Intragroup cohesion and intergroup hostility: the relation between grooming distributions and intergroup competition among female primates

In some primate species, females interact affinitively withmany related and unrelated females, whereas in other speciesfemales interact with only a small subset of available partners.One explanation for high rates of affinitive interactions amongfemale members of the same group is that they function to maintainthe group's cohesion in competition for resources against othergroups. Here, I attempt to determine if grooming is more "egalitarian"or diverse in groups that compete aggressively with their neighborsthan in groups in which females rarely take an active role inbetween-group competition. Three types of data are considered.The first concerns grooming and intergroup encounters in onepopulation of free-ranging vervet monkeys. The second concernsgrooming interactions in a captive population of vervets beforeand after females in adjacent cages began to respond aggressivelyto one another. The third involves a literature survey of avariety of species. When only female-bonded species are considered,there is no relation between the diversity of grooming withingroups and female participationin intergroup encounters. Therealso appears to be no clear relation between the strength ofthe female dominance hierarchy and the diversity of groomingamong females. Female-bonded groups are apparently composedof subgroups allied in a loose confederation against other groups.Female members of the same group may compete against other groupsas a cohesive unit, but their grooming relationships are oftensharply differentiated.     

ARTIK-52 induces replication-dependent DNA damage and p53 activation exclusively in cells of prostate and breast cancer origin

The realization, that the androgen receptor (AR) is essential for prostate cancer (PC) even after relapse following androgen deprivation therapy motivated the search for novel types of AR inhibitors. We proposed that targeting AR expression versus its function would work in cells having either wild type or mutant AR as well as be independent of androgen synthesis pathways. Previously, using a phenotypic screen in androgen-independent PC cells we identified a small molecule inhibitor of AR, ARTIK-52. Treatment with ARTIK-52 caused the loss of AR protein and death of AR-positive, but not AR-negative, PC cells. Here we present data that ARTIK-52 induces degradation of AR mRNA through a mechanism that we were unable to establish. However, we found that ARTIK-52 is toxic to breast cancer (BC) cells expressing AR, although they were not sensitive to AR knockdown, suggesting an AR-independent mechanism of toxicity. Using different approaches we detected that ARTIK-52 induces replication-dependent double strand DNA breaks exclusively in cancer cells of prostate and breast origin, while not causing DNA damage, or any toxicity, in normal cells, as well as in non-PC and non-BC tumor cells, independent of their proliferation status. This amazing specificity, combined with such a basic mechanism of toxicity, makes ARTIK-52 a potentially useful tool to discover novel attractive targets for the treatment of BC and PC. Thus, phenotypic screening allowed us to identify a compound, whose properties cannot be predicted based on existing knowledge and moreover, uncover a barely known link between AR and DNA damage response in PC and BC epithelial cells.     

The PtdIns 3-Kinase/Akt Pathway Regulates Macrophage-Mediated ADCC against B Cell Lymphoma

Macrophages are important effectors in the clearance of antibody-coated tumor cells. However, the signaling pathways that regulate macrophage-induced ADCC are poorly defined. To understand the regulation of macrophage-mediated ADCC, we used human B cell lymphoma coated with Rituximab as the tumor target and murine macrophages primed with IFNγ as the effectors. Our data demonstrate that the PtdIns 3-kinase/Akt pathway is activated during macrophage-induced ADCC and that the inhibition of PtdIns 3-kinase results in the inhibition of macrophage-mediated cytotoxicity. Interestingly, downstream of PtdIns 3-kinase, expression of constitutively active Akt (Myr-Akt) in macrophages significantly enhanced their ability to mediate ADCC. Further analysis revealed that in this model, macrophage-mediated ADCC is dependent upon the release of nitric oxide (NO). However, the PtdIns 3-kinase/Akt pathway does not appear to regulate NO production. An examination of the role of the PtdIns 3-kinase/Akt pathway in regulating conjugate formation indicated that macrophages treated with an inhibitor of PtdIns 3-kinase fail to polarize the cytoskeleton at the synapse and show a significant reduction in the number of conjugates formed with tumor targets. Further, inhibition of PtdIns 3-kinase also reduced macrophage spreading on Rituximab-coated surfaces. On the other hand, Myr-Akt expressing macrophages displayed a significantly greater ability to form conjugates with tumor cells. Taken together, these findings illustrate that the PtdIns 3-kinase/Akt pathway plays a critical role in macrophage ADCC through its influence on conjugate formation between macrophages and antibody-coated tumor cells.     

How vervet monkeys perceive their grunts: Field playback experiments

Free-ranging vervet monkeys grunt to each other in a variety of social situations: when approaching a dominant or subordinate individual, when moving into a new area of their range, or when observing another group. Like other non-human primate vocalizations, these grunts have traditionally been interpreted as a single, highly variable call that reflects the arousal state of the signaller. Field playback experiments suggest, however, that what humans initially perceive as one grunt the monkeys perceive as at least four. Each grunt carries a specific meaning that seems to depend more on its acoustic properties than on the context in which it occurs. Results suggest that the vocalizations given by monkeys during social interactions may function in a rudimentary representational manner, as if to designate objects or events in the external world.     

Effects of acute and chronic morphine on regional rat brain acetylcholine turnover rate

A simplified method to study the acetylcholine (ACh) turnover rate (TR_ACh) in brain parts of drug treated rats has been presented. In striatum and occipital cortex of rats receiving a large dose of morphine (140 μ moles/kg i.p.) or implanted chronically with morphine pellets, the TR_ACh is influenced in a different manner. The single injection of morphine reduced the synthesis of ACh in cortex but not in striatum. Morphine pellets decreased striatal TR_ACh but failed to alter the TR_ACh in occipital cortex. Naloxone reversed both changes of TR_ACh elicited by morphine although it was devoid of any effect of the synthesis of ACh in rat brain parts. We suggest that morphine may prevent the ACh release from neurons as proposed by others, however, this effect in striatum of rats receiving a single dose of morphine is masked by the simultaneous action of morphine on the dopaminergic nigrostriatal pathway which regulates the turnover rate of striatal ACh.     

Measurement of acetylcholine turnover rate in discrete areas of rat brain

The turnover rate of ACh was estimated in brain stem, two cortical areas and striatum of rat brain. The turnover rate was highest in the striatum (1.3 μmoles/g/hr); lowest in brain stem (0.092 μmoles/g/hr); and intermediate values were observed in limbic and occipital cortex. The highest ACh concentrations were measured in striatum, those in brain stem were intermediate but in the two cortical areas the ACh concentrations were the lowest. The results of the turnover estimations with the finite difference method yielded values similar to those obtained with the procedure described in this paper. Moreover, once the baseline was established, this method could be reliably used to estimate turnover rate using a single infusion time. The latter simplication would be very useful to compare ACh turnover rate in drug studies.