A transient species of poly(A)+ RNA detected by a myosin heavy chain cDNA probe in muscle cell culture during terminal differentiation

Primary cell cultures were prepared from breast muscles of 11 day 4 hour-embryonic chicks. Cytoplasmic RNAs were isolated from the cultured cells at various time intervals from day 3 to day 8. A [P32] DNA probe complementary to messenger RNA of myosin heavy chain was used to hybridize with the RNAs after gel electrophoresis. A transient species of polyadenylated RNA with a decreased mobility in electrophoresis was detected during a period of time when contractions of syncytial fibers were first observed.     

Single-cell landscape of the ecosystem in early-relapse hepatocellular carcinoma

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Involvement of Kv1.3 and p38 MAPK signaling in HIV-1 glycoprotein 120-induced microglia neurotoxicity

Inflammatory responses mediated by activated microglia play a pivotal role in the pathogenesis of human immunodeficiency virus type 1 (HIV-1)-associated neurocognitive disorders. Studies on identification of specific targets to control microglia activation and resultant neurotoxic activity are imperative. Increasing evidence indicate that voltage-gated K⁺ (K_v) channels are involved in the regulation of microglia functionality. In this study, we investigated K_v1.3 channels in the regulation of neurotoxic activity mediated by HIV-1 glycoprotein 120 (gp120)-stimulated rat microglia. Our results showed treatment of microglia with gp120 increased the expression levels of K_v1.3 mRNA and protein. In parallel, whole-cell patch-clamp studies revealed that gp120 enhanced microglia K_v1.3 current, which was blocked by margatoxin, a K_v1.3 blocker. The association of gp120 enhancement of K_v1.3 current with microglia neurotoxicity was demonstrated by experimental results that blocking microglia K_v1.3 attenuated gp120-associated microglia production of neurotoxins and neurotoxicity. Knockdown of K_v1.3 gene by transfection of microglia with K_v1.3-siRNA abrogated gp120-associated microglia neurotoxic activity. Further investigation unraveled an involvement of p38 MAPK in gp120 enhancement of microglia K_v1.3 expression and resultant neurotoxic activity. These results suggest not only a role K_v1.3 may have in gp120-associated microglia neurotoxic activity, but also a potential target for the development of therapeutic strategies.     

Isoliquiritigenin prevents hyperglycemia-induced renal injuries by inhibiting inflammation and oxidative stress via SIRT1-dependent mechanism

Diabetic nephropathy (DN) as a global health concern is closely related to inflammation and oxidation. Isoliquiritigenin (ISL), a natural flavonoid compound, has been demonstrated to inhibit inflammation in macrophages. Herein, we investigated the effect of ISL in protecting against the injury in STZ-induced type 1 DN and in high glucose-induced NRK-52E cells. In this study, it was revealed that the administration of ISL not only ameliorated renal fibrosis and apoptosis, but also induced the deterioration of renal function in diabetic mice. Mediated by MAPKs and Nrf-2 signaling pathways, respectively, upstream inflammatory response and oxidative stress were neutralized by ISL in vitro and in vivo. Moreover, as further revealed by the results of molecular docking, sirtuin 1 (SIRT1) binds to ISL directly, and the involvement of SIRT1 in ISL-mediated renoprotective effects was confirmed by studies using in vitro models of SIRT1 overexpression and knockdown. In summary, by reducing inflammation and oxidative stress, ISL has a significant pharmacological effect on the deterioration of DN. The benefits of ISL are associated with the direct binding to SIRT1, the inhibition of MAPK activation, and the induction of Nrf-2 signaling, suggesting the potential of ISL for DN treatment.Subject terms: Pharmacology, Molecular biology     

四川省自然保护区时空分布与影响因素

自然保护区是为保护具有代表性的生态系统和濒危动植物而划分的特定区域,在涵养水土,防风固沙、净化空气、保护生物多样性等方面发挥着重要作用。四川省有自然保护区166处,类型丰富多样,是中国自然保护地体系的重要组成部分,其保护对象涵盖珍稀动植物,保护功能涉及物种、水源和生态环境,与国家地质公园、湿地公园、森林公园等共同维系着中国西南地区,乃至青藏高原东缘的生态系统。因此,研究四川省自然保护区的空间分布格局及其影响因素具有重要的价值和意义。运用地理空间分析方法对1963-2018年间四川省自然保护区的空间分布和影响因素进行了研究。研究发现:①四川省自然保护区空间分布的总体特征以集聚为主,呈现集聚-随机-集聚的变化特征,且前期变化幅度大,后期变化幅度小,总体发展明显分为1963-1998年的单核形成与发展阶段和1998-2018年的双核阶段;②四川省自然保护区主要分布在成都平原向川西高原的过渡区域,其均衡度类型在时间上表现出由"差距悬殊"到"差距较大"的演变特征;③四川省自然保护区的重心活动范围相对较小,基本稳定在阿坝州南部。标准差椭圆的长短半轴和面积均变化强烈,总体呈现出大幅度的增长,空间分布由南-北向演变为东北-西南向;④自然保护区受到自然因素和社会因素的双重影响,高密度区域分布在地势适中、气候温和、河流众多、土壤肥沃、人口稀少的阿坝州南部与东部地区。未来,四川省生态功能建设应该立足国家公园、自然保护区和自然公园的特点、分布状况,对自然保护区分布较少的川西北、川东北和川南部分地区进行优化布局,以加强这些地区的生态功能建设。同时,探索自然保护区的发展模式,实现自然保护区与周边区域社会经济的协调发展。