【5月文献战报】Bioss抗体新增高分文献精彩呈现
截至目前,引用Bioss产品发表的文献共18564篇,总影响因子80606.851分,发表在Nature, Science, Cell以及Immunity等顶级期刊的文献共53篇,合作单位覆盖了清华、北大、复旦、华盛顿大学、麻省理工学院、东京大学以及纽约大学等国际研究机构上百所。
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近期收录2022年5月引用Bioss产品发表的文献共223篇(图一,绿色柱),文章影响因子(IF) 总和高达1283.088,其中,20分以上文章2篇,10分以上文献26篇(图二)。
图一
图二
Cell [IF=41.584]

文献引用抗体:bs-6285R
Anti-PRSS10 pAb
作者单位:日本东京大学医学科学研究所微生物学和免疫学系
Cell Stem Cell [IF=24.633]
文献引用抗体:bs-2433R-AF555
Anti-ATP4B/AF555 pAb; FCM
human reproduction update
[IF=15.61]
Small [IF=13.281]
文献引用抗体:
bs-4842R
Anti-Phospho-EIF2S1(Ser51) pAb
Biomaterials [IF=12.479]
文献引用抗体:bs-2593R
Anti-Caspase 3 precursor pAb; IF
progress in neurobiology
[IF=11.685]
bs-4635R
Anti-Phospho-MST1 (Thr183) pAb; IB, IF
作者单位:南开大学生命科学学院
摘要:Alzheimer’s disease (AD) is the most prevalent form of dementia in the old adult and characterized by progressive cognitive decline and neuronal damage. The mammalian Ste20-like kinase1/2 (MST1/2) is a core component in Hippo signaling, which regulates neural stem cell proliferation, neuronal death and neuroinflammation. However, whether MST1/2 is involved in the occurrence and development of AD remains unknown. In this study we reported that the activity of MST1 was increased with Aβ accumulation in the hippocampus of 5xFAD mice. Overexpression of MST1 induced AD-like phenotype in normal mice and accelerated cognitive decline, synaptic plasticity damage and neuronal apoptosis in 2-month-old 5xFAD mice, but did not significantly affect Aβ levels. Mechanistically, MST1 associated with p53 and promoted neuronal apoptosis by phosphorylation and activation of p53, while p53 knockout largely reversed MST1-induced AD-like cognitive deficits. Importantly, either genetic knockdown or chemical inactivation of MST1 could significantly improve cognitive deficits and neuronal apoptosis in 7-month-old 5xFAD mice. Our results support the idea that MST1-mediated neuronal apoptosis is an essential mechanism of cognitive deficits and neuronal loss for AD, and manipulating the MST1 activity as a potential strategy will shed light on clinical treatment for AD or other diseases caused by neuronal injury.
BIOENGINEERING &
TRANSLATIONAL MEDICINE
[IF=10.711]
文献引用抗体:bs-0195R

摘要:Abnormal endometrial receptivity is a major cause of the failure of embryo transplantation, which may lead to infertility, adverse pregnancy, and neonatal outcomes. While hormonal treatment has dramatically improved the fertility outcomes in women with endometriosis, a substantial unmet need persists in the treatment. In this study, methacrylate gelatin (GelMA) and methacrylate sericin (SerMA) hydrogel with human umbilical cord mesenchymal stem cells (HUMSC) encapsulation was designed for facilitating endometrial regeneration and fertility restoration through in situ injection. The presented GelMA/10%SerMA hydrogel showed appropriate swelling ratio, good mechanical properties, and degradation stability. In vitro cell experiments showed that the prepared hydrogels had excellent biocompatibility and cell encapsulation ability of HUMSC. Further in vivo experiments demonstrated that GelMA/SerMA@HUMSC hydrogel could increase the thickness of endometrium and improve the endometrial interstitial fibrosis. Moreover, regenerated endometrial tissue was more receptive to transfer embryos. Summary, we believed that GelMA/SerMA@HUMSC hydrogel will hold tremendous promise to repair or regenerate damaged endometrium.
kidney INTERNATIONAL
[IF=10.612]
文献引用抗体:bs-0666R
Anti-Fibronectin/FN1 pAb
作者单位:日本东京日庆大学医学院内科糖尿病、代谢和内分泌科
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