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Featured researches published by Iris Vered.


Pediatric Nephrology | 2015

Maternal and infantile hypercalcemia caused by vitamin-D-hydroxylase mutations and vitamin D intake.

Dganit Dinour; Miriam Davidovits; Shraga Aviner; Liat Ganon; Leonid Michael; Dalit Modan-Moses; Iris Vered; Haim Bibi; Yaacov Frishberg; Eli J. Holtzman

BackgroundHypercalcemia is caused by many different conditions and may lead to severe complications. Loss-of-function mutations of CYP24A1, encoding vitamin D-24-hydroxylase, have recently been identified in idiopathic infantile hypercalcemia and in adult kidney stone disease. The aim of this study was to investigate the genetics and clinical features of both infantile and maternal hypercalcemia.MethodsWe studied members of four unrelated Israeli families with hypercalcemia, namely, one woman during pregnancy and after delivery and three infants. Clinical and biochemical data were obtained from probands’ medical charts. Genomic DNA was isolated from peripheral blood and CYP24A1 was sequenced.ResultsTypical symptoms of hypercalcemia associated with the intake of recommended doses of vitamin D developed in the infants and pregnant woman. Four different loss-of-function CYP24A1 mutations were identified, two of which are reported here for the first time (p.Trp134Gly and p.Glu315*). The infants from families 1 and 2, respectively, were found to be compound heterozygotes, and the infant from family 3 and the pregnant woman were found to be homozygous.ConclusionsThis is the first report of maternal hypercalcemia caused by a CYP24A1 mutation, showing that not only infants are at risk for this complication. Our findings emphasize the importance of recognition, genetic diagnosis and proper treatment of this recently identified hypercalcemic disorder in this era of widespread vitamin D supplements.


Aging Clinical and Experimental Research | 2005

Treatment preference and tolerability with alendronate once weekly over a 3-month period: an Israeli multi-center study

Mordechai Weiss; Iris Vered; A. Joseph Foldes; Yael C. Cohen; Yael Shamir-Elron; Sophia Ish-Shalom

Background and aims: Osteoporosis is a chronic condition requiring long-term treatment, for which compliance is not easy to achieve. 70 mg of alendronate once weekly (alendronate OW) provides equivalent efficacy to treatment with 10 mg of alendronate once a day (alendronate OD); however, there are relatively few data regarding patient and physician preferences for once-weekly vs daily dosing. The aim of this study was to measure compliance, convenience, tolerance and relative preference of alendronate OW treatment among post-menopausal women with osteoporosis and physician satisfaction, compared with previous treatment with alendronate OD. Methods: This open-label, prospective multi-center trial was conducted at 14 hospitals and 150 primary-care community clinics in Israel. Post-menopausal osteoporotic women (n=3710), who had been treated for at least 1 month with alendronate OD during the preceding year, were treated with alendronate OW for 12 weeks. Convenience, satisfaction, tolerance and relative preference of alendronate OW during the trial, compared with past experience with alendronate OD, were recorded. Results: Overall, 96% of the patients preferred the alendronate OW regimen to the 10-mg daily dosage. Nearly all (98%) the patients who completed 12 weeks of treatment, including 77% of patients who had previously discontinued daily treatment due to intolerance, were willing to continue the alendronate OW regimen. Patient-reported compliance with dosing instructions was over 98%. Alendronate OW was well tolerated; only 2.8% of patients discontinued, due to adverse events. Physicians were highly satisfied with the once-weekly dosing regimen, and recommended continued treatment with alendronate OW for 99% of the patients. Conclusions: The majority of post-menopausal women with osteoporosis, including those who were previously intolerant to alendronate OD, preferred alendronate OW to the once-daily dosing regimen. It is important to consider patient preference when selecting the appropriate treatment for osteoporosis.


The Journal of Clinical Endocrinology and Metabolism | 2002

Pseudohypoaldosteronism Type II: Marked Sensitivity to Thiazides, Hypercalciuria, Normomagnesemia, and Low Bone Mineral Density

Haim Mayan; Iris Vered; Meir Mouallem; Michal Tzadok-Witkon; Rachel Pauzner; Zvi Farfel


Thyroid | 2006

Time trends of incidence rates of thyroid cancer in Israel: What might explain the sharp increase

Alexandra Lubina; Ohad Cohen; Micha Barchana; Irena Liphshiz; Iris Vered; Siegal Sadetzki; Avraham Karasik


Osteoporosis International | 2005

Alendronate for osteoporosis in men with androgen-repleted hypogonadism

Ilan Shimon; Varda Eshed; Ram Doolman; Ben-Ami Sela; Avraham Karasik; Iris Vered


Israel Medical Association Journal | 2002

Vitamin D and calcium-sensing receptor genotypes in men and premenopausal women with low bone mineral density.

Michael Eckstein; Iris Vered; Sophia Ish-Shalom; Anat Ben Shlomo; Avraham Shtriker; Nira Koren-Morag; Eitan Friedman


The Journal of Clinical Endocrinology and Metabolism | 1997

Cross Genotype Sex Hormone Treatment in Two Cases of Hypogonadal Osteoporosis

Iris Vered; Igor Kaiserman; Ben-Ami Sela; Joseph Sack


Nutrition | 2016

Hyponatremia and decreased bone density in adolescent inpatients diagnosed with anorexia nervosa

Yael Levy-Shraga; Dana David; Iris Vered; Brigitte Kochavi; Dan J. Stein; Dalit Modan-Moses


International Journal of Eating Disorders | 2007

Plasma homocysteine levels in female patients with eating disorders.

Joseph Levine; Eitan Gur; Ron Loewenthal; Tali Vishne; Tzvi Dwolatzky; Ingrid M. van Beynum; Ben-Ami Sela; Iris Vered; Galit Yosef; Dan J. Stein


Archive | 2000

The Genetic Basis for Stress Fractures

Eitan Friedman; Iris Vered; Jushua Shemer

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Dan J. Stein

University of Cape Town

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Sophia Ish-Shalom

Technion – Israel Institute of Technology

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