P Tassoni scite author profile

We used a real time mechanical sector scanner to evaluate uterine and ovarian size in a large number of normal premenarcheal girls strictly grouped according to age. In addition, we studied the relation between these parameters and puberty and sex hormone concentrations. Patients and methodsA total of 114 premenarcheal girls, whose ages ranged from 2 years to 13 years 11 months, were studied after informed parental consent had been obtained. They were all suffering from minor, nonendocrinologic, acute pathology. Each

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Variability of Growth Hormone Response to Pharmacological and Sleep Tests Performed Twice in Short Children

Tassoni

Cacciari

Cau

et al. 1990

The Journal of Clinical Endocrinology & Metabolism

116

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Forty-nine children with short stature (age range, 4.1-15.9 yr) were examined. Twenty-four (group 1) were submitted twice to an arginine and a sleep test (12-h overnight GH profile). Twenty-five patients (group 2) were submitted twice to an arginine and L-dopa test. Coefficients of variation were calculated between both the results of pharmacological (peak and area under the curve) and sleep tests [mean GH concentration (MGHC), peak, area under the curve, number of peaks above 5 micrograms/L, and peak area]. In group 1 the coefficient of variation of sleep test parameters was significantly lower than that of pharmacological tests (P less than 0.01 to less than 0.001). In the sleep test the area under the curve and MGHC were the most constant parameters. Group 2 showed no difference between the coefficients of variation of the two pharmacological tests. Considering groups 1 and 2 together, the coefficients of variation of the sleep test, in particular the MGHC and area under the curve, were lower than those of the two pharmacological tests. Eight of 24 subjects in group 1 showed a low GH level in 1 series of tests, and a normal level in the other series. Five of 18 subjects in group 2 showed an abnormally low GH response to the arginine and L-dopa tests and a normal response to the 2 repeated tests. Therefore, to prevent an erroneous interpretation of the GH test results, it is very important to perform a sleep test and repeat it whenever GH secretion seems to be deficient or at the lower limits of normalcy.

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Growth and growth factors in diabetes mellitus.

Salardi¹,

Tonioli²,

Tassoni³

et al. 1987

Archives of Disease in Childhood

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SUMMARY Growth of 79 children with diabetes was analysed at diagnosis and again after one to 10-7 years of treatment with insulin. Both sexes were tall at onset, whereas at the last observation boys alone showed significant growth retardation. Height standard deviation score (SDS), however, showed no significant fall either in 32 subjects reassessed after five years of disease or in 18 subjects examined at full stature. Skeletal maturity was not significantly impaired after treatment. Pubertal growth spurt was reduced, especially in girls and in subjects with onset of disease at or around puberty. We found no significant correlation between height and height velocity SDS and glycosylated haemoglobin values or secretion of growth hormone during the arginine test. Somatomedin C values were correlated with height velocity SDS in prepubertal boys. The results of this study suggest that there are interferences in the growth of children with diabetes but that they do not seem to have a significant influence on adult height.It is well recognised that growth is seriously impaired in cases of very poorly controlled diabetes.'

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Short stature and celiac disease: A relationship to consider even in patients with no gastrointestinal tract symptoms

Cacciari

Salardi

Lazzari

et al. 1983

The Journal of Pediatrics

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Pitfalls in diagnosing impaired growth hormone (GH) secretion: retesting after replacement therapy of 63 patients defined as GH deficient.

Cacciari

Tassoni

Parisi

et al. 1992

The Journal of Clinical Endocrinology & Metabolism

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Possible causes of error in the diagnosis of isolated GH deficiency are the variability of GH response to repeated tests, the existence of transient GH deficiencies, and the low GH levels found in short statured children with delayed puberty. Sixty-three patients with variously expressed GH deficiency were retested (1 sleep test and 2 pharmacological tests) after 1-3.9 yr of GH therapy (dose, 15 U/m2.week). Forty-eight subjects had arginine, L-dopa, and sleep tests (mean serum GH concentration) twice, while 15 had only arginine and L-dopa tests. All patients were retested 1 month after withdrawal from therapy. The criteria used to subdivide the patients were pubertal development and response to pharmacological and sleep tests at first diagnosis and on retesting. The initial diagnosis in 33 subjects (52.4%) was not confirmed, and 13 (20.6%) were no longer deficient on retesting. The percentage of normalization was high for the sleep test (43.9%), lower for the pharmacological test (24.5%), and lower still (12.9%) for pharmacological and sleep tests considered together. While none of the 28 subjects who remained prepubertal at retesting normalized in any of the tests, 13 of the 35 subjects retested during puberty did. When normalization was observed in pubertal subjects, it occurred predominantly in the sleep test. Growth velocity and height age/bone age increment ratio after the first year of therapy were no different for the groups of subjects classified according to GH secretion on retesting. Our study demonstrates that a number of children diagnosed as GH deficient do not have a true deficiency. However, such a diagnostic error seems to have little effect, at least in the first year of therapy, on the effectiveness of GH treatment.

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P Tassoni

Pelvic ultrasonography in premenarcheal girls: relation to puberty and sex hormone concentrations.

Variability of Growth Hormone Response to Pharmacological and Sleep Tests Performed Twice in Short Children

Growth and growth factors in diabetes mellitus.

Short stature and celiac disease: A relationship to consider even in patients with no gastrointestinal tract symptoms

Pitfalls in diagnosing impaired growth hormone (GH) secretion: retesting after replacement therapy of 63 patients defined as GH deficient.

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