Suppression of c-myc and c-myb expression in myeloid cell lines treated with recombinant tumor necrosis factor-alpha

Proto-oncogenes are thought to be involved in cellular differentiation and proliferation. Tumor necrosis factors (TNFs) are specific cytokines that have cytostatic and cytotoxic effects in vitro against a wide range of human tumor cells. We have previously demonstrated that recombinant TNFs (rTNFs) have an antiproliferative effect on certain human leukemic cell lines (HL-60, KBM3, KBM5) and no effect on others (K562). To study the possible role of the c-myc and c-myb oncogenes in this antiproliferative effect of TNF, we examined their expression in cell lines HL-60, KBM3, KBM5, and K562 before and after incubation with rTNF-alpha. Expression of c-myc and c-myb was elevated in all cell lines prior to incubation with rTNF-alpha. In the sensitive cell lines HL-60, KBM5, and KBM3 expression of c-myc and c-myb decreased rapidly 8-, 16-, and 4-fold, respectively, by 24 hr. K562 cells, insensitive to rTNF-alpha, exhibited no change in c-myc or c-myb expression over 24 hr. These studies demonstrated that down-regulation of c-myc and c-myb expression were associated with antiproliferative effects of rTNF-alpha on these cell lines.     

Transient expression of NADPH diaphorase activity in the mouse whisker to barrel field pathway

Summary Development of the topographic map of the somatosensory cortex of rodents appears to depend on fine-tuned patterns of neuronal activity. Nitric oxide (NO) has been described as a potent messenger in the modulation of neural activity associated with synaptic plasticity. To evaluate the role of NO in the murine somatosensory pathway, we investigated NO synthase activity by NADPH diaphorase histochemistry at crucial developmental stages. At birth, NADPH diaphorase activity was detected in the cortical plate of the developing somatosensory cortex. At day 3, diffuse NADPH diaphorase activity increased within the emerging layer 4 in the future barrel field hollows. This staining was most intense at day 6 in the barrel field hollows and became undetectable by the end of the second postnatal week. The appearance of the diffuse NADPH diaphorase staining pattern was also observed in a similar time course and topography in the ascending relays of the somatosensory cortex, specifically in the barreloids within the ventrobasal nucleus of the thalamus and the barrelettes of the trigeminal nucleus of the brainstem. Lesioning the C row of whiskers at day 1 (i.e. during the critical period of barrel formation) led to fused C barrels of diffuse NADPH diaphorase activity in the barrel fields. In addition, highly NADPH diaphorase activity-positive individual cells present in the deeper layers of the somatosensory cortex at days 0 and 3 became visible in the upper layers at day 6 and remained until day 15. In layer 4, these cells were predominantly localized in the septa at day 6 and 9. No positive individual cells were detected in barrelettes or barreloids at any age. We conclude that NADPH diaphorase activity is present during experience-dependent consolidation of synaptic contacts in the somatosensory pathway.     

Mice deficient for the HNK-1 sulfotransferase show alterations in synaptic efficacy and spatial learning and memory

The HNK-1 carbohydrate structure, a sulfated glucuronyl-lactosaminyl residue carried by many neural recognition molecules, is involved in cell interactions during ontogenetic development and in synaptic plasticity in the adult. To characterize the functional role of the HNK-1 carbohydrate in vivo, we have generated mice deficient for the HNK-1 sulfotransferase (ST). The ST-/- allele is inherited with Mendelian frequencies, and the ST-/- mice are viable and fertile. The anatomy of all major brain areas appeared histologically normal. However, basal synaptic transmission in pyramidal cells in the CA1 region of the hippocampus was increased and long-term potentiation evoked by theta-burst stimulation was reduced in ST mutants. In the water maze, ST-/- mice showed an impaired long-term memory and a poorer spatial learning when a short inter-trial interval was used. These observations indicate an essential role for the sulfate group of the HNK-1 carbohydrate in synaptic plasticity of the hippocampus.     

Immunohistological localization of tenascin-c in the developing and regenerating retinotectal system of two amphibian species

The expression pattern of the extracellular matrix molecule tenascin-C was investigated in the retinotectal system of the frog Discoglossus pictus and the salamander Pleurodeles waltl during development and optic nerve regeneration in the adult. In both species, the retina was devoid of tenascin-C immunoreactivity at all ages studied. During development, tenascin-C was distributed in a gradient in the optic nerve, with the highest immunoreactivity in the eye near part of the optic nerve. The myelin-associated glycoprotein was distributed in a gradient with opposite polarity. In Discoglossus, but not Pleurodeles, tenascin-C was detected in the anterior chiasm. In the tectum of both species, tenascin-C was observed in deep cellular and fiber layers but not in the layers receiving optic fibers or proliferative zones. The distribution patterns of tenascin-C were the same during development and in the adult, except for a disappearance of the molecule from the intraocular part of the optic nerve. After lesioning the optic nerve of adult animals, tenascin-C was strongly reexpressed in the intraocular part of the optic nerve but was only weakly upregulated in the distal optic nerve stump. In contrast, a chondroitin sulfate epitope was strongly upregulated in the distal optic nerve stump. These observations suggest that during development, tenascin-C serves as an attenuating barrier for myelinating cells in the optic nerve and contributes to the guidance of growing retinal ganglion cell axons. Due to its sustained expression in the adult, tenascin-C may have similar functions during regeneration of the lesioned adult retinotectal system. © 1995 Wiley-Liss, Inc.     

The AMOG/β2 subunit of Na,K-ATPase is not necessary for long-term survival of telencephalic grafts

Adhesion molecule on glia (AMOG) represents the β2-subunit of murine Na, K-ATPase. Mice carrying a targeted deletion of the AMOG/β2 gene exhibit tremor and limb paralysis at postnatal day (P) 15 and die 2 days after the onset of symptoms. The brains of these mice show edema and swelling of astrocytic end feet However, the cause of death has remained unclear. To identify long-term consequences of AMOG/β2 deficiency, we have grafted parts of the embryonic telencephalic anlage of AMOG/β2deficient mice into the caudoputamen of wild-type mice and analyzed the grafts up to 500 days after transplantation. Histological, immunocytochemical, and in situ hybridization techniques were applied to examine histoarchitecture, proliferation, differentiation, and long-term survival of grafts. AMOG/β2-deficient telencephalic grafts develop normally and form solid neural tissue that cannot be distinguished from control grafts by morphological features or with immunocytochemical stains for neuronal and glial markers. No signs of degeneration can be found. Expression analysis, however, revealed that no AMOG/β2 protein of possible host origin can be detected in AMOG/β2-deficient grafts. Graft-borne astrocytes express neither the AMOG/β1 nor the AMOG/β2 subunit of Na, K-ATPase as examined with immunocytochemistry and in situ hybridization. These findings indicate that AMOG/β2 is not necessary for loner-term survival of telenceohalic eraft tissue. © 1995 Wiley-Liss, Inc.     

Epithelioid angiomatosis in patients with AIDS. Report of seven cases and review of the literature

Seven cases of a distinctive vascular proliferation in patients with acquired immunodeficiency syndrome are discussed and compared with other reported cases. All cases share clinical and pathologic manifestations that can be recognized early. Warthin-Starry-positive bacilli within some of the lesions and their response to erythromycin may indicate that the proliferation is associated with an infectious agent, possibly the bacillus that causes cat-scratch disease.     

Effects of NMDA Receptor Blockade in the Developing Rat Somatosensory Cortex on the Expression of the Glia-derived Extracellular Matrix Glycoprotein Tenascin-C

The patterning of synaptic connections during development is thought to be influenced by the correlation of neuronal impulse activity. N -methyl-D-aspartate (NMDA) receptors have been implicated in the reorganization of thalamocortical afferents in the visual system. The topographic mapping of the periphery of sensory systems onto the somatosensory cortex in the whisker-barrel field of rodents has served as another important paradigm in the study of extrinsic influences on synaptic rearrangements. In a search for the molecular cues that may contribute to synaptic plasticity, we have investigated the distribution of the glia-derived extracellular matrix glycoprotein tenascin-C, which is highly expressed during the formation of the barrel field map around birth and delineates the boundaries between barrel fields after segregation of afferent inputs. Here we show that systemic and local application of NMDA receptor antagonists at postnatal day 2 inhibited the down-regulation of tenascin mRNA and protein by postnatal day 6 and prevented the appearance of tenascin-positive barrel field boundaries. Furthermore, barrels were not distinguishable by Nissl staining, and segregation of thalamocortical afferents as monitored by anterograde Dil tracing and acetylcholinesterase histochemistry was not complete. These observations indicate that expression of tenascin-C and segregation of afferent inputs are modified by NMDA receptor-dependent neuronal activity.     

Ichthyosis Follicularis in Two Girls: An Autosomal Dominant Disorder

Ichthyosis follicularis (IF) is a rare disorder of keratinization that has been described primarily in males and proposed as a possible X-linked disorder. We report two black girls with nonscarring alopecia; photophobia; follicular hyperkeratoses; hyperkeratosis of the extensor aspects of the hands, knees, and elbows; fixed, erythematous, perineal plaques; and angular cheilitis who seem to fit the clinical criteria for IF. One girl also had gingival hypertrophy and a hearing deficit. One child's father had identical symptoms. We propose that these girls may have a variant of IF that is inherited as an autosomal dominant trait.