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Phenological observations at the Botanical Garden of the Adam Mickiewicz University in Poznań were conducted on Syringa komarowii, S. meyeri, S. microphylla, S. oblata, S. reticulata, S. tomentella and S. wolfii. These observations showed the longest foliation phase in the case of S. oblata and S. meyeri, while the longest flowering phase was recorded in S. reticulata, S. microphylla and S. wolfii. Additionally, the longest period of anthesis (i.e. the period from the moment when 25% flowers bloomed to the time when 75% were out of bloom) was observed in S. oblata and S. microphylla. All examined shrubs, except for S. oblata, set fruits, which dispersal was extended to the next year (except for S. komarowii). In terms of decorative value suitable for green areas the most valuable species were S. komarowii, S. reticulata, S. meyeri, S. microphylla and S. oblata, with the three latter being the most showy shrubs in terms of autumn foliage. Moreover, S. komarowii was exceptional among the analysed species due to its large, attractive leaf blades. This lilac, together with S. meyeri, was also characterised by the most decorative inflorescences. Thanks to their stronger growth in comparison to the other species, S. komarowii, S. oblata and S. reticulata are best suited for large gardens, whereas S. meyeri and S. microphylla will prove most suitable for small gardens. All the recommended shrubs show good drought resistance.
In this paper the results of the 3-year observations (2001–2003) of seasonal rhythm of S. torminalis trees growing in Poznań in Dendrological Garden of Agricultural University and in forests of Wielkopolski National Park are presented. The observations included the course of leaf development, leaf coloration and leaf fall as well as flowering, fruit ripening and fall. Sixteen phenophases were taken into account. The differences in timing and duration of S. torminalis phenophases from year to year, between two sites and among trees within the same site are pointed out and discussed.
Ecteinascidia thurstoni is a colonial sea squirt. It has a seasonal rhythm and a tropical and subtropical distribution; it is usually present during the summer months. It synthesizes a group of molecules called ecteinascidins. One of these is ET-743, a compound that has a most original anti-tumoral activity and is today considered to be one of the most promising substances effective against various solid-type tumors (currently sold under the trade name of Yondelis for the treatment of sarcomas and related tumors; it is undergoing phase II/III clinical trails for other kinds of tumors). Worldwide, Ecteinascidia species represent the only available source of this bioactive compound, which was first discovered in E. turbinata. During the present study, the ecology of E. thurstoni along the Suez Canal and Red Sea was investigated. Its populations were observed to be highly gregarious due in part to their low larval dispersal, which is very localized; larvae therefore tend to settle close to their parent colonies. It is only recorded in shallow waters (0.5–1.5 m) as an epiphyte on the pneumatophores of mangroves by the Red Sea, on the pilings of jetties, and the metal or cement banks of the Suez Canal. The morphometric characteristics (zooid length, zooid weight, colony weight) of the Suez Canal population differ significantly from those of the Red Sea. Studying the distribution of this species and locating its different populations along the Suez Canal and Red Sea could help to characterize their genetics, chemistry and bacterial communities at different isolated locations. Ultimately, this will help to define the sources of ET-743 and hence promote its biosynthesis on a commercial scale.
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Gut clock: implication of circadian rhythms in the gastrointestinal tract

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Circadian and seasonal rhythms are a fundamental feature of all living organisms and their organelles. Biological rhythms are responsible for daily food intake; the period of hunger and satiety is controlled by the central pacemaker, which resides in the suprachiasmatic nucleus (SCN) of the hypothalamus, and communicates with tissues via bidirectional neuronal and humoral pathways. The molecular basis for circadian timing in the gastrointestinal tract (GIT) involves interlocking transcriptional/translational feedback loops which culminate in the rhythmic expression and activity of a set of clock genes and related hormones. Interestingly, it has been found that clocks in the GIT are responsible for the periodic activity (PA) of its various segments and transit along the GIT; they are localized in special interstitial cells, with unstable membrane potentials located between the longitudinal and circular muscle layers. The rhythm of slow waves is controlled in various segments of the GIT: in the stomach (about 3 cycles per min), in the duodenum (12 cycle per min), in the jejunum and ileum (from 7 to 10 cycles per min), and in the colon (12 cycles per min). The migrating motor complex (MMC) starts in the stomach and moves along the gut causing peristaltic contractions when the electrical activity spikes are superimposed on the slow waves. GIT hormones, such as motilin and ghrelin, are involved in the generation of MMCs, while others (gastrin, ghrelin, cholecystokinin, serotonin) are involved in the generation of spikes upon the slow waves, resulting in peristaltic or segmental contractions in the small (duodenum, jejunum ileum) and large bowel (colon). Additionally, melatonin, produced by neuro-endocrine cells of the GIT mucosa, plays an important role in the internal biological clock, related to food intake (hunger and satiety) and the myoelectric rhythm (produced primarily by the pineal gland during the dark period of the light-dark cycle). This appears to be an endocrine encoding of the environmental light-dark cycle, conveying photic information which is used by organisms for both circadian and seasonal organization. Motor and secretory activity, as well as the rhythm of cell proliferation in the GIT and liver, are subject to many circadian rhythms, mediated by autonomic cells and some enterohormones (gastrin, ghrelin and somatostatin). Disruption of circadian physiology, due to sleep disturbance or shift work, may result in various gastrointestinal diseases, such as irritable bowel syndrome (IBS), gastroesophageal reflux disease (GERD) or peptic ulcer disease. In addition, circadian disruption accelerates aging, and promotes tumorigenesis in the liver and GIT. Identification of the molecular basis and role of melatonin in the regulation of circadian rhythm allows researchers and clinicians to approach gastrointestinal diseases from a chronobiological perspective. Clinical studies have demonstrated that the administration of melatonin improves symptoms in patients with IBS and GERD. Moreover, our own studies indicate that melatonin significantly protects gastrointestinal mucosa, and has strong protective effects on the liver in patients with non-alcoholic steatohepatitis (NASH). Recently, it has been postulated that disruption of circadian regulation may lead to obesity by shifting food intake schedules. Future research should focus on the role of clock genes in the pathophysiology of the GIT and liver.
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