Janospira - an Ordovician microfossil in search of a Phylum

Janospira is described from early Ordovician (Arenig) rocks of northern Spitsbergen. It is a curious microfossil, probably calcareous, about 1 mm in length, made up of an initial coil which expands distally into a straight tube, at the same time as producing a narrower tube almost in line with the first but in the opposite direction. Although showing some similarities to Foraminifera, molluscs and polychaetes, there are objections to its inclusion in any of these groups, and it is equally probable that it belongs to an unknown group with a planktic early growth stage.     

Chemical synthesis of a tetradecamer in the deoxyribonucleic acid series

The chemical synthesis of a tetradecadeoxyribonucleotide, d-EtSp(A-T-G-G-A-A-A-C-T-G-C-G-G-C), is described. This oligomer, designated Fragment 4δ, constitutes the 5′-terminus of the plus strand of a projected duplex coding for S-Peptide_2–14 derived from Ribonuclease A. The Fragment was constructed by block condensation via a phosphorothioate anchor. Complications due to inadvertent phosphotriester condensations are discussed. Arguments justifying the sequence selection are presented.     

Internal Rhythmic Pattern of ECG Signal and the Efficiency of Adaptation to Cyclic Muscular Work

Spectral, coherent, and phase analysis within the low-frequency range of ECG records of athletic runners revealed that oscillations of ECG intervals (PQ-, RT-, P–T-, TP, and PP-intervals) were observed during orthostasis. These data were compared with the results of athletic exercise tests performed after the ECG examination. It was shown that the most effective type of adaptive reaction in these tests corresponds to a phase advance of the PQ-interval oscillations relative to the RT-interval oscillations. In the low-frequency range, the phases of the PQ-, RT-, and (P–T)-interval oscillations were ahead of the TP-interval oscillations, whereas the spectral density of the TP interval oscillations was significantly higher than the spectral density of the oscillations of the PC-, RT-, and (P–T)-intervals measured at the same frequency. The least effective type of adaptive reaction was shown to correlate with the phase advance of the TP-interval oscillations relative to the PQ-, RT-, and (P–T)-interval oscillations within the low-frequency range as well as with the lack of low-frequency modulation of the autospectra of the cardiac intervals of interest.     

The mutagenicity of 5-azacytidine and other inhibitors of replicative DNA synthesis in the L5178Y mouse lymphoma cell

The mutagenic potential of the cytidine analog, 5-azacytidine (Aza Cyd), was tested at the thymidine kinase (TK) gene locus of L5178Y mouse lymphoma cells. 3-h exposure to as little as 20 ng/ml Aza Cyd yielded a substantial increase in TK-deficient L5178Y cells as measured by drug-induced resistance to trifluorothymidine (TFTres) 48 h later. This mutagenic effect was diminished up to 75% when Aza Cyd was tested in the presence of either enzymatically active or heat-denatured 9000 X g supernatant prepared from rat liver homogenate. The mutagenicity of Aza Cyd was also decreased in the presence of 1-5 X 10(-3) M thymidine and eliminated in the presence of greater than 1 X 10(-5) M cytidine. Two L5178Y TK-deficient cell lines had no selective survival advantage compared to TK-competent L5178Y cell stock when plated in soft-agar medium that contained Aza Cyd. Four other specific inhibitors of scheduled DNA synthesis in mammalian cells, deoxyadenosine, aphidicolin, 1-beta-D-arabinofuranosylcytosine, and hydroxyurea were also L5178Y/TK mutagens. These data along with other published results suggest that chemicals known to disrupt nucleotide biosynthesis, alter deoxyribonucleotide pools, or directly inhibit DNA polymerase can cause stable, heritable increases in TFT resistance through mechanisms dependent upon altered replicative DNA synthesis, yet not necessarily dependent upon DNA incorporation or the binding of these mutagenic agents to nuclear DNA.