Your search keyword '"Wendy Wei"' showing total 6 results

1. Identification of an APOE ε4–specific blood‐based molecular pathway for Alzheimer's disease risk.

Author

Tao, Qiushan, Zhang, Chao, Mercier, Gustavo, Lunetta, Kathryn, Ang, Ting Fang Alvin, Akhter‐Khan, Samia, Zhang, Zhengrong, Taylor, Andrew, Killiany, Ronald J., Alosco, Michael, Mez, Jesse, Au, Rhoda, Zhang, Xiaoling, Farrer, Lindsay A., and Qiu, Wendy Wei Qiao

Subjects

DISEASE risk factors, APOLIPOPROTEIN E4, COMPLEMENT factor H, BLOOD proteins, DEFAULT mode network, APOLIPOPROTEIN E, TAU proteins

Abstract

INTRODUCTION: The precise apolipoprotein E (APOE) ε4‐specific molecular pathway(s) for Alzheimer's disease (AD) risk are unclear. METHODS: Plasma protein modules/cascades were analyzed using weighted gene co‐expression network analysis (WGCNA) in the Alzheimer's Disease Neuroimaging Initiative study. Multivariable regression analyses were used to examine the associations among protein modules, AD diagnoses, cerebrospinal fluid (CSF) phosphorylated tau (p‐tau), and brain glucose metabolism, stratified by APOE genotype. RESULTS: The Green Module was associated with AD diagnosis in APOE ε4 homozygotes. Three proteins from this module, C‐reactive protein (CRP), complement C3, and complement factor H (CFH), had dose‐dependent associations with CSF p‐tau and cognitive impairment only in APOE ε4 homozygotes. The link among these three proteins and glucose hypometabolism was observed in brain regions of the default mode network (DMN) in APOE ε4 homozygotes. A Framingham Heart Study validation study supported the findings for AD. DISCUSSION: The study identifies the APOE ε4–specific CRP–C3–CFH inflammation pathway for AD, suggesting potential drug targets for the disease. Highlights: Identification of an APOE ε4 specific molecular pathway involving blood CRP, C3, and CFH for the risk of AD.CRP, C3, and CFH had dose‐dependent associations with CSF p‐Tau and brain glucose hypometabolism as well as with cognitive impairment only in APOE ε4 homozygotes.Targeting CRP, C3, and CFH may be protective and therapeutic for AD onset in APOE ε4 carriers. [ABSTRACT FROM AUTHOR]

Published

2023

2. Regulating the balance between necroptosis, apoptosis and inflammation by inhibitors of apoptosis proteins.

Author

Vasilikos, Lazaros, Spilgies, Lisanne M, Knop, Janin, and Wong, Wendy Wei‐Lynn

Abstract

Understanding how inhibitor of apoptosis proteins (IAPs) regulate apoptosis and necroptosis has been fast‐forwarded by the use of Smac mimetics (SMs) to deplete or inhibit the IAPs, specifically cIAP1, cIAP2 and XIAP. The loss or inhibition of cIAP1, cIAP2 and XIAP causes the majority of cells to be sensitized to death receptor induced cell death, such as with tumour necrosis factor (TNF). Mouse genetics shows that there is some functional redundancy and the use of SMs has allowed us to understand how changing the composition of proteins recruited to TNF receptor 1 on TNF ligation can alter protein complex formation and activation of apoptosis or necroptosis, particularly when caspases are inhibited. Determining when or how caspase inhibition occurs physiologically combined with the loss of IAPs will be the next challenge in understanding the ability of IAPs to prevent cell death and/or limit inflammation. The February 2017 issue contains a Special Feature on Necroptotic death signalling: evolution, mechanisms and disease relevance. In recent years, research into a genetically encoded cell death program termed necroptosis has accelerated into vogue. Many laboratories are now racing to answer key questions such as: How does it occur? When does it occur? What does it do? What is it good (or not so good) for? Answers to these will ultimately guide efforts aimed at manipulating this new pathway for therapeutic benefit. In the six articles in this ICB Special Feature, the current state of play in necroptotic cell death research is dissected in considerable detail. The articles provide timely updates on what we have learnt so far and, importantly, where we might be going. Immunology & Cell Biology thanks the coordinator of this Special Feature ‐ James Vince ‐ for his planning and input. [ABSTRACT FROM AUTHOR]

Published

2017

3. NET formation can occur independently of RIPK3 and MLKL signaling.

Author

Amini, Poorya, Stojkov, Darko, Wang, Xiaoliang, Wicki, Simone, Kaufmann, Thomas, Wong, Wendy Wei‐Lynn, Simon, Hans‐Uwe, and Yousefi, Shida

Abstract

The importance of neutrophil extracellular traps (NETs) in innate immunity is well established but the molecular mechanisms responsible for their formation are still a matter of scientific dispute. Here, we aim to characterize a possible role of the receptor-interacting protein kinase 3 (RIPK3) and the mixed lineage kinase domain-like (MLKL) signaling pathway, which are known to cause necroptosis, in NET formation. Using genetic and pharmacological approaches, we investigated whether this programmed form of necrosis is a prerequisite for NET formation. NETs have been defined as extracellular DNA scaffolds associated with the neutrophil granule protein elastase that are capable of killing bacteria. Neither Ripk3-deficient mouse neutrophils nor human neutrophils in which MLKL had been pharmacologically inactivated, exhibited abnormalities in NET formation upon physiological activation or exposure to low concentrations of PMA. These data indicate that NET formation occurs independently of both RIPK3 and MLKL signaling. [ABSTRACT FROM AUTHOR]

Published

2016

4. Induction of Immunogenic Cell Death by Chemotherapeutic Platinum Complexes.

Author

Wong, Daniel Yuan Qiang, Ong, Wendy Wei Fang, and Ang, Wee Han

Subjects

*IMMUNE response, *TUMOR treatment, *CELL death, *PHAGOCYTOSIS, *CARBENES

Abstract

There is compelling evidence suggesting that the immune-modulating effects of many conventional chemotherapeutics, including platinum-based agents, play a crucial role in achieving clinical response. One way in which chemotherapeutics can engage a tumor-specific immune response is by triggering an immunogenic mode of tumor cell death (ICD), which then acts as an 'anticancer vaccine'. In spite of being a mainstay of chemotherapy, there has not been a systematic attempt to screen both existing and upcoming Pt agents for their ICD ability. A library of chemotherapeutically active Pt agents was evaluated in an in vitro phagocytosis assay, and no correlation between cytotoxicity and phagocytosis was observed. A PtII N-heterocyclic carbene complex was found to display the characteristic hallmarks of a type II ICD inducer, namely focused oxidative endoplasmic reticulum (ER) stress, calreticulin exposure, and both HMGB1 and ATP release, and thus identified as the first small-molecule immuno-chemotherapeutic agent. [ABSTRACT FROM AUTHOR]

Published

2015

5. IAPs limit activation of RIP kinases by TNF receptor 1 during development.

Author

Moulin, Maryline, Anderton, Holly, Voss, Anne K, Thomas, Tim, Wong, Wendy Wei-Lynn, Bankovacki, Aleksandra, Feltham, Rebecca, Chau, Diep, Cook, Wendy D, Silke, John, and Vaux, David L

Subjects

APOPTOSIS, TUMOR necrosis factor receptors, RECEPTOR-interacting proteins, PROTEIN kinases, ENZYME kinetics, CYTOKINE receptors, CELLULAR signal transduction

Abstract

Inhibitor of apoptosis (IAP) proteins cIAP1, cIAP2, and XIAP (X-linked IAP) regulate apoptosis and cytokine receptor signalling, but their overlapping functions make it difficult to distinguish their individual roles. To do so, we deleted the genes for IAPs separately and in combination. While lack of any one of the IAPs produced no overt phenotype in mice, deletion of cIap1 with cIap2 or Xiap resulted in mid-embryonic lethality. In contrast, Xiap−/−cIap2−/− mice were viable. The death of cIap2−/−cIap1−/− double mutants was rescued to birth by deletion of tumour necrosis factor (TNF) receptor 1, but not TNFR2 genes. Remarkably, hemizygosity for receptor-interacting protein kinase 1 (Ripk1) allowed Xiap−/−cIap1−/− double mutants to survive past birth, and prolonged cIap2−/−cIap1−/− embryonic survival. Similarly, deletion of Ripk3 was able to rescue the mid-gestation defect of cIap2−/−cIap1−/− embryos, as these embryos survived to E15.5. cIAPs are therefore required during development to limit activity of RIP kinases in the TNF receptor 1 signalling pathway. [ABSTRACT FROM AUTHOR]

Published

2012

6. Response to Heard et al.

Author

Moulin, Maryline, Voss, Anne K, Thomas, Tim, Wong, Wendy Wei‐Lynn, Cook, Wendy D, Koentgen, Frank, Vince, James, Silke, John, and Vaux, David L

Subjects

EXPERIMENTAL immunology, PERIODICAL editors, PERIODICAL publishing, PUBLISHING, MOLECULAR biology

Published

2015