Decreased peak bone mass is associated with a 3-bp deletion/insertion of the CYP19 intron 4 polymorphism: Preliminary data from the GOOS study

Kaštelan, Darko; Grubić, Zorana; Kraljević, Ivana; Đurić, Koraljka; Kardum, Iva; Dušek, Tina; Štingl, Katarína; Giljević, Zlatko; Kerhin-Brkljačić, Vesna; Suchanek, Ernest; Koršić, Mirko

doi:10.1007/bf03346329

Cited by 10 publications

(4 citation statements)

References 22 publications

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“…Many authors have observed that CYP19A1 gene mutations are associated with BMD and their presence may contribute to the development of osteoporosis [ 10 , 15 ]. Riancho et al and Kaminski et al showed that total hip BMD is higher in patients with the GG genotype compared to the GA and AA genotypes [ 15 , 16 ].…”

Section: Discussionmentioning

confidence: 99%

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Association of the CYP19A1 rs700518 Polymorphism with Selected Markers of Bone Metabolism in Women with Hyperandrogenism

Uzar

Bogacz

Sowińska-Przepiera

et al. 2022

JCM

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Hyperandrogenism is the most common endocrine disorder in women, characterized by an imbalance of normal estrogen and androgen levels in the blood. Androgens play an important role in the female body because they influence bone mineral density (BMD), body mass composition, muscle mass, mental state, and the regulation of sexual function. The reduced activity of aromatase, due to mutations in the CYP19A1 gene, reduces the estrogen pool in favor of androgens. Clinically, aromatase deficiency causes hyperandrogenism in women. Therefore, the aim of the study was to assess the effect of the CYP19A1 gene polymorphism on selected markers of bone metabolism and hormonal parameters in women with hyperandrogenism. The study group was comprised of 80 young women with hyperandrogenism who underwent measurements of bone mineral density (BMD), and determination of hormonal and metabolic parameters. Enzyme immunoassays were used to measure leptin, total sRANKL (free and bound RANKL), osteoprotegerin, and total 25-OH Vitamin D. An analysis of the CYP19A1 gene polymorphisms was performed using the real-time PCR method. The GG genotype of the CYP19A1 rs700518 polymorphism turned out to be associated with: FEI (Free Estradiol Index), SHGB concentration, estradiol concentration, and insulin concentration determined in the glucose tolerance test 60’ compared to AG and AA genotypes. Patients with the AG genotype had a higher ratio of android to gynoid fat and a greater content of visceral adipose tissue. Higher visceral tissue content may reduce BMD. In conclusion, the study showed that the CYP19A1 rs700518 polymorphism may be associated with the distribution of adipose tissue in young women with hyperandrogenism. These results suggest that patients with the AG genotype may develop osteoporosis.

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Section: Discussionmentioning

confidence: 99%

“…Girls do not develop secondary sexual characteristics properly during puberty [ 9 ]. The CYP19A1 polymorphism is related to bone mineral density (BMD), and rs700518 is one of the most studied polymorphisms in association with BMD and osteoporosis [ 10 , 11 ].…”

Section: Introductionmentioning

confidence: 99%

Association of the CYP19A1 rs700518 Polymorphism with Selected Markers of Bone Metabolism in Women with Hyperandrogenism

Uzar

Bogacz

Sowińska-Przepiera

et al. 2022

JCM

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“…Brojni ~imbenici utje~u na vr{nu ko{tanu masu, no ~ini se da najve}i utjecaj imaju neki genetski polimorfizmi. Kao geni kandidati naj~e{}e se spominju gen za receptor vitamina D (24), gen alfa 1 za kolagen tipa 1 (25), gen za aromatazu (26), gen za ~imbenik rasta sli~an inzulinu (27), gen za alfa receptor estrogena (28) i gen za receptor androgena (29). Osim naslije|a, va`nu ulogu u postizanju vr{ne ko{tane mase imaju i tjelesna aktivnost, koli~ina kalcija u prehrani, te dob ulaska u pubertet (30).…”

Section: Fiziologija Kostiunclassified

“…Istra`ivanje utjecaja pojedinih mikrosatelitskih lokusa na vr{nu ko{tanu masu u mu{karaca pokazalo je da je alel (TTTA) 7-3pb unutar gena za aromatazu povezan s ni`om vr{nom ko{tanom masom u vratu bedrene kosti (26). Sli~no tome, ni`a vr{na ko{tana masa u vratu bedrene kosti utvr|ena je u homozigota (CA) 18 /(CA) 18 (gen za IGF-1), a u lumbalnoj kralje`nici i proksimalnom dijelu bedrene kosti u nosioca alela (TA) 21 unutar gena za α-receptor estrogena (neobjavljeni podatci).…”

Section: Fiziologija Kostiunclassified

Osteoporosis in Men

Kaštelan¹

2007

Archives of Industrial Hygiene and Toxicology

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Zavod za endokrinologiju Klinike za unutra{nje bolesti, Klini~ki bolni~ki centar Zagreb, Zagreb, HrvatskaProdu`enjem o~ekivanog trajanja `ivota osteoporoza je postala rastu}i problem u ve}ini razvijenih zemalja svijeta. U radu se raspravlja o u~estalosti, patogenezi, dijagnosti~kim kriterijima i mogu}nostima lije~enja osteoporoze u mu{karaca. Svaki tre}i prijelom kuka doga|a se u mu{karaca, a vi{e od 11 % mu{karaca starijih od 50 godina do`ivi ovaj prijelom. Dijagnoza idiopatske osteoporoze primjenjuje se za mu{karce mla|e od 60 godina u kojih nema drugih mogu}ih uzroka bolesti. U njih je niska mineralna gusto}a kosti (BMD) najve}im dijelom posljedica niske vr{ne ko{tane mase. U oko 30 % mu{karaca nalazi se sekundarna osteoporoza, a involucijska osteoporoza nastaje u mu{karaca starijih od 60 godina, kao rezultat smanjenja koncentracije testosterona i IGF-1. S obzirom na rezultate istra`ivanja koja su pokazala da vrijednost BMD-a u oba spola pru`a sli~ne informacije o riziku prijeloma, ~ini se da se postoje}i kriteriji za dijagnozu osteoporoze u `ena mogu iskoristiti i za mu{karce. U lije~enju, bisfosfonati i teriparatid dokazano i zna~ajno pove}avaju BMD u mu{karaca. Primjena androgena pokazala se u~inkovitom u mu{karaca s hipogonadizmom, no opravdanost njihove primjene u eugonada jo{ uvijek je predmet rasprava. Pove}anjem znanja o metabolizmu kosti i ko{tanoj pregradnji u novije vrijeme otvorila su se vrata ~itavom nizu molekula koje bi u budu}nosti mogle postati temelj lije~enja osteoporoze u mu{karaca. Arh Hig Rada Toksikol 2007;58:25-32 Produ`enjem o~ekivanog trajanja `ivota osteoporoza postaje rastu}i problem u ve}ini razvijenih zemalja svijeta. S javnozdravstvenog gledi{ta `ene su zanimljivije nego mu{karci budu}i da `ive du`e i da u svakoj dobi imaju ni`u mineralnu gusto}u kosti (BMD, od engl. bone mineral density) u usporedbi s mu{karcima, {to uz ubrzani gubitak ko{tane mase u prvim godinama nakon menopauze, pridonosi znatno ve}em riziku prijeloma kosti. Ipak, svaki tre}i prijelom kuka doga|a se u mu{karaca (1), a vi{e od 11 % mu{karaca starijih od 50 godina do`ivi ovaj prijelom (2). Uz to smrtnost nakon prijeloma kuka u mu{karaca je dvostruko ~e{}a nego u `ena (3). Sli~no tome, i u mu{karaca s drugim osteoporoti~nim prijelomima, osim u onih s prijelomima kralje`aka, ve}a je stopa smrtnosti. KLJU^NE RIJE^I: epidemiologija osteoporoze, genetika, kvantitativni ultrazvuk petne kosti, lije~enje osteoporoze Ka{telan D. OSTEOPOROSIS IN MEN U^ESTALOST OSTEOPOROZEU~estalost osteoporoze u mu{karaca starijih od 50 godina tri puta je manja nego u `ena iste dobi, {to je otprilike sukladno spolnim razlikama za rizik osteoporoti~nog prijeloma (4). No, pri procjeni u~estalosti osteoporoze potrebno je na umu imati ~injenicu da u~estalost ovisi o referentnim vrijednostima na osnovi kojih je izra~unata vrijednost T koja pokazuje odstupanje BMD pojedinca od prosje~ne vrijednosti BMD u mladoj zdravoj populaciji, na temelju ~ega se odre|uje dijagnoza osteoporoze (T≤ -2,5). Uzmemo li kao referentnu populaciju za izra~un vr...

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