Xinjun Yang scite author profile

Xinjun Yang

3Publications

1Citation Statement Received

149Citation Statements Given

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145

Affiliations

Shandong Provincial Hospital, Shandong First Medical University

Publications

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A retrospective study of 1064‐nm Q‐switched Nd:YAG laser therapy for acquired bilateral nevus of Ota‐like macules

Yang

Tianyu

et al. 2023

Skin Research and Technology

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Background The therapeutic efficacy of laser treatments for acquired bilateral nevus of Ota‐like macules (ABNOM) varies among studies, and few studies have evaluated the factors affecting therapeutic effects. Aims To evaluate the efficacy and safety of 1064‐nm Q‐switched Nd:YAG laser (QSNYL) therapy for ABNOM and to identify the factors influencing the outcome. Methods A total of 110 patients with ABNOM were retrospectively evaluated and received two‐to‐nine treatment sessions. The effects of different factors on the therapeutic effect were analyzed on the basis of the number of treatments, age at first treatment, skin type, lesion color, affected area, number of lesion sites, and presence of concomitant melasma. Results The curative effect was positively correlated with the treatment time and negatively correlated with the increasing age at first treatment (p < 0.05). The curative effect was better in patients with skin type III than those with type IV ( p < 0.05) and in patients with a lesion area of less than 10 cm2 than those with a larger affected area (p < 0.05). Additionally, the treatment effect was poorer in patients with concomitant melasma (p < 0.05). The treatment effect was not significantly correlated with the lesion color or number of affected sites (p > 0.05). Eleven patients (10%) developed postinflammatory hyperpigmentation (PIH). Conclusions Early and repeated QSNYL therapy achieved satisfactory results for ABNOM. The risk of PIH after laser treatment is highest among patients with older age, darker lesion color, and darker skin color. For patients with ABNOM with concurrent melasma, low‐energy laser therapy is recommended to reduce the risk of melasma aggravation.

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TUBA1C: a new potential target of LncRNA EGFR-AS1 promotes gastric cancer progression

et al. 2023

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Background The lack of obvious symptoms of early gastric cancer (GC) as well as the absence of sensitive and specific biomarkers results in poor clinical outcomes. Tubulin is currently emerging as important regulators of the microtubule cytoskeleton and thus have a strong potential to be implicated in a number of disorders, however, its mechanism of action in gastric cancer is still unclear. Tubulin alpha-1 C (TUBA1C) is a subtype of α-tubulin, high TUBA1C expression has been shown to be closely related to a poor prognosis in various cancers, this study, for the first time, revealed the mechanism of TUBA1C promotes malignant progression of gastric cancer in vitro and in vivo. Methods The expression of lncRNA EGFR-AS1 was detected in human GC cell lines by qRT–PCR. Mass spectrometry experiments following RNA pulldown assays found that EGFR-AS1 directly binds to TUBA1C, the CCK8, EdU, transwell, wound-healing, cell cycle assays and animal experiments were conducted to investigate the function of TUBA1C in GC. Combined with bioinformatics analyses, reveal interaction between Ki-67, E2F1, PCNA and TUBA1C by western blot. Rescue experiments furtherly demonstrated the relationship of EGFR-AS1and TUBA1C. Results TUBA1C was proved to be a direct target of EGFR-AS1, and TUBA1C promotes gastric cancer proliferation, migration and invasion by accelerating the progression of the cell cycle from the G1 phase to the S phase and activating the expression of oncogenes: Ki-67, E2F1 and PCNA. Conclusion TUBA1C is a new potential target of LncRNA EGFR-AS1 promotes gastric cancer progression and could be a novel biomarker and therapeutic target for GC.

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TUBA1C: a new potential target of LncRNA EGFR-AS1 promotes gastric cancer progression

Wang

Cui

Yang

et al. 2022

Preprint

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Background: The lack of obvious symptoms of early GC as well as the absence of sensitive and specific biomarkers results in poor clinical outcomes. High TUBA1C expression has been shown to be closely related to a poor prognosis in in various cancers, however, the role of TUBA1C in GC have not yet been elucidated. This study, for the first time, revealed that TUBA1C drives the growth of GC cell lines both in vitro and in vivo. Methods: The expression of lncRNA EGFR-AS1 was detected in human GC cell lines by qRT–PCR. MS experiments following RNA pulldown assays found that EGFR-AS1 directly binds to TUBA1C, the CCK8, EdU, transwell, wound-healing, cell cycle assays and animal experiments were conducted to investigate the function of TUBA1C in GC. Combined with bioinformatics analyses, reveal interaction between E2F1, Ki-67, PCNA and TUBA1C by western blot. Rescue experiments furtherly demonstrated the relationship of EGFR-AS1and TUBA1C. Results: TUBA1C was proved to be a direct target of EGFR-AS1, TUBA1C promotes gastric cancer proliferation, migration and invasion by accelerating the progression of the cell cycle from the G1 phase to the S phase and activating the expression of tumor suppressor genes: E2F1, Ki-67, and PCNA. Conclusions: TUBA1C is a new potential target of LncRNA EGFR-AS1 promotes gastric cancer progression and could be a novel biomarker and therapeutic target for GC.

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Xinjun Yang

A retrospective study of 1064‐nm Q‐switched Nd:YAG laser therapy for acquired bilateral nevus of Ota‐like macules

TUBA1C: a new potential target of LncRNA EGFR-AS1 promotes gastric cancer progression

TUBA1C: a new potential target of LncRNA EGFR-AS1 promotes gastric cancer progression

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