Sphingomyelin synthase 1 enhances BCR signaling to promote lupus-like autoimmune response

Wang, Chenqiong; Ming, Bingxia; Wu, Xiaoqian; Wu, Tong; Cai, Shaozhe; Hu, Peng; Tang, Jungen; Tan, Zheng; Liu, Chaohong; Zhong, Jixin; Zheng, Fang; Dong, Lingli

doi:10.1016/j.ebiom.2019.06.038

Cited by 9 publications

(10 citation statements)

References 41 publications

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“…A recent study showed that SMS1 deficiency suppressed B-cell activation and lupus-like autoimmunity such as systemic lupus erythematosus (SLE). 115 In an in vitro culture system of B cells, IgM-mediated activation and differentiation into plasma cells were suppressed in SMS1 deficient cells. Interestingly, supplementation of SM in the culture media recovered both activation and differentiation in SMS1-KO B cells.…”

Section: Phenotypes Of Smss-ko Mice In Disease Modelsmentioning

confidence: 99%

Ceramide/Sphingomyelin Rheostat Regulated by Sphingomyelin Synthases and Chronic Diseases in Murine Models

Taniguchi

Okazaki

2020

J Lipid Atheroscler

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Ceramide and sphingomyelin (SM) are major components of the double membranebound sphingolipids. Ceramide is an essential bioactive lipid involved in numerous cell processes including apoptosis, necrosis, and autophagy-dependent cell death. Inversely, SM regulates opposite cellular processes such as proliferation and migration by changing receptor-mediated signal transduction in the lipid microdomain. SM is generated through a transfer of phosphocholine from phosphatidylcholine to ceramide by SM synthases (SMSs). Research during the past several decades has revealed that the ceramide/SM balance in cellular membranes regulated by SMSs is important to decide the cell fate, survival, and proliferation. In addition, recent experimental studies utilizing SMS knockout mice and murine disease models provide evidence that SMS-regulated ceramide/SM balance is involved in human diseases. Here, we review the basic structural and functional characteristics of SMSs and focus on their cellular functions through the regulation of ceramide/SM balance in membrane microdomains. In addition, we present the pathological or physiological implications of SMSs by analyzing their role in SMS-knockout mice and human disease models. This review finally presents evidence indicating that the regulation of ceramide/SM balance through SMS could be a therapeutic target for human disorders.

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Section: Phenotypes Of Smss-ko Mice In Disease Modelsmentioning

confidence: 99%

Ceramide/Sphingomyelin Rheostat Regulated by Sphingomyelin Synthases and Chronic Diseases in Murine Models

Taniguchi

Okazaki

2020

J Lipid Atheroscler

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“…In addition, although 2OHOA can activate both SMS1 and SMS2, we believe that its therapeutic effect on lupus is achieved via activation of SMS2. This is because a recent study showed that systemic SMS1 deficiency attenuated the pathogenesis of lupus in pristane and bm12 models (Wang et al, 2019), in which innate immune responses play a central regulatory role in pathogenesis (Han et al, 2017;Shi et al, 2014;Zhao et al, 2007). Therefore, the evidence points to SMS2 as the primary target of 2OHOA in autoreactive dsDNA-specific GC B cells, in keeping with the highly upregulated expression of SMS2, but not SMS1, in these cells (Figure 4).…”

Section: Discussionmentioning

confidence: 70%

SMS2 deficiency impairs PKCδ-regulated B cell tolerance in the germinal center

Stanek

Huan

et al. 2021

Cell Reports

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“…47 Moreover, T-and B-cell activations through their receptors were prevented by SM depletion of DRMs in SMS1-KO mice, resulting in SM-deficient amelioration of hepatitis or systemic lupus erythematosus, but not in SMS2-KO mice. 19,48 Furthermore, JEV can achieve infection by attaching to target cell membranes through SMS1-generated SM. 23 Consequently, SMS1-KO mice are protected from JEV infection and JEV-mediated encephalitis.…”

Section: Discussionmentioning

confidence: 99%

A novel mechanism of thrombocytopenia by PS exposure through TMEM16F in sphingomyelin synthase 1 deficiency

Fujii¹,

Taniguchi²,

Nagaya

et al. 2021

Blood Advances

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Sphingomyelin synthase 1 (SMS1) contributes to the generation of membrane sphingomyelin (SM) and affects SM-mediated physiological functions. Here, we describe the hematologic phenotypes, such as reduced circulating platelets and dysfunctional hemostasis, in SMS1-deficient (SMS1-KO) mice. SMS1-KO mice display pathologic manifestations related to idiopathic thrombocytopenia (ITP), including relatively high amounts of peripheral blood reticulated platelets, enhanced megakaryopoiesis in the bone marrow and spleen, and splenomegaly. Deficiency of SMS1, but not SMS2, prevented SM production and enhanced phosphatidylserine (PS) externalization on the plasma membranes of platelets and megakaryocytes. Consequently, SMS1-KO platelets were excessively cleared by macrophages in the spleen. Multimer formation in the plasma membrane of TMEM16F, a known calcium (Ca2+)-activated nonselective ion channel and Ca2+-dependent PS scramblase, was enhanced; the result was PS externalization to outer leaflets through increased Ca2+ influx in immortalized mouse embryonic fibroblasts established from SMS1-KO mice (SMS1-KO tMEFs), as seen with SMS1-KO platelets. Thus, SMS1 deficiency changed the TMEM16F distribution on the membrane microdomain, regulating Ca2+ influx-dependent PS exposure. SMS1-KO tMEFs in which TMEM16F was knocked out by using the CRISPR/Cas9 system lacked both the Ca2+ influx and excess PS exposure seen in SMS1-KO tMEFs. Therefore, SM depletion on platelet membrane microdomains due to SMS1 deficiency enhanced PS externalization via a Ca2+ influx through TMEM16F activation, leading to elevated platelet clearance and causing hemostasis dysfunction through thrombocytopenia. Our current findings show that the SM-rich microdomain generated by SMS1 is a potent regulator of thrombocytopenia through TMEM16F, suggesting that its dysfunction may be a novel additional mechanism of ITP.

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Sphingomyelin synthase 1 enhances BCR signaling to promote lupus-like autoimmune response

Cited by 9 publications

References 41 publications

Ceramide/Sphingomyelin Rheostat Regulated by Sphingomyelin Synthases and Chronic Diseases in Murine Models

Ceramide/Sphingomyelin Rheostat Regulated by Sphingomyelin Synthases and Chronic Diseases in Murine Models

SMS2 deficiency impairs PKCδ-regulated B cell tolerance in the germinal center

A novel mechanism of thrombocytopenia by PS exposure through TMEM16F in sphingomyelin synthase 1 deficiency

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