Complement C1q-induced activation of β-catenin signalling causes hypertensive arterial remodelling

Sumida, Tomokazu; Naito, Atsuhiko T.; Nomura, Seitaro; Nakagawa, Akito; Higo, Tomoaki; Hashimoto, Akihito; Okada, Katsuki; Sakai, Tomohiro; Ito, Masamichi; Yamaguchi, Toshihiro; Oka, Tôru; Akazawa, Hiroshi; Lee, Jong-Kook; Minamino, Tohru; Offermanns, Stefan; Noda, Tetsuo; Botto, Marina; Kobayashi, Yoshio; Morita, Hiroyuki; Manabe, Ichiro; Nagai, Toshio; Shiojima, Ichiro; Komuro, Issei

doi:10.1038/ncomms7241

Cited by 50 publications

(45 citation statements)

References 42 publications

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“…We also demonstrated decreased levels of C1qa , a polypeptide chain of complement subcomponent C1q. Complement C1q-induced activation of β-catenin signaling has recently been shown to contribute to hypertensive arterial remodeling [45]. Contrary to our expectations, C1qa levels were decreased in our FR placentas, again highlighting the inconsistencies of whether cellular protective mechanisms are impaired or enhanced in response to adverse environments in these pathologic conditions of pregnancy.…”

Section: Discussioncontrasting

confidence: 97%

Gestational food restriction decreases placental interleukin-10 expression and markers of autophagy and endoplasmic reticulum stress in murine intrauterine growth restriction

Chu¹,

Thamotharan²,

Ganguly³

et al. 2016

Nutrition Research

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Intrauterine growth restriction (IUGR) affects up to 10% of pregnancies and often results in short- and long- term sequelae for offspring. The mechanisms underlying IUGR are poorly understood, but it is known that healthy placentation is essential for nutrient provision to fuel fetal growth, and is regulated by immunologic inputs. We hypothesized that in pregnancy, maternal food restriction (FR) resulting in IUGR would decrease the overall immunotolerant milieu in the placenta, leading to increased cellular stress and death. Our specific objectives were to evaluate: (1) key cytokines (e.g. IL10) that regulate maternal-fetal tolerance, (2) cellular processes (autophagy and ER stress) that are immunologically-mediated and important for cellular survival and functioning, and (3) evaluate the resulting IUGR phenotype and placental histopathology. After subjecting pregnant mice to mild and moderate FR from gestational day (GD) 10 to 19, we collected placentas and embryos at GD19. We examined RNA sequencing data to identify immunologic pathways affected in IUGR-associated placentas and validated mRNA expression changes of genes important in cellular integrity. We also evaluated histopathologic changes in vascular and trophoblastic structures as well as protein expression changes in autophagy, ER stress, and apoptosis in the mouse placentas. Several differentially expressed genes were identified in FR compared to control mice, including a considerable subset that regulates immune tolerance, inflammation and cellular integrity. In summary, maternal food restriction decreases anti-inflammatory effect of IL10 and suppresses placental autophagic and ER stress responses, despite evidence of dysregulated vascular and trophoblast structures leading to IUGR.

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Section: Discussioncontrasting

confidence: 97%

Gestational food restriction decreases placental interleukin-10 expression and markers of autophagy and endoplasmic reticulum stress in murine intrauterine growth restriction

Chu¹,

Thamotharan²,

Ganguly³

et al. 2016

Nutrition Research

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“…Since aberrant Wnt signaling is implicated in cancer and other degenerative diseases 75 , complement components may promote Wnt-dependent degenerative phenotypes during aging. In support of this notion, C1q was shown to promote hypertension-induced arterial remodeling through enhanced β-catenin signaling and aberrant proliferation of vascular smooth muscle cells 76 . Interestingly, complement downmodulates the expression of Klotho, a transmembrane co-receptor for FGF signaling that exerts pleiotropic anti-aging functions in various tissues 77 .…”

Section: Complement In Inflammatory Diseasesmentioning

confidence: 90%

Novel mechanisms and functions of complement

et al. 2017

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Progress in the beginning of the 21st century transformed our perception of complement from a blood-based antimicrobial system to a global regulator of immunity and tissue homeostasis. More recent years have witnessed remarkable advances regarding structure-function insights, mechanisms and locations of complement activation, thereby adding new layers of complexity in the biology of complement. This complexity is readily reflected by the multifaceted and contextual involvement of complement-driven networks in a wide range of inflammatory and neurodegenerative disorders and cancer. This Review provides an updated view of new and previously unanticipated functions of complement and how these impact immunity and disease pathogenesis.

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“…For example, C1q has been reported to play an important role in nerve pruning (Stevens et al, 2007) Wnt/Beta-catenin signalling (Naito et al, 2012;Sumida et al, 2015). Also a role for C1q was reported on neoangiogenesis (Bossi et al, 2014).…”

Section: C1q Traditional and Non-traditional Rolesmentioning

confidence: 96%