Your search keyword '"Kalnins, Renate"' showing total 59 results

51. Limbic P3 potentials, seizure localization, and surgical pathology in temporal lobe epilepsy.

Author

Puce, Aina, Kalnins, Renate M., Berkovic, Samuel F., and Bladin, Peter F.

Published

1989

52. Gerstmann-Sträussler-Scheinker disease with coincidental familial onset.

Author

Hudson, Arthur J., Farrell, Michael A., Kalnins, Renate, and Kaufmann, John C. E.

Published

1983

53. Distribution of catecholamine uptake sites in human brain as determined by quantitative [3H] mazindol autoradiography.

Author

Donnan, Geoffrey A., Kaczmarczyk, Stan J., Paxinos, George, Chilco, Peter J., Kalnins, Renate M., Woodhouse, Dianne G., and Mendelsohn, Frederick A. O.

Published

1991

54. Lymphoma of the trigeminal nerve - the need for histological diagnosis.

Author

Perera, Chandrashan, Fitt, Gregory, Kalnins, Renate, Lee, Stewart, and Gonzalvo, Augusto

Subjects

TUMOR growth, BRAIN tumor treatment, LYMPHOMAS, HOSPITAL radiological services, CRANIAL nerves, B cells, MANAGEMENT, TUMOR treatment

Abstract

CNS lymphoma involving the trigeminal nerve is a rare condition which presents as a cavernous sinus lesion. It may mimic the radiological appearance of other lesions, and biopsy is essential before considering empirical radiotherapy for lesions in this region. We report the radiological, histopathological and operative findings of a primary non Hodgkin B cell lymphoma involving the trigeminal nerve. [ABSTRACT FROM AUTHOR]

Published

2014

55. Ontogeny of pemphigus and bullous pemphigoid antigens in human skin.

Author

Muller, H. K., Kalnins, Renate, and Sutherland, R. C.

Subjects

PEMPHIGUS, ANTIGENS, IMMUNOFLUORESCENCE, SKIN diseases, DERMATOLOGY, MEDICAL research

Abstract

The development of pemphigus and bullous pemphigoid antigens in twenty-nine human foetuses aged 9–40 weeks has been examined by immunofluorescence. Pemphigus antigen was weakly demonstrable in the epidermal intercellular area at 9 weeks and strongly after 12 weeks. Bullous pemphigoid antigen was weak and patchy at 12 weeks and only consistently demonstrable with bright linear immunofluorescence of the basement membrane zone after 23 weeks. Morphologically detectable epidermal basement membrane is already present by 9 weeks gestation. [ABSTRACT FROM AUTHOR]

Published

1973

56. Life-Threatening Focal Status Epilepticus due to Occult Cortical Dysplasia

Author

Desbiens, Richard, Berkovic, Samuel F., Dubeau, François, Andermann, Frederick, Laxer, Kenneth D., Harvey, Simon, Leproux, François, Melanson, Denis, Robitaille, Yvon, Kalnins, Renate, Olivier, André, Fabinyi, Gavin, and Barbaro, Nicholas M.

Abstract

• OBJECTIVE. —Neuronal migration disorders are usually, but not necessarily, demonstrated by magnetic resonance imaging. Preoperative suspicion of these anomalies in the presence of normal magnetic resonance studies has important practical implications. This study delineates some clinical features that permit early suspicion of focal cortical dysplasia localized in the central and precentral regions. DESIGN. —In a retrospective case series, we studied the clinical presentation of four consecutive patients with normal preoperative magnetic resonance images in whom focal cortical dysplasia was found in the surgical specimen. SETTING. —Patients were seen in three referral centers specializing in epilepsy surgery. PATIENTS. —Four patients (three female), between the ages of 4 and 21 years, had intractable partial seizures leading to resective brain surgery. INTERVENTION. —Three patients had corticectomies in the central (two patients) or frontal (one patient) regions. One underwent an en bloc resection of the central area after two unsuccessful corticectomies and cortical transcetion. RESULTS. —Three patients presented with life-threatening focal motor status epilepticus necessitating intubation, and one had epilepsia partialis continua. All had had seizures previously, and the attacks progressed to intractability after 1½ to 3 years. Surgery led to control of the seizures, but only two patients became seizure free (mean follow-up, 15.7 months). All but one developed a postoperative deficit, which eventually improved. CONCLUSIONS. —Focal cortical dysplasia should be suspected when life-threatening focal motor status epilepticus or epilepsia partialis continua occur in children or young persons without another obvious cause. Normal magnetic resonance studies do not exclude neuronal migration disorders.

Published

1993

57. Regional and temporal effects of 1-methyl-4-phenyl-1,2,3,6-tetrahydropyridine on dopamine uptake sites in mouse brain

Author

Donnan, Geoffrey A., primary, Kaczmarczyk, Stan J., additional, McKenzie, John S., additional, Rowe, Peter J., additional, Kalnins, Renate M., additional, and Mendelsohn, Frederick A.O., additional

Published

1987

58. Cognitive consequences of coexisting temporal lobe developmental malformations and hippocampal sclerosis

Author

Mitchell, L. Anne, Briellmann, Regula S., Kalnins, Renate M., and Jackson, Graeme D.

Published

2000

59. Increased anterior temporal lobe T2 times in cases of hippocampal sclerosis: a multi-echo T2 relaxometry study at 3 T.

Author

Briellmann RS, Syngeniotis A, Fleming S, Kalnins RM, Abbott DF, and Jackson GD

Subjects

Adult, Cerebral Cortex abnormalities, Cerebral Cortex pathology, Dominance, Cerebral physiology, Feasibility Studies, Female, Humans, Male, Sclerosis diagnosis, Software Design, Temporal Lobe pathology, Epilepsy, Temporal Lobe diagnosis, Hippocampus pathology, Image Processing, Computer-Assisted methods, Magnetic Resonance Imaging methods

Abstract

Background and Purpose: Increased T2 relaxation times in the ipsilateral hippocampus are present in patients with hippocampal sclerosis. Visual assessment of T2-weighted images of these patients suggests increased signal intensity in the anterior temporal lobe as well. Our aim was to assess hippocampal and anterior temporal T2 relaxation times in patients with partial epilepsy by using a new T2-relaxometry sequence implemented by using a 3-T General Electric imaging unit., Methods: Coronal view T2 maps were generated by using an eight-echo Carr-Purcell-Meiboom-Gill sequence (TE, 28-231) with an acquisition time of 7 min on a 3-T General Electric Signa Horizon LX imaging unit. T2 relaxation times were measured in the hippocampus and anterior temporal lobe of 30 healthy control volunteers and 20 patients with partial epilepsy., Results: For the 30 control volunteers, the mean hippocampal T2 relaxation time was 98 +/- 2.8 ms. In all measured areas, the asymmetry index was small (<0.01). For the 15 patients with independent evidence of hippocampal sclerosis established by visual, volumetric, and, when available, pathologic criteria, mean hippocampal T2 relaxation times were 118 +/- 7 ms (P <.0001) on the ipsilateral side and 101 +/- 4 ms (P =.005) on the contralateral side. The T2 values were also increased in the anterior temporal lobe (ipsilateral: 82 +/- 6 ms, P <.0001; contralateral: 79 +/- 6 ms, P =.01) as compared with the values for the control volunteers (75 +/- 3 ms). The five patients with focal cortical dysplasia had hippocampal T2 relaxation times that were not different from control values., Conclusion: T2 relaxometry at 3 T is feasible and useful and confirmed marked ipsilateral hippocampal signal intensity increase in patients with hippocampal sclerosis. Importantly, definite signal intensity change was also present in the anterior temporal lobe. T2 relaxometry is a sensitive means of identifying abnormalities in the hippocampus and other brain structures.

Published

2004