Identification of multiple HPV types on spermatozoa from human sperm donors

Human papillomaviruses (HPV) may cause sexually transmitted disease. High-risk types of HPV are involved in the development of cervical cell dysplasia, whereas low-risk types may cause genital condyloma. Despite the association between HPV and cancer, donor sperm need not be tested for HPV according to European regulations. Consequently, the potential health risk of HPV transmission by donor bank sperm has not been elucidated, nor is it known how HPV is associated with sperm. The presence of 35 types of HPV was examined on DNA from semen samples of 188 Danish sperm donors using a sensitive HPV array. To examine whether HPV was associated with the sperm, in situ hybridization were performed with HPV-6, HPV-16 and -18, and HPV-31-specific probes. The prevalence of HPV-positive sperm donors was 16.0% and in 66.7% of these individuals high-risk types of HPV were detected. In 5.3% of sperm donors, two or more HPV types were detected. Among all identified HPV types, 61.9% were high-risk types. In situ hybridization experiments identified HPV genomes particularly protruding from the equatorial segment and the tail of the sperm. Semen samples from more than one in seven healthy Danish donors contain HPV, most of them of high-risk types binding to the equatorial segment of the sperm cell. Most HPV-positive sperm showed decreased staining with DAPI, indicative of reduced content of DNA. Our data demonstrate that oncogenic HPV types are frequent in men.     

Messenger RNA recognition in Escherichia coli: a possible second site of interaction with 16S ribosomal RNA.

Examination of the nucleotides following the ATG or GTG initiation codons of a file of 251 genes from Escherichia coli has shown that 247 (98.4%) of them contain a sequence of at least three and 168 (66.9%) of them a sequence of at least four consecutive nucleotides that is complementary to some part of the 16 nt at the 5' terminus of the bacterial 16S rRNA. It is proposed that this sequence, which falls within the first 24 nt coding for the genetic message, might be involved in mRNA recognition through a mechanism analogous to the well-established 'Shine--Dalgarno' interaction with the 3' terminus of the 16S rRNA. Comparison of these data with data derived from a file of 117 'false' gene starts that have a Shine--Dalgarno-like sequence followed by a suitably spaced ATG or GTG triplet but which are believed not to lie at the beginnings of genetic messages shows the association that we have found to be statistically significant at the 99.9% level.     

Das piezoelektrische Verhalten der menschlichen Zahnhartgewebe

Zusammenfassung Bei menschlichen Zähnen wurde piezoelektrisches Verhalten festgestellt; dieses ist gebunden an den Kollagenfaseranteil des Dentins und des Zahnzementes. Schmelz ist nicht piezoelektrisch; entmineralisierte Zähne zeigen ein verstärktes piezoelektrisches Verhalten.Es besteht eine piezoelektrische Achse in der physiologischen Zahnlängsrichtung, deren Richtungssinn bei allen Zähnen des Ober- und Unterkiefers gleich ist und offenbar der morphogenetischen Entwicklungsrichtung des Zahnes entspricht. Außerdem besteht rund um die piezoelektrische Längsachse herum in allen radialen Richtungen zwischen Pulpahöhle und Zahnaußenseite piezoelektrisches Verhalten, das möglicherweise in Beziehung zur Struktur der Dentinlamellen und damit zur morphogenetischen Zahnentwicklung in radialer Richtung steht.Die piezoelektrischen Effekte zeigen von Zahn zu Zahn eine erhebliche biologische Streubreite. Bei unserem Untersuchungsmaterial lagen die Effekte zwischen 3,5·10^–10 und 1,9·10^–9 est E Ldg./dyn. Diese Werte entsprechen etwa 0,5 bis 2,8% des piezoelektrischen Koeffizienten d₁₁ von -Quarz.

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Summary Human teeth are piezoelectric. This is due to the collagen-fibril content of the dentine and tooth cement. Enamel is not piezoelectric; decalcified teeth show increased piezoelectric behaviour.There is a piezoelectrical axis corresponding to the physiological longitudinal tooth axis, which is in the same direction in all teeth of both upper and lower jaws, and which seems to correspond to the morphogenetical development axis of teeth. Piezoelectric behaviour also exists between the pulp cavity and outer surface of the tooth in all directions radial to the piezoelectric longitudinal axis. The latter is possibly due to the dentine lamellae, and therefore may be connected with the radial direction of morphogenetical tooth development.The piezoelectric effects show large biological variations in different teeth. The effects from our research materials vary between 3.5·10^–10 and 1.9·10^–9 e.s.u./dynes. These results correspond to about 0.5 to 2.8% of the piezoelectrical coefficient d₁₁ of -quartz.

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Unterstützt durch Sachbeihilfen der Deutschen Forschungsgemeinschaft.

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cand. med. dent. und derzeit Doktorand an der Klinik und Poliklinik für Zahn-, Mund- und Kieferkrankheiten, Universität Kiel.     

Distinct morphological and mito-inhibitory effects induced by TGF-β1, HGF and EGF on mouse,rat and human hepatocytes

TGF-1 is known as a potent inhibitor of proliferation of rat and human hepatocytes. In this study we show that the effects of TGF-1 are quite different on mouse hepatocytes. In rat and human hepatocytes, TGF-1 inhibited DNA synthesis and also inhibited the morphological changes induced by growth factors in rat and human hepatocytes. In contrast, addition of TGF-1 to mouse hepatocytes resulted in pronounced alterations in morphology of these cells. These changes were similar to those induced by HGF and EGF. The induction of structural changes by TGF-1 was noted only in mouse hepatocytes. Mouse hepatocytes were also much more resistant to the mito-inhibitory effect of TGF-1. These findings suggest profound differences in hepatocyte growth regulation between these species and may relate to observed differences in susceptibility to carcinogenesis.Abbreviations EGF epidermal growth factor - HGF hepatocyte growth factor - SF scatter factor - TGF-1 transforming growth factor beta type one     

Photoaffinity labelling of the TSH receptor on FRTL5 cells

An investigation of the properties of TSH receptors on FRTL5 cells using affinity labelling with a 125I-labelled photoactive derivative of TSH is described. Our studies suggest that FRTL5 cells contain 2 principal types of cell surface TSH receptors. One form, probably a precursor, consists of a single polypeptide chain (Mr 120,000) with an intrachain loop of amino acids formed by a disulphide bridge. The other type of receptor consists of a water-soluble A chain (Mr 55,000) linked to an amphiphilic B chain (Mr 35,000) by a disulphide bridge. The 2 chain structure is probably derived from the single chain 120,000 protein by enzymatic cleavage of peptide sequences within the loop of amino acids formed by the intrachain disulphide bridge.     

Effects of bicarbonate on fluid and electrolyte transport by the guinea pig gallbladder: A bicarbonate-chloride exchange

Summary Fluid transport and net fluxes of Na, K, Cl and HCO₃ by guinea pig gallbladder were investigatedin vitro. A perfused gallbladder preparation was devised to simultaneously study unidirectional fluxes of²²Na and³⁶Cl. The net Cl flux exceeded the net Na flux during fluid absorption in the presence of HCO₃. This Cl excess was counter-balanced by a net HCO₃ secretion: a HCO₃–Cl exchange. PGE₁ reversed the direction of fluid transport and abolished the net Cl flux. The magnitude of the HCO₃ secretion remained unchanged, but shifted from a HCO₃–Cl exchange to a net secretion of NaHCO₃ and KHCO₃. Furosemide inhibited both the HCO₃–Cl exchange and HCO₃ secretion after PGE₁ without influencing fluid absorption. Ouabain inhibited the HCO₃–Cl exchange as well as fluid absorption; only the effect on the HCO₃ secretion was entirely reversible. Secreted HCO₃ appeared not to be derived from metabolic sources since HCO₃ secretion was abolished in a HCO₃-free bathing medium. HCO₃ secretion was also dependent on the Na concentration of the bathing fluid. Three lines of evidence are presented in favor of an active HCO₃ secretion in guinea pig gallbladder. HCO₃ is secreted against: (i) a chemical gradient, (ii) an electrical gradient and (iii) the direction of fluid movement under control conditions.     

Defining dysbiosis and its influence on host immunity and disease

Mammalian immune system development depends on instruction from resident commensal microorganisms. Diseases associated with abnormal immune responses towards environmental and self antigens have been rapidly increasing over the last 50 years. These diseases include inflammatory bowel disease (IBD), multiple sclerosis (MS), type I diabetes (T1D), allergies and asthma. The observation that people with immune mediated diseases house a different microbial community when compared to healthy individuals suggests that pathogenesis arises from improper training of the immune system by the microbiota. However, with hundreds of different microorganisms on our bodies it is hard to know which of these contribute to health and more importantly how? Microbiologists studying pathogenic organisms have long adhered to Koch's postulates to directly relate a certain disease to a specific microbe, raising the question of whether this might be true of commensal–host relationships as well. Emerging evidence supports that rather than one or two dominant organisms inducing host health, the composition of the entire community of microbial residents influences a balanced immune response. Thus, perturbations to the structure of complex commensal communities (referred to as dysbiosis) can lead to deficient education of the host immune system and subsequent development of immune mediated diseases. Here we will overview the literature that describes the causes of dysbiosis and the mechanisms evolved by the host to prevent these changes to community structure. Building off these studies, we will categorize the different types of dysbiosis and define how collections of microorganisms can influence the host response. This research has broad implications for future therapies that go beyond the introduction of a single organism to induce health. We propose that identifying mechanisms to re‐establish a healthy complex microbiota after dysbiosis has occurred, a process we will refer to as rebiosis, will be fundamental to treating complex immune diseases.     

Signaling unmasked: Autophagy and catalase promote programmed cell death

Autophagy contributes to the removal of harmful cellular refuse, whereas catalase plays an important protective role by detoxifying reactive oxygen species. We recently found that autophagy and catalase are also required for promoting programmed cell death induced during plant immune responses. Here we discuss the difficulties in identifying cell death effectors, which are also required to maintain cellular homeostasis, and how their prodeath roles were unmasked using an unbiased forward genetics approach.     

Chromium distribution in subcellular components between fresh and starved subsurface bacterial consortium

Summary The distribution of chromium in subcellular components was examined with a fresh and starved denitrifying consortium by performing Cr⁺⁶ equilibration and cell fractionation tests. The cell wall fraction of 50 day starved cells adsorbed approximately 100% more chromium than did the cell wall fraction in fresh cells. The soluble fraction of 50 day old cells showed less affinity for chromium than fresh cells.