Your search keyword '"Haworth, K. E."' showing total 10 results

1. SPAG6 overexpression decreases the pro-apoptotic effect of daunorubicin in acute myeloid leukemia cells through the ROS/JNK MAPK axis in a GSTP1-dependent manner.

Author

Luo, Jie, Ding, Li, Pan, Shirui, Luo, Jing, Zhao, Haiqiu, Yin, Jiaxiu, Su, Rong, Zhang, Jiamin, and Liu, Lin

Abstract

Introduction: As a malignant hematological disease, the incidence of acute myeloid leukemia (AML) has exhibited an upward trend in recent years. Nevertheless, certain limitations persist in the treatment of AML. Sperm-associated antigen 6 (SPAG6) has been implicated in the onset and progression of various human cancers, with its expression levels significantly elevated in AML. Consequently, we undertook a series of experiments to investigate the role and underlying mechanisms of SPAG6 in AML cell lines. Methods: In the in vitro experiments of this study, DEPs and GO and KEGG enrichment analysis subsequent to SPAG6 down-regulation were detected by TMT. CCK8 was employed to determine cell viability. The levels of apoptosis and ROS were measured by flow cytometry. In the in vivo experiments, a xenografted tumor model was constructed, and the expression of SPAG6 and GSTP1 in tumor tissues was detected by IHC. Results: Ultimately, our findings indicated that over-expression of SPAG6 promoted cell growth and decreased reactive oxygen species (ROS) and malondialdehyde levels. Furthermore, SPAG6 knockdown was found to diminish mitochondrial membrane potential and facilitate cell apoptosis. In vivo , SPAG6 could also promote tumor growth, suggesting that SPAG6 may serve as a pro-tumor factor. In addition, daunorubicin (DNR) may cause oxidative stress and initiate apoptosis, resulting in oxidative damage to AML cells. However, the overexpression of SPAG6 may attenuate the efficacy of DNR. This was due to SPAG6 promoted GSTP1 expression, thereby reducing ROS levels. Simultaneously, the elevation of GSTP1 and JNK complex may reduce the expression of p-JNK and inhibit the activation of JNK pathway, which might inhibit cell apoptosis. Discussion: In conclusion, our experiments suggested that upregulated SPAG6 might mitigate the pro-apoptotic effects of DNR through ROS/JNK MAPK axis in a GSTP1-dependent manner. [ABSTRACT FROM AUTHOR]

Published

2024

2. Revolutionizing pediatric neuroblastoma treatment: unraveling new molecular targets for precision interventions.

Author

Min Zheng, Kumar, Ankush, Sharma, Vishakha, Behl, Tapan, Sehgal, Aayush, Wal, Pranay, Shinde, Nirmala Vikram, Kawaduji, Bhosale Sachin, Kapoor, Anupriya, Anwer, Md. Khalid, Gulati, Monica, Bairong Shen, Singla, Rajeev K., and Bungau, Simona Gabriela

Subjects

NEUROBLASTOMA, PEDIATRIC therapy, DRUG target, GENE enhancers, CARRIER proteins, TREATMENT effectiveness

Abstract

Neuroblastoma (NB) is the most frequent solid tumor in pediatric cases, contributing to around 15% of childhood cancer-related deaths. The wideranging genetic, morphological, and clinical diversity within NB complicates the success of current treatment methods. Acquiring an in-depth understanding of genetic alterations implicated in the development of NB is essential for creating safer and more efficient therapies for this severe condition. Several molecular signatures are being studied as potential targets for developing new treatments for NB patients. In this article, we have examined the molecular factors and genetic irregularities, including those within insulin gene enhancer binding protein 1 (ISL1), dihydropyrimidinase-like 3 (DPYSL3), receptor tyrosine kinase-like orphan receptor 1 (ROR1) and murine double minute 2-tumor protein 53 (MDM2-P53) that play an essential role in the development of NB. A thorough summary of the molecular targeted treatments currently being studied in preclinical and clinical trials has been described. Recent studies of immunotherapeutic agents used in NB are also studied in this article. Moreover, we explore potential future directions to discover new targets and treatments to enhance existing therapies and ultimately improve treatment outcomes and survival rates for NB patients. [ABSTRACT FROM AUTHOR]

Published

2024

3. Early life epigenetics and childhood outcomes: a scoping review.

Author

Hari Gopal S, Alenghat T, and Pammi M

Abstract

Epigenetics is the study of changes in gene expression, without a change in the DNA sequence that are potentially heritable. Epigenetic mechanisms such as DNA methylation, histone modifications, and small non-coding RNA (sncRNA) changes have been studied in various childhood disorders. Causal links to maternal health and toxin exposures can introduce epigenetic modifications to the fetal DNA, which can be detected in the cord blood. Cord blood epigenetic modifications provide evidence of in-utero stressors and immediate postnatal changes, which can impact both short and long-term outcomes in children. The mechanisms of these epigenetic changes can be leveraged for prevention, early detection, and intervention, and to discover novel therapeutic modalities in childhood diseases. We report a scoping review of early life epigenetics, the influence of maternal health, maternal toxin, and drug exposures on the fetus, and its impact on perinatal, neonatal, and childhood outcomes. IMPACT STATEMENT: Epigenetic changes such as DNA methylation, histone modification, and non-coding RNA have been implicated in the pathophysiology of various disease processes. The fundamental changes to an offspring's epigenome can begin in utero, impacting the immediate postnatal period, childhood, adolescence, and adulthood. This scoping review summarizes current literature on the impact of early life epigenetics, especially DNA methylation on childhood health outcomes., (© 2024. The Author(s), under exclusive licence to the International Pediatric Research Foundation, Inc.)

Published

2024

4. CUT homeobox genes: transcriptional regulation of neuronal specification and beyond.

Author

Leyva-Díaz, Eduardo

Subjects

GENETIC regulation, GENETIC transcription regulation, HOMEOBOX genes, GENE expression, DEVELOPMENTAL biology, GENE families

Abstract

CUT homeobox genes represent a captivating gene class fulfilling critical functions in the development and maintenance of multiple cell types across a wide range of organisms. They belong to the larger group of homeobox genes, which encode transcription factors responsible for regulating gene expression patterns during development. CUT homeobox genes exhibit two distinct and conserved DNA binding domains, a homeodomain accompanied by one or more CUT domains. Numerous studies have shown the involvement of CUT homeobox genes in diverse developmental processes such as body axis formation, organogenesis, tissue patterning and neuronal specification. They govern these processes by exerting control over gene expression through their transcriptional regulatory activities, which they accomplish by a combination of classic and unconventional interactions with the DNA. Intriguingly, apart from their roles as transcriptional regulators, they also serve as accessory factors in DNA repair pathways through protein-protein interactions. They are highly conserved across species, highlighting their fundamental importance in developmental biology. Remarkably, evolutionary analysis has revealed that CUT homeobox genes have experienced an extraordinary degree of rearrangements and diversification compared to other classes of homeobox genes, including the emergence of a novel gene family in vertebrates. Investigating the functions and regulatory networks of CUT homeobox genes provides significant understanding into the molecular mechanisms underlying embryonic development and tissue homeostasis. Furthermore, aberrant expression or mutations in CUT homeobox genes have been associated with various human diseases, highlighting their relevance beyond developmental processes. This review will overview the well known roles of CUT homeobox genes in nervous system development, as well as their functions in other tissues across phylogeny. [ABSTRACT FROM AUTHOR]

Published

2023

5. Epigenetic signature of very low birth weight in young adult life.

Author

Kuula J, Czamara D, Hauta-Alus H, Lahti J, Hovi P, Miettinen ME, Ronkainen J, Eriksson JG, Andersson S, Järvelin MR, Sebert S, Räikkönen K, Binder EB, and Kajantie E

Abstract

Background: Globally, one in ten babies is born preterm (<37 weeks), and 1-2% preterm at very low birth weight (VLBW, <1500 g). As adults, they are at increased risk for a plethora of health conditions, e.g., cardiometabolic disease, which may partly be mediated by epigenetic regulation. We compared blood DNA methylation between young adults born at VLBW and controls., Methods: 157 subjects born at VLBW and 161 controls born at term, from the Helsinki Study of Very Low Birth Weight Adults, were assessed for peripheral venous blood DNA methylation levels at mean age of 22 years. Significant CpG-sites (5'-C-phosphate-G-3') were meta-analyzed against continuous birth weight in four independent cohorts (pooled n = 2235) with cohort mean ages varying from 0 to 31 years., Results: In the discovery cohort, 66 CpG-sites were differentially methylated between VLBW adults and controls. Top hits were located in HIF3A, EBF4, and an intergenic region nearest to GLI2 (distance 57,533 bp). Five CpG-sites, all in proximity to GLI2, were hypermethylated in VLBW and associated with lower birth weight in the meta-analysis., Conclusion: We identified differentially methylated CpG-sites suggesting an epigenetic signature of preterm birth at VLBW present in adult life., Impact: Being born preterm at very low birth weight has major implications for later health and chronic disease risk factors. The mechanism linking preterm birth to later outcomes remains unknown. Our cohort study of 157 very low birth weight adults and 161 controls found 66 differentially methylated sites at mean age of 22 years. Our findings suggest an epigenetic mark of preterm birth present in adulthood, which opens up opportunities for mechanistic studies., (© 2024. The Author(s).)

Published

2024

6. Aberrant expression of SPAG6 and NM23 predicts poor prognosis of human osteosarcoma.

Author

Zhengqi Bao, Ruizhi Zhu, Huagang Fan, Yuchen Ye, Tian Li, and Damin Chai

Subjects

OSTEOSARCOMA, PROGNOSIS, IMMUNOSTAINING, CHINESE people, OVERALL survival

Abstract

Objective: To investigate the expression and clinical significance of sperm-associated antigen 6 and NM23 proteins in human osteosarcoma. Methods: The specimens of conventional osteosarcoma with follow-up from 42 Chinese patients were analyzed in this study, and 12 cases of osteochondroma were considered controls. The expression of SPAG6 and NM23 was inspected using immunohistochemical staining, qRT-PCR, and Western blotting methods. Results: The positive expression rate of SPAG6 protein (71.43%) in 42 cases of osteosarcoma tissue was significantly higher than that (33.33%) in 12 cases of osteochondroma tissues (p < 0.05), while the positive rate of NM23 protein (35.71%) in osteosarcoma tissue was lower than that (58.33%) in osteochondroma tissue (p < 0.05). The mRNA and protein levels of SPAG6 were significantly higher than those of the adjacent normal tissues, while the expression of NM23 was lower in osteosarcoma tissues than that in the controls (p < 0.05 for all). There was a positive relationship between the expression of SPAG6 and pathological grade, metastasis, and Enneking stage (p < 0.05 for all). The overall survival rate of osteosarcoma patients with SPAG6 positive expression was significantly lower than that with SPAG6 negative expression. The relationship between the expression of NM23 and pathological grade,metastasis, and Enneking stage was negative (p < 0.05 for all). The overall survival rate of the osteosarcoma patients with NM23 positive expression was higher than that of the patients with NM23 negative expression (p < 0.05). Conclusion: Overexpression of SPAG6 and low expression of NM23 are negatively related to pathological grade, metastasis, and Enneking stage and prognosis of osteosarcoma patients. This suggested that SPAG6 and NM23 should be considered candidate prognostic biomarkers for patients with osteosarcoma. [ABSTRACT FROM AUTHOR]

Published

2022

7. Understanding the development of oral epithelial organs through single cell transcriptomic analysis.

Author

Qianlin Ye, Bhojwani, Arshia, and . Hu, Jimmy K

Subjects

CELL analysis, TASTE buds, SPATIOTEMPORAL processes, EPITHELIAL cells, SALIVARY glands, GENE regulatory networks

Abstract

During craniofacial development, the oral epithelium begins as a morphologically homogeneous tissue that gives rise to locally complex structures, including the teeth, salivary glands and taste buds. How the epithelium is initially patterned and specified to generate diverse cell types remains largely unknown. To elucidate the genetic programs that direct the formation of distinct oral epithelial populations, we mapped the transcriptional landscape of embryonic day 12 mouse mandibular epithelia at single cell resolution. Our analysis identified key transcription factors and gene regulatory networks that define different epithelial cell types. By examining the spatiotemporal patterning process along the oral-aboral axis, our results propose a model in which the dental field is progressively confined to its position by the formation of the aboral epithelium anteriorly and the non-dental oral epithelium posteriorly. Using our data, we also identified Ntrk2 as a proliferation driver in the forming incisor, contributing to its invagination. Together, our results provide a detailed transcriptional atlas of the embryonic mandibular epithelium, and unveil new genetic markers and regulators that are present during the specification of various oral epithelial structures. [ABSTRACT FROM AUTHOR]

Published

2022

8. The conundrum of pharyngeal teeth origin: the role of germ layers, pouches, and gill slits.

Author

Huysseune, Ann, Cerny, Robert, and Witten, P. Eckhard

Subjects

EPIBLAST, DENTITION, EMBRYOLOGY, GILLS, ECTODERM, TEETH, CLEFT palate children

Abstract

There are several competing hypotheses on tooth origins, with discussions eventually settling in favour of an 'outside‐in' scenario, in which internal odontodes (teeth) derived from external odontodes (skin denticles) in jawless vertebrates. The evolution of oral teeth from skin denticles can be intuitively understood from their location at the mouth entrance. However, the basal condition for jawed vertebrates is arguably to possess teeth distributed throughout the oropharynx (i.e. oral and pharyngeal teeth). As skin denticle development requires the presence of ectoderm‐derived epithelium and of mesenchyme, it remains to be answered how odontode‐forming skin epithelium, or its competence, were 'transferred' deep into the endoderm‐covered oropharynx. The 'modified outside‐in' hypothesis for tooth origins proposed that this transfer was accomplished through displacement of odontogenic epithelium, that is ectoderm, not only through the mouth, but also via any opening (e.g. gill slits) that connects the ectoderm to the epithelial lining of the pharynx (endoderm). This review explores from an evolutionary and from a developmental perspective whether ectoderm plays a role in (pharyngeal) tooth and denticle formation. Historic and recent studies on tooth development show that the odontogenic epithelium (enamel organ) of oral or pharyngeal teeth can be of ectodermal, endodermal, or of mixed ecto–endodermal origin. Comprehensive data are, however, only available for a few taxa. Interestingly, in these taxa, the enamel organ always develops from the basal layer of a stratified epithelium that is at least bilayered. In zebrafish, a miniaturised teleost that only retains pharyngeal teeth, an epithelial surface layer with ectoderm‐like characters is required to initiate the formation of an enamel organ from the basal, endodermal epithelium. In urodele amphibians, the bilayered epithelium is endodermal, but the surface layer acquires ectodermal characters, here termed 'epidermalised endoderm'. Furthermore, ectoderm–endoderm contacts at pouch–cleft boundaries (i.e. the prospective gill slits) are important for pharyngeal tooth initiation, even if the influx of ectoderm via these routes is limited. A balance between sonic hedgehog and retinoic acid signalling could operate to assign tooth‐initiating competence to the endoderm at the level of any particular pouch. In summary, three characters are identified as being required for pharyngeal tooth formation: (i) pouch–cleft contact, (ii) a stratified epithelium, of which (iii) the apical layer adopts ectodermal features. These characters delimit the area in which teeth can form, yet cannot alone explain the distribution of teeth over the different pharyngeal arches. The review concludes with a hypothetical evolutionary scenario regarding the persisting influence of ectoderm on pharyngeal tooth formation. Studies on basal osteichthyans with less‐specialised types of early embryonic development will provide a crucial test for the potential role of ectoderm in pharyngeal tooth formation and for the 'modified outside‐in' hypothesis of tooth origins. [ABSTRACT FROM AUTHOR]

Published

2022

9. Spectroscopic Techniques for Dentistry Applications : Recent Advances

Author

Ashutosh Kumar Shukla and Ashutosh Kumar Shukla

Subjects

Mouth--Diseases, Spectrum analysis, Lasers in dentistry, Lasers

Abstract

Spectroscopic techniques have potential applications in many different fields. This book presents a general overview of different spectroscopic techniques and explores how they might be used for dentistry applications. With a general introduction to different techniques, the book discusses a wide range of spectroscopy techniques, with individual chapters focusing on specific techniques important to dentistry applications. Such techniques include Laser-induced Breakdown Spectroscopy (LIBS), Raman Spectroscopy, Fluorescence Spectroscopy and Electron Spin Resonance (ESR) spectroscopy. The book also covers molecular spectroscopic techniques such as UV-Visible Spectroscopy, Near-infrared Spectroscopy and Mid-infrared Spectroscopy. This book is suitable for Professionals and researchers in academia and Industry, as well as advanced students involved with EPR Spectroscopy and dentistry.Key Features:The book highlights different spectroscopic techniques for dentistry applications. Each chapter includes a brief review followed by recent trends.Individual chapter content will be designed to address the needs of technicians in addition to researchers.

Published

2022

10. The associations between maternal BMI and gestational weight gain and health outcomes in offspring at age 1 and 7 years

Author

Chiavaroli, Valentina, Hopkins, Sarah A., Biggs, Janene B., Rodrigues, Raquel O., Seneviratne, Sumudu N., Baldi, James C., McCowan, Lesley M. E., Cutfield, Wayne S., Hofman, Paul L., and Derraik, José G. B.

Published

2021