ARP101 inhibits α-MSH-stimulated melanogenesis by regulation of autophagy in melanocytes

Autophagy is a cooperative process between autophagosomes and lysosomes that degrades cellular organelles. Although autophagy regulates the turnover of cellular components, its role in melanogenesis is not clearly established. Previously, we reported that ARP101 induces autophagy in various cancer cells. Here, we show that ARP101 inhibits melanogenesis by regulation of autophagy. ARP101 inhibited α-MSH-stimulated melanin synthesis and suppressed the expression of tyrosinase and TRP1 in immortalized mouse melanocytes. ARP101 also induced autophagy in melanocytes. Knockdown of ATG5 reduced both anti-melanogenic activity and autophagy mediated by ARP101 in α-MSH treated melanocytes. Electron microscopy analysis further revealed that autophagosomes engulf melanin or melanosome in α-MSH and ARP101-treated cells. Collectively, our results suggest that ARP101 inhibits α-MSH-stimulated melanogenesis through the activation of autophagy in melanocytes.     

Towards quantitative cytotaxonomy of primates: Idiogram construction of great ape chromosomes by «fourier-warping»

To faciliate quatitative comparative cytogenetics of primate chromosomes we present a new type of idiogram from human and great ape chromosomes. These idiograms were obtained by computer densitometry and «Fourier-Warping» (FW) as described elsewhere (Maurier & Wienberg, 1991). In contrast to published idiograms, the «FW-idiograms» represent the mean position, width and density of each band and the mean resolution of the chromosome sample under investigation. In species that deverged about 6–12 my we were able to extract the representative banding features and to demonstrate conservation and change in the karyotype of human and great apes.     

« Chaetopsina ivoriensis » a new species of Dematiaceous Hyphomycetes

Abstract

The discover and morphological characters of a Dematiaceous Hyphomycetes are described. The material, studied under a morphological point of view directly collected on the natural substratum, allows us to establish the appartenance to the genus Chaetopsina. Since this species does not appeare described till now, the Authors propose for it the nomenclature ivoriensis as a new species.     

«Active» selection may participate in the evolution of primates

Selection pressures in the evolution of morphological characters which are exclusive to primates were discussed. While the evolutionary change in some morphological characters of primates can be explained by natural or sexual selection, there are also morphological characters of primates, such as some regions of neocortices, which are involved in social interactions and whose evolutionary changes can hardly be explained by natural or sexual selection alone. Furthermore, recent studies have demonstrated that relative sizes of brain, neocortex and some thalamic nuclei of brains differ significantly by social structure in primates. Based on these and other findings, we propose here that “active” selection pressures may have favored a variety of morphological characters related to social interactions, the selection pressures which are derived from social interactions and are operative within animals or troops. The introduction of concept of active selection will be useful in developing conceptual frameworks for understanding of the mechanism of evolution of primates, in particular, of hominids.     

Molecular basis of the regulation of Beclin 1-dependent autophagy by the γ-herpesvirus 68 Bcl-2 homolog M11

γ-Herpesviruses (γHVs), including important human pathogens such as Epstein Barr virus, Kaposi’s sarcoma-associated HV, and the murine γHV68, encode homologs of the anti-apoptotic, cellular Bcl-2 (cBcl-2) to promote viral replication and pathogenesis. The precise molecular details by which these proteins function in viral infection are poorly understood. Autophagy, a lysosomal degradation pathway, is inhibited by the interaction of cBcl-2s with a key autophagy effector, Beclin 1, and can also be inhibited by γHV Bcl 2s. Here we investigate the γHV68 M11-Beclin 1 interaction in atomic detail, using biochemical and structural approaches. We show that the Beclin 1 BH3 domain is the primary determinant of binding to M11 and other Bcl 2s, and this domain binds in a hydrophobic groove on M11, reminiscent of the binding of different BH3 domains to other Bcl-2s. Unexpectedly, regions outside of, but contiguous with, the Beclin 1 BH3 domain also contribute to this interaction. We find that M11 binds to Beclin 1 more strongly than do KSHV Bcl-2 or cBcl-2. Further, the differential affinity of M11 for different BH3 domains is caused by subtle, yet significant, variations in the atomic details of each interaction. Consistent with our structural analysis, we find that Beclin 1 residues L116 and F123, and M11 residue pairs G86+R87 and Y60+L74, are required for M11 to bind to Beclin 1 and down-regulate autophagy. Thus, our results suggest that M11 inhibits autophagy through a mechanism that involves the binding of the Beclin 1 BH3 domain in the M11 hydrophobic surface groove.     

Foreword: Predicting the responses of animals to their nutrients - quo vadimus?

For its 2006 Annual Meeting BSAS organised an invited session on ‘Responses to Nutrients’. The session was appropriately chaired by Professor Colin Whittemore, who was responsible for the first systematic approach to the integration of information about an animal its feed and the environment in which it was kept, with a view to predicting its responses and simulating its performance (Whittemore and Fawcett, 1976). In his usual indomitable fashion Professor Whittemore questioned whether there was a need for such a session. Was there anything that we did not already about know animals responded to their intake of nutrients? After all models of growth for pigs and poultry have in the past 30 years been able not only to predict such responses, but at the same time to deal with the more challenging task of voluntary feed intake prediction. Such models have been used increasingly to optimise feed and feeding programmes in pig and poultry enterprises worldwide. On the other hand, in ruminants many applied feeding models are still largely based on meeting animal requirements.     

Mechanism of NF-κB signaling pathway and autophagy in the regulation of osteoblast differentiation

Objective: The objective of the present work was to investigate a possible mechanism of NF-κB signaling pathway and autophagy in the regulation of osteoblast differentiation, and provide experimental basis for the study of tooth eruption disorder.

Methods: Mouse osteoblast-like (MC3T3-E1) cells were inoculated with a cell density of 70%. According to the grouping experimental design, Western blot and monodansylcadaverine (MDC) detection were conducted after dosing for 24?h. The cells were divided into the following five groups: blank control group; 6.25?µg/mL SN50 group; 12.5?µg/mL SN50 group; 25?µg/mL SN50 group and 50?µg/mL SN50 group.

Results: Western blot analysis revealed that the expression of LC3 protein was present in the blank control group; 6.25?µg/mL SN50 group; 12.5?µg/mL SN50 group and 50?µg/mL SN50 group, with no significant differences among these groups. However, the expression of LC3 protein was significantly lower in the 25?µg/mL SN50 group. MDC detection showed that, in the blank control group; 6.25?µg/mL SN50 group; 12.5?µg/mL SN50 group and 50?µg/mL SN50 group, there was obvious green fluorescence in the cytoplasm of the osteoblasts. However, in the 25?µg/mL SN50 group, it was found that there were significantly fewer green fluorescent particles.

Conclusion: The osteoblast itself had a strong function of autophagy. The appropriate concentration of SN50 in blocking the NF-κB pathway of the osteoblast was associated with the obvious inhibition of autophagy. However, the relationship between NF-κB signaling pathway and autophagy in the process of tooth eruption requires further study.     

Ultrastructural characteristics of « Diplotaxis erucoides (L.) DC. » suspensor

Abstract

The development and general morphology of Diplotaxis erucoides (L.) DC. suspensor is of the « Onagrad Type », « Alyssum Variation ». Maximum growth of the suspensor occurs from the globular to the early heart stage of embryo development. The suspensor starts then to degenerate disintegrating shortly after the torpedo stage of the embryo.

The wall ingrowths of the long, tapering, basal cell are especially abundant at the cell's micropilar pole which is closely surrounded by well developed wall ingrowths formed by the endosperm. Wall ingrowths and plasmodesmata are present on the suspensor cells cross walls with the exception of the cell closest to the embryo. No such structures in fact are present on the walls separating this last cell both from the embryo and from the rest of the suspensor. Wall ingrowths are generally associated with numerous, large, mitochondria.

The morphological data seem to indicate that absorption and transport of nutrients from the surrounding tissues is a main function of the suspensor. The possibility of an elaborative and secretory function of this structure is discussed.     

HucMSC exosome-transported 14-3-3ζ prevents the injury of cisplatin to HK-2 cells by inducing autophagy in vitro

Background aims

On the basis of previous studies, exosomes secreted by human umbilical cord mesenchymal stromal cell (hucMSC-ex) could prevent and repair acute kidney injury induced by cisplatin in rats. However, its potential mechanism is still unclear. In the present study, the model with hucMSC-ex pretreated human renal tubular epithelial cell lines HK-2 that could prevent the injury of cisplatin was successfully established.

Biphasic and dosage-dependent regulation of osteoclastogenesis by β-catenin

Wnt/β-catenin signaling is a critical regulator of skeletal physiology. However, previous studies have mainly focused on its roles in osteoblasts, while its specific function in osteoclasts is unknown. This is a clinically important question because neutralizing antibodies against Wnt antagonists are promising new drugs for bone diseases. Here, we show that in osteoclastogenesis, β-catenin is induced during the macrophage colony-stimulating factor (M-CSF)-mediated quiescence-to-proliferation switch but suppressed during the RANKL-mediated proliferation-to-differentiation switch. Genetically, β-catenin deletion blocks osteoclast precursor proliferation, while β-catenin constitutive activation sustains proliferation but prevents osteoclast differentiation, both causing osteopetrosis. In contrast, β-catenin heterozygosity enhances osteoclast differentiation, causing osteoporosis. Biochemically, Wnt activation attenuates whereas Wnt inhibition stimulates osteoclastogenesis. Mechanistically, β-catenin activation increases GATA2/Evi1 expression but abolishes RANKL-induced c-Jun phosphorylation. Therefore, β-catenin exerts a pivotal biphasic and dosage-dependent regulation of osteoclastogenesis. Importantly, these findings suggest that Wnt activation is a more effective treatment for skeletal fragility than previously recognized that confers dual anabolic and anti-catabolic benefits.