Welcome to Wei Lab!
Wei lab belongs to Department of Immunology, School of Basic Medical Sciences, Fudan University. We study vascular immunology by focusing on non-coding RNAs and organelle interactions and attempt to get better understanding of  macrophage phenotypic plasticity and pathophysiology of atherosclerosis. We cooperate with Prof. Le Kang's group in Guangzhou National Lab, and focus on the metabolic reprogramming of antigen presenting cells in HDM-induced allergic asthma.

魏园园课题组隶属于复旦大学基础医学院免疫学系。我们从事血管免疫学研究,非编码RNA及细胞器互作的角度出发,着力于阐明巨噬细胞极化的分子调控机制、巨噬细胞能量代谢转换在动脉粥样硬化形成过程中的作用以及巨噬细胞在肥胖与动脉粥样硬化关系中的作用。我们与广州实验室康乐院士课题组合作,聚焦于抗原呈递细胞的代谢重编程在尘螨引起的过敏性哮喘中的作用
LAB NEWS
2023-8    热烈祝贺课题组博士后解玉怀博士获得国自然青年项目(2024-2026)资助!
2023-10  祝贺课题组第一个博士研究生贾云慧顺利完成学位答辩!
NEW PUBLICATIONS
Regulation of microRNA (miRNA) function by modulating its biogenesis and targeting in the immune system. Immune cells orchestrate miRNA function through regulating or modifying the key enzymes and proteins involved in miRNA biogenesis, such as Exportin 5, Dicer, Ago2, and some RNA binding proteins (RBPs). Moreover, miRNAs may selectively target mRNAs according to the miRNA site types in distinct immune cells. miRNA-mediated targeting may also be regulated by competing endogenous RNA (ceRNAs) or affected by alternative poly(A) site usage in immune responses. The events in the miRNA biogenesis and targeting pathways that are able to be regulated during immune responses are summarized in the boxes outlined with dash lines and numbered according to the text. The arrows with solid lines indicate each step in the process of miRNA biogenesis, while the arrows with dash lines indicate how that step is modulated in immune cells.
Long non-coding RNAs (lncRNAs) represent crucial transcriptional and post-transcriptional gene regulators during antimicrobial responses in the host innate immune system. Studies have shown that lncRNAs are expressed in a highly tissue- and cell-specific- manner and are involved in the differentiation and function of innate immune cells, as well as inflammatory and antiviral processes, through versatile molecular mechanisms. These lncRNAs function via the interactions with DNA, RNA, or protein in either cis or trans pattern, relying on their specific sequences or their transcriptions and processing. The dysregulation of lncRNA function is associated with various human non-infectious diseases, such as inflammatory bowel disease, cardiovascular diseases, and diabetes mellitus. Here, we provide an overview of the regulation and mechanisms of lncRNA function in the development and differentiation of innate immune cells, and during the activation or repression of innate immune responses. These elucidations might be beneficial for the development of therapeutic strategies targeting inflammatory and innate immune-mediated diseases.
Yunhui Jia & Yuanyuan Wei. Modulators of MicroRNA Function in the Immune System.
Int. J. Mol. Sci. 2020; 21(7): 2357.

Yuhuai Xie, Yuanyuan Wei*. A Novel Regulatory Player in the Innate Immune System: Long Non-coding RNAs. Int. J. Mol. Sci. 2021; 22(17), 9535.


He J, Zhu Y, Wang B, Yang P, Guo W, Liang B, Jiang F, Wang H, Wei Y*, Kang L*. The piRNA-guided intron removal from pre-mRNAs regulates density-dependent reproductive strategy. Cell Reports. 2022; 39:110593.


Jia Y, Cheng L, Yang J, Mao J, Xie Y, Yang X,Zhang X, Wang D, Zhao Z, Schober A, Wei Y*. miR-223-3p Prevents Necroptotic Macrophage Death by Targeting Ripk3 in a Negative Feedback Loop and Consequently Ameliorates Advanced Atherosclerosis. Arterioscler Thromb Vasc Biol. 2024 Jan;44(1):218-237.
BACKGROUND:  The  formation  of  large  necrotic  cores  results  in  vulnerable  atherosclerotic  plaques,  which  can  lead  to  severe cardiovascular diseases. However, the specific regulatory mechanisms underlying the development of necrotic cores remain unclear.
METHODS: To evaluate how the modes of lesional cell death are reprogrammed during the development of atherosclerosis, the expression levels of key proteins that are involved in the necroptotic, apoptotic, and pyroptotic pathways were compared between different stages of plaques in humans and mice. Luciferase assays and loss-of-function studies were performed to identify the microRNA-mediated regulatory mechanism that protects foamy macrophages from necroptotic cell death. The role of this mechanism in atherosclerosis was determined by using a knockout mouse model with perivascular drug administration and tail vein injection of microRNA inhibitors in Apoe −/−  mice.
RESULTS: Here, we demonstrate that the necroptotic, rather than the apoptotic or pyroptotic, pathway is more activated in advanced unstable plaques compared with stable plaques in both humans and mice, which closely correlates with necrotic core formation. The upregulated expression of Ripk3 (receptor-interacting protein kinase 3) promotes the C/EBPβ (CCAAT/enhancer  binding  protein  beta)-dependent  transcription  of  the  microRNA  miR-223-3p,  which  conversely  inhibits  Ripk3 expression and forms a negative feedback loop to regulate the necroptosis of foamy macrophages. The knockout of the Mir223 gene in bone marrow cells accelerates atherosclerosis in Apoe −/−  mice, but this effect can be rescued by Ripk3 deficiency  or  treatment  with  the  necroptosis  inhibitors  necrostatin-1  and  GSK-872.  Like  the  Mir223  knockout,  treating Apoe −/−  mice with miR-223-3p inhibitors increases atherosclerosis.
CONCLUSIONS: Our study suggests that miR-223-3p expression in macrophages protects against atherosclerotic plaque rupture by limiting the formation of necrotic cores, thus providing a potential microRNA therapeutic candidate for atherosclerosis.
CURRENT RESEARCH INTERESTS
Atherosclerosis is a leading -but potentially preventable- cause of death and disability worldwide resulting in devastating diseases, such as myocardial infarction due to coronary artery disease or stroke. The current concept of atherogenesis includes a central role of apolipoprotein B-containing lipoproteins, such as LDL or remnant lipoproteins, which trigger a chronic inflammatory response of the vessel wall dominated by the  infiltration of monocyte-derived macrophages. Multiple stimuli, including cytokines, chemokines and modified lipoproteins, may dynamically modulate the macrophage phenotype in atherosclerotic lesions. Our lab aims to understand how macrophage phenotype is regulated during atherosclerosis progression, and figure out the potential therapeutic application of targeting macrophages in atherosclerosis.

Regulatory RNAs in macrophages and atherosclerosis

Our research has found that regulatory RNAs, such as miRNAs, play crucial roles in atherosclerosis by regulating macrophage polarization and metabolism. However, how regulatory RNA functions are modulated in macrophages  during atherosclerosis progression is still unknown.
Metabolic reprogramming of antigen presenting cells in HDM induced allergic asthma

When encountered with allergen, antigen presenting cells are not only activated to priming type 2 immune response, but also accompanied with metabolic reprogramming. How the immune reaction type is influenced by the metabolic changes of antigen presenting cells is not well-understood.
Contribution of organelle interactions to macrophage functions
and atherosclerosis progression

It is known that organelles communicate with each other to maintain cellular homeostasis. However, how signals are transduced among organelles to determine the immune functions of macrophages has not been clear yet.