the EsoFLIP group; 64 min [IQR 51–77 min] for the E + CRE group; p < 0.01). Median fluoroscopy times were also shorter for patients who underwent EsoFLIP (0.16 min [IQR 0–0.30 min] for EsoFLIP dilation; 0.30 min [IQR 0.23–0.55] for the E + CRE group; p = 0.003). There were no complications or unplanned hospitalizations in either group. Conclusion: EsoFLIP dilation of esophageal strictures was faster and required less fluoroscopy than CRE balloon dilation combined with EndoFLIP in children, while being equally as safe. Prospective studies are needed to further compare the two modalities. [ABSTRACT FROM AUTHOR]

Published

2023

14. Beremagene Geperpavec: First Approval.

Author

Dhillon, Sohita

Subjects

*BIOTHERAPY, *DRUG approval, *BIOLOGICAL products, *GENE therapy, *EPIDERMOLYSIS bullosa, *DRUG development, *CUTANEOUS therapeutics, *WOUND care

Abstract

Beremagene geperpavec-svdt (VYJUVEK™) is a topically applied, redosable, live, replication defective herpes simplex virus-1 (HSV-1) vector -based gene therapy that is being developed by Krystal Biotech to deliver functional human collagen type VII alpha 1 chain (COL7A1) genes in patients with both, dominant and recessive dystrophic epidermolysis bullosa. Beremagene geperpavec can transduce both keratinocytes and fibroblasts and restore functional COL7 protein. In May 2023, beremagene geperpavec received its first approval in the US for the treatment of wounds in patients ≥ 6 months of age with dystrophic epidermolysis bullosa with mutation(s) in the COL7A1 gene. A Marketing Authorization Application for beremagene geperpavec in Europe is planned for the second half of 2023. This article summarizes the milestones in the development of beremagene geperpavec leading to this first approval for dystrophic epidermolysis bullosa. [ABSTRACT FROM AUTHOR]

Published

2023

15. Epidermolysis bullosa in oral health: clinical manifestations and salivary alterations.

Author

de Azevedo, Brenda Lamônica Rodrigues, Roni, Gabriel Marim, Dettogni, Raquel Spinassé, Torrelio, Rosalie Matuk Fuentes, Leal, Lucas Fernandes, and da Gama-de-Souza, Letícia Nogueira

Subjects

*SYMPTOMS, *ORAL mucosa, *EPIDERMOLYSIS bullosa, *ORAL manifestations of general diseases, *MUCOUS membranes, *GENETIC disorders

Abstract

Epidermolysis bullosa (EB) is an inherited disease characterized by the fragility of the skin and mucous membranes. All types/subtypes of EB can lead to alterations in the mouth and glands. Objective: To evaluate clinical manifestations of EB on the oral mucosa and alterations in salivary flow. Materials and methods: Sociodemographic and clinical data were obtained from EB individuals. The salivary flow analysis was performed in EB and in non-EB patients. Fischer's exact test was applied to the qualitative variables, and the Mann–Whitney test was applied to the quantitative data. Results: A total of 11 cases of EB were evaluated, and 3 types of EB were diagnosed (recessive dystrophic—RDEB; junctional—JEB; and simplex—EBS). Only individuals with RDEB or JEB showed the oral manifestation of the disease. The most affected sites were the lips (54%), hard palate (36%), and oral mucosa (27%). Ulcer and ankyloglossia were diagnosed in all RDEB cases. Regarding salivary flow, an intragroup comparison revealed an increase in stimulated versus unstimulated collection in the control sample (p = 0.0064). The EB group showed no difference (p = 0.6086). We also observed no differences in salivary volume between the control and EB groups (p = 0.7117 and p = 0.5557, unstimulated and stimulated flows, respectively). Conclusions: No oral manifestations were observed in EBS subjects. It is unclear whether individuals with EB are predisposed to manifest hyposalivation. Clinical relevance: Severe cases of EB show broad alterations in the oral mucosa, whereas the saliva needs to be better evaluated. [ABSTRACT FROM AUTHOR]

Published

2023

16. Characterization of novel therapies for epidermolysis bullosa in clinical development: a cross-sectional analysis.

Author

Sandoval, Aaron Gabriel W., Kempinski, Heidi, Hartman, Shelley, and Badiavas, Evangelos V.

Published

2024

17. Targeting Multiple Hallmarks of Skin Aging: Preclinical and Clinical Efficacy of a Novel Growth Factor-Based Skin Care Serum.

Author

Naughton, Gail K., Jiang, Lily I., Makino, Elizabeth T., Chung, Robin, Nguyen, Audrey, Cheng, Tsing, Kadoya, Kuniko, and Mehta, Rahul C.

Subjects

*SKIN aging, *SKIN care, *CELLULAR aging, *SKIN regeneration, *CELL communication, *GENE expression, *PRESBYCUSIS, *EPIDERMOLYSIS bullosa

Abstract

Introduction: The aging process involves numerous biological mechanisms that have been characterized and proposed as the "hallmarks of aging." Targeting the processes and pathways related to these hallmarks of aging that cause and promote skin aging could provide anti-aging benefits. A novel topical growth factor-based skin care serum (A+) was developed using human fibroblast conditioned media. This study aimed to assess the effects of A+ on four hallmarks of aging and its clinical efficacy in skin rejuvenation in subjects with moderate to severe overall facial photodamage. Methods: Preclinical studies included immunohistochemistry in human ex vivo skin, and gene expression analysis in human 3D skin models. A 24-week, vehicle placebo-controlled study, including FaceQ patient-reported outcomes and skin biopsy analysis, was performed to assess clinical efficacy and tolerability. Results: Treatment with A+ resulted in reduced expression of cell senescence biomarker H2A.J and upregulation of genes associated with proteasome, autophagy, stemness, and intercellular communication. Clinical assessments showed A+ provided significantly greater reductions in sagging, coarse lines/wrinkles, fine lines/wrinkles, overall photodamage, and overall hyperpigmentation compared with placebo. Subjects felt they appeared younger-looking, reporting a median decrease in self-perceived age of 6 years after 12 weeks of use. Decreased levels of H2A.J and increased expression of key dermal extracellular matrix and epidermal barrier components, including collagen and elastin, were observed in skin biopsy samples. Conclusion: The present study shows for the first time the potential effects of a topical growth factor-based cosmeceutical on cellular processes related to four hallmarks of aging (cellular senescence, loss of proteostasis, stem cell exhaustion, and altered intercellular communication) to help delay the aging process and restore aged skin. A+ targets the biological mechanisms underlying the aging process itself and stimulates skin regeneration, resulting in rapid and significant clinical improvements. [ABSTRACT FROM AUTHOR]

Published

2023

18. Harnessing the Anti-Inflammatory Effects of Perinatal Tissue Derived Therapies for the Treatment of Inflammatory Skin Diseases: A Comprehensive Review.

Author

Khalilzad, Mohammad Amin, Mohammadi, Javad, Najafi, Sajad, Amirsaadat, Soumaye, Zare, Sona, Khalilzad, Mitra, Shamloo, Amir, Khaghani, Ayoub, Peyrovan, Aysan, Khalili, Seyedeh Fatemeh Sadati, Fayyaz, Negin, and Zare, Solmaz

Subjects

*EPIDERMOLYSIS bullosa, *SKIN diseases, *SKIN inflammation, *ATOPIC dermatitis, *PEMPHIGUS

Abstract

Dealing with chronic inflammatory skin conditions like atopic dermatitis and psoriasis can be extremely difficult. Current treatments, such as topical corticosteroids, often have limitations and side effects. However, researchers have discovered that the placenta’s remarkable properties may provide a breakthrough in effectively addressing these skin conditions. The placenta comprises three essential tissues: decidua, placental membrane, and umbilical cord. Placental derivatives have shown significant potential in treating psoriasis by reducing inflammatory cytokines and inhibiting keratinocyte proliferation. In the case of atopic dermatitis, umbilical cord stem cells have demonstrated anti-inflammatory effects by targeting critical factors and promoting anti-inflammatory cytokines. The scope of benefits associated with placental derivatives transcends these specific applications. They also potentially address other inflammatory skin diseases, such as vitiligo, by stimulating melanin production. Moreover, these derivatives have been leveraged in the treatment of pemphigus and epidermolysis bullosa (EB), showcasing potential as a wound dressing that could eliminate the necessity for painful dressing changes in EB patients. In summary, the integration of placental derivatives stands to revolutionize our approach to inflammatory skin conditions owing to their distinct properties and the prospective benefits they offer. This comprehensive review delves into the current applications of placental derivatives in addressing inflammatory skin diseases, presenting a novel treatment approach.Graphical Abstract: Dealing with chronic inflammatory skin conditions like atopic dermatitis and psoriasis can be extremely difficult. Current treatments, such as topical corticosteroids, often have limitations and side effects. However, researchers have discovered that the placenta’s remarkable properties may provide a breakthrough in effectively addressing these skin conditions. The placenta comprises three essential tissues: decidua, placental membrane, and umbilical cord. Placental derivatives have shown significant potential in treating psoriasis by reducing inflammatory cytokines and inhibiting keratinocyte proliferation. In the case of atopic dermatitis, umbilical cord stem cells have demonstrated anti-inflammatory effects by targeting critical factors and promoting anti-inflammatory cytokines. The scope of benefits associated with placental derivatives transcends these specific applications. They also potentially address other inflammatory skin diseases, such as vitiligo, by stimulating melanin production. Moreover, these derivatives have been leveraged in the treatment of pemphigus and epidermolysis bullosa (EB), showcasing potential as a wound dressing that could eliminate the necessity for painful dressing changes in EB patients. In summary, the integration of placental derivatives stands to revolutionize our approach to inflammatory skin conditions owing to their distinct properties and the prospective benefits they offer. This comprehensive review delves into the current applications of placental derivatives in addressing inflammatory skin diseases, presenting a novel treatment approach. [ABSTRACT FROM AUTHOR]

Published

2024

19. The 25th World Congress of Dermatology, Singapore, 3–8 July, 2023: Research Highlights.

Author

Fraser, Kathy A.

Subjects

*THERAPEUTIC use of monoclonal antibodies, *PSORIASIS, *ALOPECIA areata, *DRUG efficacy, *TRITERPENES, *CONFERENCES & conventions, *JANUS kinases, *ATOPIC dermatitis, *NEUROTRANSMITTER uptake inhibitors, *EPIDERMOLYSIS bullosa, *PEPTIDES, *PATIENT safety, *CHEMICAL inhibitors

Abstract

The article provides an overview of the recent World Congress of Dermatology held in Singapore with the theme "Dermatology Beyond Borders.It mentions the notable studies discussed at the congress include the results of clinical trials for novel treatments for psoriasis, atopic dermatitis, and alopecia areata, showcasing advancements in dermatological research and potential treatment options.

Published

2023

20. Genome Editing in Therapy of Genodermatoses.

Author

Ivanenko, A. V., Evtushenko, N. A., and Gurskaya, N. G.

Subjects

*GENOME editing, *ANIMAL disease models, *EPIDERMOLYSIS bullosa, *DNA repair, *GENETIC disorders, *NUCLEASES

Abstract

This review is devoted to the prospects for the use of fundamentally important approaches and methods for the correction and therapy of genodermatoses, a group of inherited skin diseases. The greatest number of methods was applicable for the group of inherited epidermolysis bullosa. Gene replacement using viral and non-viral methods of delivery to cells has been replaced by genome editing using programmable nucleases used both in vitro and in vivo. The focus is on more widely used methods applied in vitro to various cell types. The description of the methods used is classified based on the use of DNA break repair pathways: the canonical non-homologous end-reconnection pathway—cNHEJ, and directed homologous recombination—HDR. The choice of editing strategy depends on the type of mutation causing the disease, the type of mutation inheritance, and the nucleotide environment of the mutation. Animal disease models obtained by genome editing are considered. The experience of developing methods for editing the genome and their application for the treatment of genodermatoses, previously recognized as incurable, is summarized. [ABSTRACT FROM AUTHOR]

Published

2022

21. First Report of Symmetrical Drug-related Intertriginous and Flexural Exanthema (SDRIFE or Baboon Syndrome) After Erenumab Application for Migraine Prevention.

Author

Göbel, Carl H., Heinze, Axel, Karstedt, Sarah, Cirkel, Anna, Münte, Thomas F., and Göbel, Hartmut

Subjects

*ERENUMAB, *EXANTHEMA, *MIGRAINE, *BABOONS, *MONOCLONAL antibodies, *EPIDERMOLYSIS bullosa

Abstract

Introduction: Symmetrical drug-related intertriginous and flexural exanthema (SDRIFE), formerly also called baboon syndrome, is characterized by symmetrical erythematous rash with typical localization in the gluteal and intertriginous areas. A type IV delayed hypersensitivity immune response is thought to be responsible for its development. CGRP monoclonal antibodies (CGRP mAbs) are a new class of drugs for the prevention of migraine. We present the first case of SDRIFE occurring in temporal relation to the use of erenumab for migraine prevention. Case: A 48-year-old female patient with migraine received erenumab 140 mg subcutaneously in the thigh area for the prevention of migraine in repetitive cycles, each 1 month apart. Initially, the patient experienced no side effects. After the third cycle, a masseuse incidentally noticed a reddish, circular rash in the buttock area during a back massage. There were no other symptoms. The skin changes resolved spontaneously. Two years later, approximately 40 h after reapplication of erenumab 140 mg, the patient experienced a severe pain in the buttock area centered over the anal crease. The area of pain extended in a circular pattern with approximately 20 cm in diameter. The pain started abruptly and reached a severe intensity within about 30 min. Sitting on the buttocks was no longer possible for the patient. There was marked allodynia and hyperpathia in the entire buttocks region. A flat, broad-based blister-like skin swelling developed in this region. The blisters began opening up on the fourth day after the onset of the skin reaction. In addition, there was a pronounced redness in the entire buttock area. Here, the patient felt a strong burning pain, similar to a scald. Results: The symptoms lasted for a period of 10 days. From this point on, they fully subsided under concomitant therapy with prednisolone. Conclusion: SDRIFE as a rare dermatological side effect should be considered in the monitoring of skin lesions during migraine prophylaxis. In view of the high migraine prevalence, knowledge of this uncommon syndrome is important. It is crucial to recognize the relationship between the medication and the circumscribed exanthema occurring distant from the injection site. [ABSTRACT FROM AUTHOR]

Published

2022

22. Epidermolysis Bullosa: A Review of the Tissue-Engineered Skin Substitutes Used to Treat Wounds.

Author

du Rand, Alex, Hunt, John M. T., Feisst, Vaughan, and Sheppard, Hilary M.

Subjects

*EPIDERMOLYSIS bullosa, *WOUND healing, *SKIN injuries, *WOUNDS & injuries, *INVESTIGATIONAL therapies

Abstract

Skin wound healing is a crucial process for regenerating healthy skin and avoiding the undesired consequences associated with open skin wounds. For epidermolysis bullosa (EB), a debilitating group of fragile skin disorders currently without a cure, skin blistering can often be severe and heal poorly, increasing susceptibility to life-threatening complications. To prevent these, investigational therapies have been exploring the use of tissue-engineered skin substitutes (TESSs) aimed at replacing damaged skin and promoting long-term wound closure. These products have either been developed in house or commercially sourced and are composed of allogeneic or autologous human skin cells, often with some form of bioscaffolding. They can be broadly classified based on their cellular composition: keratinocytes (epidermal substitutes), fibroblasts (dermal substitutes) or a combination of both (composite substitutes). Encouraging long-term wound healing has been achieved with epidermal substitutes. However, these substitutes have not demonstrated the same efficacy for all patients, which may be due to the molecular heterogeneity observed between EB subtypes. Autologous composite TESSs, which more closely resemble native human skin, are therefore being investigated and may hold promise for treating an extended range of patients. Additionally, future TESSs for EB are focused on using gene-corrected patient skin cells, which have already demonstrated remarkable long-term wound healing capabilities. In this review, we provide an overview of the different TESSs that have been investigated in clinical studies to treat patients with EB, as well as their long-term wound healing results. Where available, we describe the methods used to develop these products to inform future efforts in this field. [ABSTRACT FROM AUTHOR]

Published

2022

23. Novel variants in LAMA3 and COL7A1 and recurrent variant in KRT5 underlying epidermolysis bullosa in five Chinese families.

Author

Wang, Rongrong, Sun, Liwei, Habulieti, Xiaerbati, Liu, Jiawei, Guo, Kexin, Yang, Xueting, Ma, Donglai, and Zhang, Xue

Abstract

Epidermolysis bullosa (EB) is a group of clinically and genetically heterogeneous diseases characterized by trauma-induced mucocutaneous fragility and blister formation. Here, we investigated five Chinese families with EB, and eight variants including a novel nonsense variant (c.47G>A, p.W16*) in LAMA3, a known recurrent variant (c.74C>T, p.P25L) in KRT5, 2 novel (c.2531T>A, p.V844E; c.6811_6814del, p.R2271fs) and 4 known (c.6187C>T, p.R2063W; c.7097G>A, p.G2366D; c.8569G>T, p.E2857*; c.3625_3635del, p.S1209fs) variants in COL7A1 were detected. Notably, this study identified a nonsense variant in LAMA3 that causes EB within the Chinese population and revealed that this variant resulted in a reduction in LAMA3 mRNA and protein expression levels by nonsense-mediated mRNA decay. Our study expands the mutation spectra of Chinese patients with EB. [ABSTRACT FROM AUTHOR]

Published

2022

24. Eye Involvement and Management in Inherited Epidermolysis Bullosa.

Author

Bachir, Yasmine, Daruich, Alejandra, Marie, Couanon, Robert, Matthieu P., and Bremond-Gignac, Dominique

Subjects

*THERAPEUTICS, *OCULAR manifestations of general diseases, *CORNEA diseases, *GENE therapy, *HEALTH care teams, *EPIDERMOLYSIS bullosa, *DISEASE management, *DIFFUSION of innovations

Abstract

Inherited epidermolysis bullosa (EB) is a group of genetic rare diseases associated with skin fragility, which leads to the formation of blisters, erosions, and scars on the skin and mucous membranes. Epidermolysis bullosa includes four main types and some several clinical subtypes including EB simplex, junctional EB, dystrophic EB, and Kindler's EB. Ocular involvement ranged from 51 to 68% in EB and can cause irreversible damages if not properly managed. Corneal erosions are the most common finding among series, including our cohort. We review here clinical and pathological features of ocular involvement in EB and the main keys for management, with a focus on recent innovative therapies. [ABSTRACT FROM AUTHOR]

Published

2022

25. Aprepitant: Drug ineffective: 2 case reports.

Subjects

*EPIDERMOLYSIS bullosa, *QUALITY of life, *CONGENITAL disorders, *HUMAN abnormalities, *DRUGS, *ITCHING

Abstract

The article in Reactions Weekly discusses two case reports of children with epidermolysis bullosa (EB) who showed drug ineffectiveness while being treated with aprepitant for associated pruritus. A 13-month-old boy and a 7-year-old boy were prescribed aprepitant monthly for their refractory pruritus, but after several months of treatment, no improvement was noted in their quality of life or reduction in itching, leading to the discontinuation of aprepitant. The study highlights the challenges in managing EB-associated pruritus and the need for further research on effective treatment options. [Extracted from the article]

Published

2024

26. Nephrotic syndrome, skin involvement, and chronic lung disease: Answers.

Author

Atmis, Bahriye, Cevizli, Derya, Cagli, Cagla, Saribas, Emel, Karakulak, Veysel, Ozcan, Dilek, Gok, Beyza Irem, Erdogan, Kivilcim Eren, Gonlusen, Gulfiliz, and Bayazit, Aysun K.

Subjects

*BIOPSY, *PATHOGENESIS, *GENETIC mutation, *SEQUENCE analysis, *NEPHROTIC syndrome, *STEROIDS, *MICROSCOPY, *INTERSTITIAL lung diseases, *DRUG resistance, *RISK assessment, *EPIDERMOLYSIS bullosa, *DISEASE risk factors, *CHILDREN

Abstract

The article presents the discussion on nephrotic syndrome, skin involvement, and chronic lung disease. Topics include diagnostic approach to the steroid-resistant nephrotic syndrome in children with extrarenal fndings; and light microscopy of the biopsy showing focal segmental glomerulosclerosis, mononuclear cell infltration .

Published

2023

27. A rare homozygous missense mutation of COL7A1 in a Vietnamese family.

Author

Duong, Nguyen Thuy, Anh, Luong Thi Lan, Sau, Nguyen Huu, Anh, Nguyen Bao, Miyake, Noriko, Van Hai, Nong, and Matsumoto, Naomichi

Subjects

MISSENSE mutation, VIETNAMESE people, GENETIC counseling, EPIDERMOLYSIS bullosa, PRENATAL diagnosis, GENETIC mutation

Abstract

We present a homozygous missense mutation in the COL7A1 gene (NM_000094.4: c.6262G>A, p.G2088R) in a case of inversa recessive dystrophic epidermolysis bullosa (RDEB-I) from a nonconsanguineous Vietnamese family. Although a heterozygous form of this mutation in combination with a premature termination codon allele has been shown to cause RDEB-I, this is the first report of homozygosity of this mutation as the etiology. Here, we investigated the molecular basis of the patient's disease for prenatal diagnosis after genetic counseling of the parents. [ABSTRACT FROM AUTHOR]

Published

2022

28. Apoptolysis: a less understood concept in the pathogenesis of Pemphigus Vulgaris.

Author

Ramani, Pratibha, Ravikumar, Renu, Pandiar, Deepak, Monica, K., Krishnan, Reshma Poothakulath, Ramasubramanian, Abilasha, and Sukumaran, Gheena

Subjects

PEMPHIGUS vulgaris, MUCOUS membranes, AUTOANTIBODIES, ORAL manifestations of general diseases, AUTOIMMUNE diseases, EPIDERMOLYSIS bullosa

Abstract

Pemphigus Vulgaris (PV) is a severe autoimmune disease characterized by supra-basal blisters in the skin and mucous membranes of a wide range of mammals, including humans. It not only affects the skin but also has severe oral manifestations. It has been stated that auto-antibodies are produced, for unknown reasons, which are directed against desmogleins present on the epithelium and thus leads to acantholysis and intraepithelial blistering. But the exact mechanism is still not completely understood. Here we would like to shed light on a new pathologic mechanism i.e., apoptolysis, which emphasizes that apoptotic enzymes contribute to acantholysis development both in terms of molecular events and chronologic sequence. A possible role of apoptolysis has been discussed in purview of PV. [ABSTRACT FROM AUTHOR]

Published

2022

29. Intestinal Failure in Junctional Epidermolysis Bullosa: Mild Skin Disease, Severe Diarrhea.

Author

DeMaria, Karen A., Fink, Christopher, Pepper, Michael, Rieger, Kerri, Tan, Serena Y., and Namjoshi, Shweta S.

Published

2022

30. Severe Basilar impression in osteogenesis imperfecta treated with halo gravity traction, occipitocervicothoracic fusion, foramen magnum and upper cervical decompression and expansive duroplasty: a technical note.

Author

Jannelli, Gianpaolo, Moiraghi, Alessandro, Paun, Luca, Tessitore, Enrico, Dayer, Romain, and Bartoli, Andrea

Subjects

*BASILAR invagination, *OSTEOGENESIS imperfecta, *SPINAL surgery, *CRANIOVERTEBRAL junction, *BONE diseases, *SPINAL tuberculosis, *EPIDERMOLYSIS bullosa

Abstract

Osteogenesis imperfecta (OI) is a rare bone disease due to an abnormal synthesis of 1-type collagen. OI is frequently associated with basilar impression (BI), defined by the elevation of the clivus and floor of the posterior fossa with subsequent migration of the upper cervical spine and the odontoid peg into the base of the skull. Bone intrinsic fragility leading to fractures and deformity, brainstem compression and impaired CSF circulation at cranio-vertebral junction (CVJ) makes the management of these conditions particularly challenging. Different surgical strategies, including posterior fossa decompression with or without instrumentation, transoral or endonasal decompression with posterior occipito-cervical fusion, or halo gravity traction with posterior instrumentation have been reported, but evidence about best modalities treatment is still debated. In this technical note, we present a case of a 16-years-old patient, diagnosed with OI and BI, treated with halo traction, occipito-cervico-thoracic fixation, foramen magnum and upper cervical decompression, and expansive duroplasty. We focus on technical aspects, preoperative work up and postoperative follow up. We also discuss advantages and limitations of this strategy compared to other surgical techniques. [ABSTRACT FROM AUTHOR]

Published

2022

31. Long-Term Follow-Up Outcomes of 19 Patients with Osteogenesis Imperfecta Type XI and Bruck Syndrome Type I Caused by FKBP10 Variants.

Author

Yüksel Ülker, Aylin, Uludağ Alkaya, Dilek, Elkanova, Leyla, Şeker, Ali, Akpınar, Evren, Akarsu, Nurten Ayşe, Uyguner, Zehra Oya, and Tüysüz, Beyhan

Subjects

*OSTEOGENESIS imperfecta, *TREATMENT effectiveness, *BONE densitometry, *EPIDERMOLYSIS bullosa, *INTRAVENOUS therapy

Abstract

Osteogenesis imperfecta type XI (OI-XI) and Bruck syndrome type I (BS1) are two rare disorders caused by biallelic variants in the FKBP10, characterized by early-onset bone fractures and progressive skeletal deformities. The patients with OI-XI, also co-segregated with autosomal-recessive epidermolysis bullosa simplex caused by KRT14 variant, have been reported. In this study, the follow-up clinical features of the patients with OI-XI and BS1 phenotypes due to biallelic FKBP10 variants are compared. The aim of this study is to investigate the follow-up findings of OI-XI and BS1 phenotypes in patients with the FKBP10 variants. A total of 19 children, ten males and nine females, from 16 unrelated families were included in the study. FKBP10 variants were investigated by next-generation sequencing (NGS) based panel gene test or Sanger sequencing. Seventeen patients were followed between 1.5 and 16.8 years, and the last follow-up age was between 2 and 24.6 years (median 10.7 years). They received intravenous bisphosphonate infusions once every 3 months in follow-up period. We identified four different biallelic FKBP10 variants, two of which are novel (c.890_897dup TGATGGAC, p.Gly300Ter and c.1256 + 1G > A) in 16 families. Five of these patients also had findings of epidermolysis bullosa simplex, and the same biallelic c.612T > A (p.Tyr204Ter) variant in KRT14, as well as FKBP10, were identified. Twelve patients were diagnosed with OI-XI; whereas, seven were diagnosed with BS1. The BS1 phenotype was late-onset and the annual fracture number was lower. After bisphosphonate treatment, bone mineral densitometry Z score at L1–L4 increased (p = 0.005) and the number of annual fractures decreased (p = 0.036) in patients with OI-XI. However, no significant effect of bisphosphonate treatment was found on these values in BS1 patients. Despite the treatment, the rate of scoliosis and long bone deformity had increased in both groups at the last examination; and, only two patients could take a few steps with the aid of a walker, while others were not ambulatory, and they used wheelchairs for mobility. We identified two novel variants in FKBP10. Families originating from the same geographic region and having the same variant suggest founder effects. Although the number of fractures decreased with bisphosphonate treatment, none of our patients were able to walk during the follow-up. This study is valuable in terms of showing the follow-up findings of patients with FKBP10 variants for the first time. [ABSTRACT FROM AUTHOR]

Published

2021

32. Application of topical gentamicin—a new era in the treatment of genodermatosis.

Author

Wang, Shan, Yang, Zhou, Liu, Ying, Zhao, Mu-Tong, Zhao, Juan, Zhang, Huan, Liu, Zong-Yang, Wang, Xiao-Ling, Ma, Lin, and Yang, Yong-Hong

Abstract

Background: The clinical use of gentamicin always lies in its antimicrobial activity in the past as an aminoglycoside antibiotic. However, in the past decade, there were considerable interests in therapeutic approaches in treating hereditary diseases. Some of the genodermatosis is caused by nonsense mutations that create premature termination codons and lead to the production of truncated or non-functional proteins. Gentamicin could induce readthrough of nonsense mutations and enable the synthesis of full-length proteins. We focus on previous publications on topical application of gentamicin and review its utility in genetic skin diseases. Data sources: We search the MEDLINE through PubMed, EMBASE databases, and the Clinical Trials Registry Platform from January 1960 to July 2020 using the key search terms "gentamicin, topical gentamicin, genodermatosis, genetic skin diseases". Results: The application of gentamicin in genodermatosis yielded promising results, both in vivo and in vitro, including Nagashima-type palmoplantar keratosis, epidermolysis bullosa, Hailey–Hailey disease, hereditary hypotrichosis simplex of the scalp, etc. Conclusions: Topical gentamicin is a potential treatment option for genodermatosis caused by nonsense mutation. [ABSTRACT FROM AUTHOR]

Published

2021

33. Surgical treatment of post-infectious hydrocephalus in infants.

Author

Padayachy, L., Ford, L., Dlamini, N., and Mazwi, A.

Subjects

*HYDROCEPHALUS, *INFANTS, *NEUROSURGEONS, *THERAPEUTICS, *ETIOLOGY of diseases, *EPIDERMOLYSIS bullosa, *POST-infectious disorders

Abstract

The management of post-infective hydrocephalus in infants remains a challenging task for the pediatric neurosurgeon. The decision-making curve is often complex in that appropriate temporizing measures need to be implemented to properly clear any infection within the CSF before any decision can be made regarding a permanent solution. The etiology differs at varying stages of neonatal development, and the weight of the child, skin fragility, and relevant surgical treatment options are often important limiting factors. Deciding on the optimal treatment option involves assessing the etiology, age, and clinical and radiological features of the individual case and selecting the most appropriate surgical option. [ABSTRACT FROM AUTHOR]

Published

2021

34. Investigational Treatments for Epidermolysis Bullosa.

Author

Hou, Ping-Chen, Wang, Han-Tang, Abhee, Stasha, Tu, Wei-Ting, McGrath, John A., and Hsu, Chao-Kai

Subjects

*HUMAN abnormality genetics, *SKIN diseases, *CELLULAR therapy, *INVESTIGATIONAL drugs, *GENETIC testing, *GENETIC disorders, *MOLECULAR pathology, *DRUG design, *MEDICAL care, *PATIENTS, *BLISTERS, *GENE therapy, *QUALITY of life, *EPIDERMOLYSIS bullosa, *DRUG development, *WOUND care, *RECOMBINANT proteins, *DISEASE management, *SYMPTOMS

Abstract

Epidermolysis bullosa (EB) is a heterogeneous group of rare inherited blistering skin disorders characterized by skin fragility following minor trauma, usually present since birth. EB can be categorized into four classical subtypes, EB simplex, junctional EB, dystrophic EB and Kindler EB, distinguished on clinical features, plane of blister formation in the skin, and molecular pathology. Treatment for EB is mostly supportive, focusing on wound care and patient symptoms such as itch or pain. However, therapeutic advances have also been made in targeting the primary genetic abnormalities as well as the secondary inflammatory footprint of EB. Pre-clinical or clinical testing of gene therapies (gene replacement, gene editing, RNA-based therapy, natural gene therapy), cell-based therapies (fibroblasts, bone marrow transplantation, mesenchymal stromal cells, induced pluripotential stem cells), recombinant protein therapies, and small molecule and drug repurposing approaches, have generated new hope for better patient care. In this article, we review advances in translational research that are impacting on the quality of life for people living with different forms of EB and which offer hope for improved clinical management. [ABSTRACT FROM AUTHOR]

Published

2021

35. Review of the Latest Methods of Epidermolysis Bullosa and Other Chronic Wounds Treatment Including BIOOPA Dressing.

Author

Nita, Magdalena, Pliszczyński, Jacek, Kosieradzki, Maciej, and Fiedor, Piotr

Subjects

*EPIDERMOLYSIS bullosa, *CHRONIC wounds & injuries, *MEDICAL personnel, *BONE marrow cells, *PLURIPOTENT stem cells, *GENETIC transformation, *SKIN regeneration

Abstract

Epidermolysis bullosa (EB) is a hereditary genetic skin disorder, classified as a type of genodermatosis, which causes severe, chronic skin blisters associated with painful and potentially life-threatening complications. Currently, there is no effective therapy or cure for EB. However, over the past decade, there have been several important advances in treatment methods, which are now approaching clinical application, including gene therapy, protein replacement therapy, cell therapy (allogeneic fibroblasts, mesenchymal stromal cells), bone marrow stem cell transplant, culture/vaccination of revertant mosaic keratinocytes, gene editing/engineering, and the clinical application of inducible pluripotent stem cells. Tissue engineering scientists are developing materials that mimic the structure and natural healing process to promote skin reconstruction in the event of an incurable injury. Although a cure for EB remains elusive, recent data from animal models and preliminary human clinical trials have raised the expectations of patients, clinicians, and researchers, where modifying the disease and improving patients' quality of life are now considered attainable goals. In addition, the lessons learned from the treatment of EB may improve the treatment of other genetic diseases. [ABSTRACT FROM AUTHOR]

Published

2021

36. Dapsone/Thalidomide: Rebound effect in the form of epidermolysis bullosa acquisita relapse: case report.

Subjects

*EPIDERMOLYSIS bullosa, *DISEASE relapse, *SUBSTANCE abuse relapse, *DAPSONE, *CONGENITAL disorders, *THALIDOMIDE

Abstract

This article from Reactions Weekly discusses a case report of a 15-year-old girl with epidermolysis bullosa acquisita (EBA) who experienced a rebound effect in the form of EBA relapse after reducing her doses of dapsone and thalidomide. The girl had been receiving dapsone 150mg/day and thalidomide 75mg/day for her EBA, and had a history of a BP-like phenotype. However, when the doses of the medications were reduced, she experienced two episodes of disease relapse. This case highlights the potential for rebound effects when reducing doses of dapsone and thalidomide in EBA patients. [Extracted from the article]

Published

2024

37. Multiple drugs: Lack of efficacy: 9 case reports.

Subjects

*SPINAL muscular atrophy, *TREATMENT failure, *DRUG efficacy, *EPIDERMOLYSIS bullosa, *DEXMEDETOMIDINE, *PHENOBARBITAL, *BENZODIAZEPINES

Abstract

A case series involving nine patients (six girls and three boys) is described in this article. The patients experienced treatment failure while being treated with various medications for conditions such as insomnia, refractory dystonia, and refractory psychomotor agitation crisis. Despite receiving therapies such as melatonin, diazepam, niaprazine, and others, the treatments were not effective. Some patients received off-label intranasal dexmedetomidine as an alternative treatment. Unfortunately, several patients died, but the cause of death was not stated. [Extracted from the article]

Published

2024

38. Rituximab: Various toxicities.

Subjects

*CORONARY artery bypass, *COUGH, *COVID-19 pandemic, *COVID-19, *FEVER, *BLOOD pressure, *EPIDERMOLYSIS bullosa

Abstract

This article discusses a case series involving 15 patients who experienced various toxicities while being treated with rituximab for epidermolysis bullosa aquisita (EBA). The patients, ranging in age from approximately 29 to 64 years, developed symptoms such as sore throat, fever, cough, COVID-19 infection, urticaria, angioedema, arthralgia, edema, nausea, mild headache, blood pressure rise, and dyspnea. The article provides specific details about several patients' medical histories, previous treatments, disease durations, and responses to rituximab therapy. [Extracted from the article]

Published

2024

39. The severity of malnutrition in children with epidermolysis bullosa correlates with disease severity.

Author

Manjunath, Seema, Mahajan, Rahul, De, Dipankar, Handa, Sanjeev, Attri, Savita, Behera, Banchha Nidhi, Bhasin, Sadhna Lal, and Bolia, Rishi

Subjects

*MALNUTRITION in children, *EPIDERMOLYSIS bullosa, *DYSTROPHY, *NUTRITIONAL status, *REGRESSION analysis

Abstract

WHO defines malnutrition as severe if the z-scores are less than − 3 Standard deviation (SD), moderate if between − 2 and − 3 SD and mild if between − 2 SD to – 1 SD. This study was aimed to assess nutritional aspects of Indian children suffering from EB and to evaluate the effect of severity of EB on the severity of malnutrition. In this study, pediatric EB patients were evaluated prospectively for baseline nutritional status using anthropometric parameters and WHO growth charts, and its correlation with disease severity using instrument for Scoring Clinical Outcomes for Research of Epidermolysis Bullosa-iscorEB. In second phase, an individualized diet chart was given to meet the energy, protein and micronutrients needs and its effects were observed after 6 months. The median age of participants was 3 years (IQR-9). Of 57 patients, malnutrition was seen in 40.35% patients (22.81%-moderate and 17.54%-severe), and significantly correlated with iscorEB (r = 0.45, p < 0.0001). On bivariate regression analysis, iscorEB was independently associated with moderate-to-severe malnutrition (p = 0.047; OR 1.038, CI 1.011–1.066). iscorEB enabled the identification of patients with moderate-to-severe malnutrition with an Area Under Receiver Operating Curve (AUROC) of 0.72 (95%CI 0.58–0.85; p < 0.005). In phase 2, there was significant improvement in nutritional status in children with recessive dystrophic EB (RDEB) and dominant dystrophic EB (DDEB) subtype (p < 0.0001). The severity of malnutrition in EB children significantly correlates with disease severity, and is an independent predictor of moderate-to-severe malnutrition. [ABSTRACT FROM AUTHOR]

Published

2021

40. Clinical Perspectives of Gene-Targeted Therapies for Epidermolysis Bullosa.

Author

Welponer, Tobias, Prodinger, Christine, Pinon-Hofbauer, Josefina, Hintersteininger, Arno, Breitenbach-Koller, Hannelore, Bauer, Johann W., and Laimer, Martin

Subjects

*EPIDERMOLYSIS bullosa, *MOLECULAR biology, *PROTEIN expression, *TRANSLATIONAL research, *ORPHAN drugs, *MOLECULAR genetics, *ANIMAL models in research

Abstract

New insights into molecular genetics and pathomechanisms in epidermolysis bullosa (EB), methodological and technological advances in molecular biology as well as designated funding initiatives and facilitated approval procedures for orphan drugs have boosted translational research perspectives for this devastating disease. This is echoed by the increasing number of clinical trials assessing innovative molecular therapies in the field of EB. Despite remarkable progress, gene-corrective modalities, aimed at sustained or permanent restoration of functional protein expression, still await broad clinical availability. This also reflects the methodological and technological shortcomings of current strategies, including the translatability of certain methodologies beyond preclinical models as well as the safe, specific, efficient, feasible, sustained and cost-effective delivery of therapeutic/corrective information to target cells. This review gives an updated overview on status, prospects, challenges and limitations of current gene-targeted therapies. [ABSTRACT FROM AUTHOR]

Published

2021

41. Differential binding of human and murine IgGs to catalytic and cell wall binding domains of Staphylococcus aureus peptidoglycan hydrolases.

Author

Wang, Min, van den Berg, Sanne, Mora Hernández, Yaremit, Visser, Aafke Hinke, Vera Murguia, Elias, Koedijk, Dennis G.A.M., Bellink, Channah, Bruggen, Hilde, Bakker-Woudenberg, Irma A. J. M., van Dijl, Jan Maarten, and Buist, Girbe

Subjects

*IMMUNOGLOBULIN G, *STAPHYLOCOCCUS aureus, *PEPTIDOGLYCAN hydrolase, *EPIDERMOLYSIS bullosa, *IMMUNE response

Abstract

Staphylococcus aureus is an opportunistic pathogen causing high morbidity and mortality. Since multi-drug resistant S. aureus lineages are nowadays omnipresent, alternative tools for preventive or therapeutic interventions, like immunotherapy, are urgently needed. However, there are currently no vaccines against S. aureus. Surface-exposed and secreted proteins are regarded as potential targets for immunization against S. aureus infections. Yet, many potential staphylococcal antigens of this category do not elicit protective immune responses. To obtain a better understanding of this problem, we compared the binding of serum IgGs from healthy human volunteers, highly S. aureus-colonized patients with the genetic blistering disease epidermolysis bullosa (EB), or immunized mice to the purified S. aureus peptidoglycan hydrolases Sle1, Aly and LytM and their different domains. The results show that the most abundant serum IgGs from humans and immunized mice target the cell wall-binding domain of Sle1, and the catalytic domains of Aly and LytM. Interestingly, in a murine infection model, these particular IgGs were not protective against S. aureus bacteremia. In contrast, relatively less abundant IgGs against the catalytic domain of Sle1 and the N-terminal domains of Aly and LytM were almost exclusively detected in sera from EB patients and healthy volunteers. These latter IgGs may contribute to the protection against staphylococcal infections, as previous studies suggest that serum IgGs protect EB patients against severe S. aureus infection. Together, these observations focus attention on the use of particular protein domains for vaccination to direct potentially protective immune responses towards the most promising epitopes within staphylococcal antigens. [ABSTRACT FROM AUTHOR]

Published

2021

42. Single-keratinocyte transcriptomic analyses identify different clonal types and proliferative potential mediated by FOXM1 in human epidermal stem cells.

Author

Enzo, Elena, Secone Seconetti, Alessia, Forcato, Mattia, Tenedini, Elena, Polito, Maria Pia, Sala, Irene, Carulli, Sonia, Contin, Roberta, Peano, Clelia, Tagliafico, Enrico, Bicciato, Silvio, Bondanza, Sergio, and De Luca, Michele

Subjects

HUMAN stem cells, STEM cell culture, KERATINOCYTE differentiation, STEM cells, CHROMOSOME segregation, EPIDERMOLYSIS bullosa, REGENERATIVE medicine

Abstract

Autologous epidermal cultures restore a functional epidermis on burned patients. Transgenic epidermal grafts do so also in genetic skin diseases such as Junctional Epidermolysis Bullosa. Clinical success strictly requires an adequate number of epidermal stem cells, detected as holoclone-forming cells, which can be only partially distinguished from the other clonogenic keratinocytes and cannot be prospectively isolated. Here we report that single-cell transcriptome analysis of primary human epidermal cultures identifies categories of genes clearly distinguishing the different keratinocyte clonal types, which are hierarchically organized along a continuous, mainly linear trajectory showing that stem cells sequentially generate progenitors producing terminally differentiated cells. Holoclone-forming cells display stem cell hallmarks as genes regulating DNA repair, chromosome segregation, spindle organization and telomerase activity. Finally, we identify FOXM1 as a YAP-dependent key regulator of epidermal stem cells. These findings improve criteria for measuring stem cells in epidermal cultures, which is an essential feature of the graft. Epidermal cultures can treat skin diseases, such as Junctional Epidermolysis Bullosa, but the signature of stem cells is unclear. By single cell RNAseq analyses on human keratinocytes, the authors identify the molecular profile of holoclones and the role of FOXM1 in regulating the proliferative potential of epidermal stem cells. [ABSTRACT FROM AUTHOR]

Published

2021

43. Pathogenetic Therapy of Epidermolysis Bullosa: Current State and Prospects.

Author

Ryumina, I. I., Goryunov, K. V., Silachev, D. N., Shevtsova, Yu. A., Babenko, V. A., Marycheva, N. M., Kotalevskaya, Yu. Yu., Zubkov, V. V., and Zubkov, G. T.

Subjects

*EPIDERMOLYSIS bullosa, *MESENCHYMAL stem cells, *HEMATOPOIETIC stem cells, *MOLECULAR genetics, *GENETIC disorders, *BASAL lamina, *ORAL mucosa

Abstract

Epidermolysis bullosa is a severe hereditary disease caused by mutations in genes encoding cutaneous basement membrane proteins. These mutations lead to dermal-epidermal junction failure and, as a result, to disturbances in the morphological integrity of the skin. Clinically, it manifests in the formation of blisters on the skin or mucosa that in some cases can turn into non-healing chronic wounds, which not only impairs patient's quality of life, but also is a live-threatening condition. Now, the main approaches in the treatment of epidermolysis bullosa are symptomatic therapy and palliative care, though they are little effective and are aimed at reducing the pain, but not to complete recovery. In light of this, the development of new treatment approaches aimed at correction of genetic defects is in progress. Various methods based on genetic engineering technologies, transplantation of autologous skin cells, progenitor skin cells, as well as hematopoietic and mesenchymal stem cells are studied. This review analyzes the pathogenetic methods developed for epidermolysis bullosa treatment based on the latest achievements of molecular genetics and cellular technologies, and discusses the prospects for the use of these technologies for the therapy of epidermolysis bullosa. [ABSTRACT FROM AUTHOR]

Published

2021

44. Prenatally diagnosed congenital pyloric atresia in consecutive three siblings: a case report.

Author

Saka, Ryuta, Yamamoto, Dan, Kuroda, Seika, Ibuka, Souji, Kodama, Tasuku, and Hasegawa, Toshimichi

Subjects

FETAL ultrasonic imaging, HUMAN abnormalities, SIBLINGS, PRENATAL diagnosis, DIAGNOSIS, EPIDERMOLYSIS bullosa

Abstract

Background: Congenital pyloric atresia (CPA) is a rare gastrointestinal anomaly frequently associated with epidermolysis bullosa (EB). Although the complications of familial isolated CPA are minor, delays in diagnosis can increase the chances of morbidity. Case presentation: Three female infants born to a Japanese mother presented with CPA at birth. There was no consanguinity between the parents, and the spacing between pregnancies was 2 years in each case. All 3 siblings had a prenatal diagnosis of CPA owing to polyhydramnios and a dilated stomach, without dilatation of the rest of the gastrointestinal tract. All patients underwent reconstructive surgeries for establishing bowel continuity (Case 1, pyloromyotomy; Case 2, gastroduodenostomy in a diamond fashion; and Case 3, gastroduodenostomy in a side-to-side fashion) soon after birth. Their postoperative courses were uneventful, and they grew up healthily, without any complications. Conclusion: Fetal ultrasonography is useful for diagnosing CPA prenatally. Successful prenatal diagnosis can lead to timely intervention after birth. [ABSTRACT FROM AUTHOR]

Published

2021

45. Multiple drugs: Lack of efficacy and off-label use.

Subjects

*OFF-label use (Drugs), *DRUG efficacy, *SLEEP quality, *SLEEP interruptions, *EPIDERMOLYSIS bullosa, *ITCHING

Abstract

A 23-month-old boy with recessive dystrophic epidermolysis bullosa (DEB) experienced a lack of efficacy with hydroxyzine, dimetindene, lorazepam, and gabapentin for his condition. As a result, he received off-label treatment with dupilumab, which led to significant improvement in his symptoms, including reduced itching and improved sleep quality. After 14 months of treatment, the boy continues to show positive results with no observed side effects. [Extracted from the article]

Published

2024

46. Multiple drugs: Lack of efficacy and off-label use.

Subjects

*OFF-label use (Drugs), *DRUG efficacy, *SLEEP quality, *SLEEP interruptions, *EPIDERMOLYSIS bullosa, *ITCHING

Abstract

A 23-month-old boy with recessive dystrophic epidermolysis bullosa (DEB) experienced a lack of efficacy with hydroxyzine, dimetindene, lorazepam, and gabapentin for his condition. As a result, he received off-label treatment with dupilumab, which led to significant itch reduction and improvement in skin lesions. The boy has been undergoing treatment for 14 months and continues to show positive results without any observed side effects. [Extracted from the article]

Published

2024

47. Vitamin-E: Lack-of-efficacy.

Subjects

*BOTULINUM toxin, *CLOBETASOL, *VITAMIN E, *EPIDERMOLYSIS bullosa, *BOTULINUM A toxins, *CONTACT dermatitis, *WOUND healing

Abstract

A 51-year-old woman with localised epidermolysis bullosa simplex did not experience any improvement in her condition after being treated with vitamin-E. She had been diagnosed with the condition at the age of 3 and had been prescribed vitamin-E, but it had no effect. She later sought help from a dermatologist for recurring blisters on her palms and fingers and was diagnosed with allergic contact dermatitis. The woman also experienced difficulties with wound healing after childbirth and her children were asymptomatic. [Extracted from the article]

Published

2024

48. Allantoin/allium-cepa/heparin/Mucopolysaccharide-polysulphate: Lack of efficacy.

Subjects

*SKIN care, *EPIDERMOLYSIS bullosa, *QUALITY of life

Abstract

A 23-year-old man with dystrophic epidermolysis bullosa pruriginosa (DEB-Pr) experienced a lack of efficacy with mucopolysaccharide-polysulfate and allantoin/allium-cepa/heparin treatments. The man had a history of nodules and severe itching on his skin, and his family members also had similar symptoms. After discontinuing the ineffective treatments, the man received SC dupilumab injections every 2 weeks, which provided relief from itching and improved his quality of life. Cryotherapy was also administered to improve his skin lesions. [Extracted from the article]

Published

2024

49. Bezold–Jarisch reflex causing bradycardia and hypotension in a case of severe dystrophic cervical kyphotic deformity: a case report and review of literature.

Author

Dilip Chand Raja, Soundararajan, Rajasekaran, Shanmuganathan, Sri Vijayanand, K. S., Shetty, Ajoy Prasad, and Kanna, Rishi Mugesh

Subjects

*BRADYCARDIA, *PACEMAKER cells, *LITERATURE reviews, *CARDIAC pacemakers, *SPINAL surgery, *ADOLESCENT idiopathic scoliosis, *EPIDERMOLYSIS bullosa

Abstract

Purpose: A 17-year-old adolescent with neurofibromatosis and severe cervicothoracic deformity was identified to have thoracic inlet compression leading to bradycardia and hypotension, only during prone positioning, and we discuss its successful management. Methods: Preoperative halo-gravity traction reduced the deformity from 126° to 91°. During prone positioning, sudden onset bradycardia was followed by asystole, which disappeared immediately on turning over to supine position. Surgery was called off after two additional failed attempts of prone positioning. Results: A retrospective analysis of CT and MRI showed severe narrowing of the thoracic inlet. In this patient, the right thoracic inlet was severely narrow, and prone positioning caused a further dynamic compromise stimulating right vagal nerve. The right vagus supplies the sinoatrial node, which is the natural pacemaker of the heart, and its stimulation causes sympathetic inhibition. Bezold–Jarisch reflex is a cardio-inhibitory reflex occurring due to vagal stimulation resulting in sudden bradycardia, asystole, and hypotension. To facilitate prone positioning, the medial end of the clavicles, along with limited manubrium excision, was performed relieving the vagal compression. C2–T4 instrumented decompression followed by anterior reconstruction and cervical plating was performed. The postoperative period was uneventful, and the final deformity was 45°. Conclusion: Bezold–Jarisch Reflex as a result of narrow thoracic inlet caused by cervical kyphosis and compensatory hyperlordosis of the upper thoracic spine has never been reported. This case highlights the need to introspect into thoracic inlet morphology in severe cervicothoracic deformities. Thoracic inlet decompression is an efficient way of addressing this unique complication. [ABSTRACT FROM AUTHOR]

Published

2020

50. Über die Problematik der klinischen Entscheidungsfindung aufgrund von Fallbeschreibungen – ethische Implikationen am Beispiel eines Falls von Carmi Syndrom.

Author

Muensterer, Oliver J. and Paul, Norbert W.

Abstract

Copyright of Ethik in der Medizin is the property of Springer Nature and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2020