Your search keyword '"Jia-Lei Hu"' showing total 10 results

1. Immunogenicity and safety of a severe acute respiratory syndrome coronavirus 2 inactivated vaccine in healthy adults: randomized, double-blind, and placebo-controlled phase 1 and phase 2 clinical trials

Author

Hong-Xing Pan, Jian-Kai Liu, Bao-Ying Huang, Gui-Fan Li, Xian-Yun Chang, Ya-Fei Liu, Wen-Ling Wang, Kai Chu, Jia-Lei Hu, Jing-Xin Li, Dan-Dan Zhu, Jing-Liang Wu, Xiao-Yu Xu, Li Zhang, Meng Wang, Wen-Jie Tan, Wei-Jin Huang, Feng-Cai Zhu, and Jing Ni

Subjects

Medicine

Abstract

Abstract. Background:. The significant morbidity and mortality resulted from the infection of a severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) call for urgent development of effective and safe vaccines. We report the immunogenicity and safety of an inactivated SARS-CoV-2 vaccine, KCONVAC, in healthy adults. Methods:. Phase 1 and phase 2 randomized, double-blind, and placebo-controlled trials of KCONVAC were conducted in healthy Chinese adults aged 18 to 59 years. The participants in the phase 1 trial were randomized to receive two doses, one each on Days 0 and 14, of either KCONVAC (5 or 10 μg/dose) or placebo. The participants in the phase 2 trial were randomized to receive either KCONVAC (at 5 or 10 μg/dose) or placebo on Days 0 and 14 (0/14 regimen) or Days 0 and 28 (0/28 regimen). In the phase 1 trial, the primary safety endpoint was the proportion of participants experiencing adverse reactions/events within 28 days following the administration of each dose. In the phase 2 trial, the primary immunogenicity endpoints were neutralization antibody seroconversion and titer and anti-receptor-binding domain immunoglobulin G seroconversion at 28 days after the second dose. Results:. In the phase 1 trial, 60 participants were enrolled and received at least one dose of 5-μg vaccine (n = 24), 10-μg vaccine (n = 24), or placebo (n = 12). In the phase 2 trial, 500 participants were enrolled and received at least one dose of 5-μg vaccine (n = 100 for 0/14 or 0/28 regimens), 10-μg vaccine (n = 100 for each regimen), or placebo (n = 50 for each regimen). In the phase 1 trial, 13 (54%), 11 (46%), and seven (7/12) participants reported at least one adverse event (AE) after receiving 5-, 10-μg vaccine, or placebo, respectively. In the phase 2 trial, 16 (16%), 19 (19%), and nine (18%) 0/14-regimen participants reported at least one AE after receiving 5-, 10-μg vaccine, or placebo, respectively. Similar AE incidences were observed in the three 0/28-regimen treatment groups. No AEs with an intensity of grade 3+ were reported, expect for one vaccine-unrelated serious AE (foot fracture) reported in the phase 1 trial. KCONVAC induced significant antibody responses; 0/28 regimen showed a higher immune responses than that did 0/14 regimen after receiving two vaccine doses. Conclusions:. Both doses of KCONVAC are well tolerated and able to induce robust immune responses in healthy adults. These results support testing 5-μg vaccine in the 0/28 regimen in an upcoming phase 3 efficacy trial. Trial Registration:. http://www.chictr.org.cn/index.aspx (No. ChiCTR2000038804, http://www.chictr.org.cn/showproj.aspx?proj=62350; No. ChiCTR2000039462, http://www.chictr.org.cn/showproj.aspx?proj=63353).

Published

2021

2. Immunity duration of a recombinant adenovirus type-5 vector-based Ebola vaccine and a homologous prime-boost immunisation in healthy adults in China: final report of a randomised, double-blind, placebo-controlled, phase 1 trial

Author

Jing-Xin Li, PhD, Li-Hua Hou, PhD, Fan-Yue Meng, MSc, Shi-Po Wu, PhD, Yue-Mei Hu, BS, Qi Liang, BS, Kai Chu, MSc, Zhe Zhang, BS, Jun-Jie Xu, PhD, Rong Tang, MSc, Wen-Juan Wang, MSc, Pei Liu, ProfPhD, Jia-Lei Hu, MSc, Li Luo, MSc, Rong Jiang, MSc, Feng-Cai Zhu, MSc, and Wei Chen, PhD

Subjects

Public aspects of medicine, RA1-1270

Abstract

Summary: Background: The 2013–15 Ebola virus disease epidemic in west Africa greatly accelerated the development of Ebola vaccine. We aimed to analyse the immune persistence induced by one shot of an adenovirus type-5 vector-based Ebola virus vaccine up to 6 months and the effect of boosting with a homologous vector in healthy adults in China. Methods: In a randomised, double-blind, placebo-controlled, phase 1 clinical trial in one site in Jiangsu Province, China, 120 healthy adults aged 18–60 years received an initial dose of intramuscular adenovirus type-5 Ebola virus vaccine of 4·0 × 1010 viral particles, 1·6 × 1011 viral particles, or placebo, and were followed up to day 168. Participants were subsequently re-recruited to receive a booster dose of the same vaccine or placebo, in the same dose, at month 6. Women who were pregnant, breastfeeding, or planned to become pregnant during the next month were excluded. Randomisation was conducted by computer-generated block randomisation. Randomisation data were unmasked for interim analysis of the data obtained between days 0–28 but not disclosed to participants or site staff. Safety and immunogenicity analysis were done on the intention-to-treat population. We aimed to assess the safety profile of the experimental vaccine and the immunity responses to a single-dose immunisation or a homologous prime-boost regimen. Primary outcomes were Ebola glycoprotein-specific ELISA antibody responses 28 days post-boost and the occurrences of adverse reactions post-boost. The original trial and the extended booster study were registered with ClinicalTrials.gov, numbers NCT02326194 and NCT02533791, respectively. Findings: Between Dec 28, 2014, and Jan 9, 2015, we enrolled 210 volunteers. 90 participants were not randomised due to not meeting inclusion criteria (61), meeting exclusion criteria (4), or withdrawal of consent (25). 120 people were randomly assigned to receive intramuscular Ebola vaccine at 4·0 × 1010 viral particles (low dose, n=40), Ebola vaccine at 1·6 × 1011 viral particles (high dose, n=40), or placebo (n=40, in two groups of 20). After prime vaccination, the geometric mean titer (GMT) of ELISA EC90 peaked at 682·7 (95% CI 424·3–1098·5) in the low-dose vaccine group and 1305·7 (970·1–1757·2) in the high-dose vaccine group at day 28, and then fell gradually through the next a few months to 575·5 (394·8–838·8) in the high-dose vaccine group and 197·9 (107·9–362·7) in the low-dose vaccine group at day 168. No specific response was recorded in the placebo group with a GMT of 5·0. Of the 120 participants involved in the initial trial, ten participants declined to participate, and 110 were included in the boost immunisation: 38 received the low dose, 35 received the high dose, and 37 received the placebo. At day 28 after boost vaccination, the ELISA EC90 titres rapidly rose to 6110 (95% CI 4705–7935) in the low-dose group and to 11825 (8904–15705) in the high dose group. 78 of 110 participants reported at least one solicited adverse reaction within the first 7 days after booster administration. Both of the groups who received vaccine showed significantly higher incidence of mild or moderate solicited adverse reactions than did the placebo group. Interpretation: The adenovirus 5-vectored Ebola vaccine of 1·6 × 1011 viral particles was highly immunogenic and safe. The lower dose of 4·0 × 1010 viral particles was also safe, but immunogenicity seemed to be more vulnerable to the pre-existing immunity of adenovirus 5. A homologous priming-boosting regimen with adenovirus type-5 Ebola vaccine at 6 months interval was able to elicit greater antibody responses with longer duration. These results support an immunisation strategy to implement a booster injection for a more durable protection against Ebola virus disease. Funding: Chinese Ministry of Science and Technology and The National Health and Family Planning Commission, Beijing Institute of Biotechnology, and Tianjin CanSino Biotechnology.

Published

2017

3. Sikokianin D, A New C-3/C-3'-Biflavanone from the Roots of Wikstroemia indica

Author

Jie Li, Lin-Yan Lu, Ling-Hui Zeng, Chong Zhang, Jia-Lei Hu, and Xiang-Rong Li

Subjects

Wikstroemia indica, sikokianin D, C-3/C-3"-biflavanone, Organic chemistry, QD241-441

Abstract

A new 3,3′′-biflavanone, sikokianin D (1), was isolated from the roots of Wikstroemia indica, together with two known compounds. Their structures were elucidated by chemical evidence and spectral analyses, including HR-ESI-MS, and 1D- and 2D-NMR techniques.

Published

2012

4. A New C-3/C-3'-Biflavanone from the Roots of Stellera chamaejasme L

Author

Jie Yang, Xiang-Rong Li, Jia-Lei Hu, Xin Cao, Wei Zhao, and Jie Li

Subjects

Stellera chamaejasme, Thymelaeaceae, biflavanone, Organic chemistry, QD241-441

Abstract

A new 3, 3”-biflavanone, neochamaejasmin C (1), was isolated from the roots of Stellera chamaejasme L., together with four known compounds. Their structures and configurations were elucidated by spectroscopic methods, including 2D-NMR techniques.

Published

2011

5. SIRT1 but not its increased expression is essential for lifespan extension in caloric-restricted mice

Author

Ying Li, Jia-Lei Hu, Valter D. Longo, Evi M. Mercken, Michael W. McBurney, Rafael de Cabo, Susan M. Krzysik-Walker, and Min Wei

Subjects

Aging, medicine.medical_specialty, media_common.quotation_subject, Longevity, Calorie restriction, Mice, SIRT1, Sirtuin 1, Internal medicine, medicine, Animals, RNA, Messenger, media_common, Short Takes, Regulation of gene expression, Genetics, biology, anti-aging, Caloric theory, Heterozygote advantage, Cell Biology, Endocrinology, Gene Expression Regulation, biology.protein, caloric restriction, lifespan, hormones, hormone substitutes, and hormone antagonists

Abstract

The SIRT1 deacetylase is one of the best-studied putative mediators of some of the anti-aging effects of calorie restriction (CR), but its role in CR-dependent lifespan extension has not been demonstrated. We previously found that mice lacking both copies of SIRT1 displayed a shorter median lifespan than wild-type mice on an ad libitum diet. Here, we report that median lifespan extension in CR heterozygote SIRT1(+/-) mice was identical (51%) to that observed in wild-type mice, but SIRT1(+/-) mice displayed a higher frequency of certain pathologies. Although larger studies in additional genetic backgrounds are needed, these results provide strong initial evidence for the requirement of SIRT1 for the lifespan extension effects of CR, but suggest that its high expression is not required for CR-induced lifespan extension.

Published

2013

6. Sikokianin D, A New C-3/C-3'-Biflavanone from the Roots of Wikstroemia indica

Author

Chong Zhang, Jie Li, Ling-Hui Zeng, Xiang-Rong Li, Lin-Yan Lu, and Jia-Lei Hu

Subjects

Magnetic Resonance Spectroscopy, Traditional medicine, Organic Chemistry, Pharmaceutical Science, sikokianin D, Biology, Wikstroemia indica, biology.organism_classification, Plant Roots, Article, Analytical Chemistry, C-3/C-3"-biflavanone, Chemistry (miscellaneous), Drug Discovery, Botany, Biflavonoids, Molecular Medicine, Wikstroemia, Physical and Theoretical Chemistry

Abstract

A new 3,3''-biflavanone, sikokianin D (1), was isolated from the roots of Wikstroemia indica, together with two known compounds. Their structures were elucidated by chemical evidence and spectral analyses, including HR-ESI-MS, and 1D- and 2D-NMR techniques.

Published

2012

7. The N-terminus of histone H3 is required for de novo DNA methylation in chromatin

Author

Jia Lei Hu, Guoliang Xu, Runrui Zhang, Kangling Zhang, Bo O. Zhou, and Jin-Qiu Zhou

Subjects

Saccharomyces cerevisiae Proteins, Saccharomyces cerevisiae, In Vitro Techniques, Biology, Methylation, Models, Biological, DNA Methyltransferase 3A, Histones, Mice, Histone methylation, Histone H2A, Animals, Histone code, DNA (Cytosine-5-)-Methyltransferases, DNA, Fungal, RNA-Directed DNA Methylation, Epigenomics, Multidisciplinary, urogenital system, EZH2, DNA Methylation, Biological Sciences, Molecular biology, Chromatin, Recombinant Proteins, Histone methyltransferase, DNA methylation

Abstract

DNA methylation and histone modification are two major epigenetic pathways that interplay to regulate transcriptional activity and other genome functions. Dnmt3L is a regulatory factor for the de novo DNA methyltransferases Dnmt3a and Dnmt3b. Although recent biochemical studies have revealed that Dnmt3L binds to the tail of histone H3 with unmethylated lysine 4 in vitro, the requirement of chromatin components for DNA methylation has not been examined, and functional evidence for the connection of histone tails to DNA methylation is still lacking. Here, we used the budding yeast Saccharomyces cerevisiae as a model system to investigate the chromatin determinants of DNA methylation through ectopic expression of murine Dnmt3a and Dnmt3L. We found that the N terminus of histone H3 tail is required for de novo methylation, while the central part encompassing lysines 9 and 27, as well as the H4 tail are dispensable. DNA methylation occurs predominantly in heterochromatin regions lacking H3K4 methylation. In mutant strains depleted of H3K4 methylation, the DNA methylation level increased 5-fold. The methylation activity of Dnmt3a largely depends on the Dnmt3L's PHD domain recognizing the histone H3 tail with unmethylated lysine 4. Functional analysis of Dnmt3L in mouse ES cells confirmed that the chromatin-recognition ability of Dnmt3L's PHD domain is indeed required for efficient methylation at the promoter of the endogenous Dnmt3L gene. These findings establish the N terminus of histone H3 tail with an unmethylated lysine 4 as a chromatin determinant for DNA methylation.

Published

2009

8. A New C-3/C-3'-Biflavanone from the Roots of Stellera chamaejasme L

Author

Xiang-Rong Li, Wei Zhao, Jie Li, Xin Cao, Jie Yang, and Jia-Lei Hu

Subjects

Chemistry, Stereochemistry, Proton Magnetic Resonance Spectroscopy, Communication, Organic Chemistry, biflavanone, Pharmaceutical Science, Plant Roots, Analytical Chemistry, lcsh:QD241-441, lcsh:Organic chemistry, Chemistry (miscellaneous), Thymelaeaceae, Stellera chamaejasme, Drug Discovery, Flavanones, Molecular Medicine, Physical and Theoretical Chemistry, Carbon-13 Magnetic Resonance Spectroscopy

Abstract

A new 3, 3"-biflavanone, neochamaejasmin C (1), was isolated from the roots of Stellera chamaejasme L., together with four known compounds. Their structures and configurations were elucidated by spectroscopic methods, including 2D-NMR techniques.

Published

2011

9. Reprogramming of mouse and human somatic cells by high-performance engineered factors

Author

Juan Gao, Dajiang Qin, Jing Jiang, Xia Kuang, Guoliang Xu, Jiekai Chen, Jia‐Lei Hu, Jinsong Li, Jing Liu, Keyu Lai, Jian Zhang, Xi‐Xiao Wei, Yang Wang, Duanqing Pei, and Zhang Lei

Subjects

Homeobox protein NANOG, Somatic cell, Induced Pluripotent Stem Cells, Biology, Biochemistry, Transactivation, Mice, SOX2, Genetics, Animals, Humans, Induced pluripotent stem cell, Molecular Biology, reproductive and urinary physiology, Homeodomain Proteins, SOXB1 Transcription Factors, fungi, Scientific Reports, Cellular Reprogramming, Embryonic stem cell, Cell biology, embryonic structures, sense organs, Stem cell, biological phenomena, cell phenomena, and immunity, Reprogramming, Octamer Transcription Factor-3

Abstract

Reprogramming somatic cells to become induced pluripotent stem cells (iPSCs) by using defined factors represents an important breakthrough in biology and medicine, yet remains inefficient and poorly understood. We therefore devised synthetic factors by fusing the VP16 transactivation domain to OCT4 (also known as Pou5f1), NANOG and SOX2, respectively. These synthetic factors could reprogramme both mouse and human fibroblasts with enhanced efficiency and accelerated kinetics. Remarkably, Oct4–VP16 alone could efficiently reprogramme mouse embryonic fibroblasts (MEFs) into germline-competent iPSCs. Furthermore, episomally delivered synthetic factors could reproducibly generate integration-free iPSCs from MEFs with enhanced efficiency. Our results not only demonstrate the feasibility of engineering more potent reprogramming factors, but also suggest that transcriptional reactivation of OCT4 target genes might be a rate-limiting step in the conversion of somatic cells to pluripotent cells. Synthetic factor-based reprogramming might lead to a paradigm shift in reprogramming research.

Published

2011

10. Regulation of DNA methylation activity through Dnmt3L promoter methylation by Dnmt3 enzymes in embryonic development

Author

Ying Jin, Taiping Chen, Guoliang Xu, Jia Lei Hu, Hiroyuki Sasaki, Ye Guang Hu, Ryutaro Hirasawa, Kenichiro Hata, Evani Viegas-Péquignot, En Li, Muriel Rigolet, and Chunliang Li

Subjects

endocrine system, Methyltransferase, Transcription, Genetic, Biology, DNA Methyltransferase 3A, Mice, Epigenetics of physical exercise, Histone methylation, Genetics, Animals, Humans, Point Mutation, DNA (Cytosine-5-)-Methyltransferases, Embryo Implantation, Promoter Regions, Genetic, Molecular Biology, RNA-Directed DNA Methylation, Genetics (clinical), Embryonic Stem Cells, urogenital system, EZH2, Immunologic Deficiency Syndromes, Cell Differentiation, General Medicine, Methylation, DNA Methylation, Molecular biology, Disease Models, Animal, Histone methyltransferase, embryonic structures, DNA methylation

Abstract

The genomic DNA is methylated by de novo methyltransferases Dnmt3a and Dnmt3b during early embryonic development. The establishment of appropriate methylation patterns depends on a fine regulation of the methyltransferase activity. The activity of both enzymes increases in the presence of Dnmt3L, a Dnmt3a/3b-like protein. However, it is unclear how the function of Dnmt3L is regulated. We found here that the expression of Dnmt3L is controlled via its promoter methylation during embryonic development. Genetic studies showed that Dnmt3a, Dnmt3b and Dnmt3L are all involved in the methylation of the Dnmt3L promoter. Disruption of both Dnmt3a and Dnmt3b genes in mouse rendered the Dnmt3L promoter devoid of methylation, causing incomplete repression of the Dnmt3L transcription in embryonic stem cells and embryos. Disruption of either Dnmt3a or Dnmt3b led to reduced methylation and increased transcription of Dnmt3L, but severe hypomethylation occurred only when Dnmt3b was deficient. Consistent with the major contribution of Dnmt3b in the Dnmt3L promoter methylation, methylation of Dnmt3L was significantly reduced in mouse models of the human ICF syndrome carrying point mutations in Dnmt3b. Interestingly, Dnmt3L also contributes to the methylation of its own promoter in embryonic development. We thus propose an auto-regulatory mechanism for the control of DNA methylation activity whereby the activity of the Dnmt3L promoter is epigenetically modulated by the methylation machinery including Dnmt3L itself. Insufficient methylation of the DNMT3L promoter during embryonic development due to deficiency in DNMT3B might be implicated in the pathogenesis of the ICF syndrome.

Published

2008