| dc.contributor.advisor | Erbaş, Tomris | tr_TR |
| dc.contributor.author | Çınar, Neşe | tr_TR |
| dc.date.accessioned | 2015-10-14T10:03:35Z | |
| dc.date.available | 2015-10-14T10:03:35Z | |
| dc.date.issued | 2013 | tr_TR |
| dc.identifier.uri | http://hdl.handle.net/11655/919 | |
| dc.description.abstract | Background and aim: A common polymorphic variant of the growth hormone
receptor (GHR) consists of genomic deletion of exon 3 (d3-GHR) or full-length
genotype (fl-GHR). d3-GHR is associated with increased responsiveness to signal
transduction of the exogenous GH. The aim of this study was to determine the
relationship between the d3-GHR polymorphism and clinical parameters and
comorbidities of the acromegalic patients.
Methods: 118 acromegalic patients (61F/57M, age: 50.3±12.2 yrs) and 108 healthy
controls (94F/ 14M, age: 41.1±11.1 yrs) were included in the study. Genotype
analysis was performed by PCR. The prevalence of d3-GHR polymorphism was
compared in patients and controls. Demographic features, GH, IGF-1 levels at
diagnosis, features of the adenoma, treatment modalities, and comorbidities of the
patients were evaluated. Impact of d3-GHR polymorphism on these parameters was
evaluated.
Results: Seventy-one patients (60.2%) were fl/fl-GHR, 40 patients (33.9%) were
heterozygotes (fl/d3-GHR) and seven patients (5.9%) were homozygotes (d3/d3-
GHR) for genomic deletion of exon 3. The prevalence of fl/fl-GHR, fl/d3-GHR and
d3/d3-GHR in controls were 57.4%, 29.6% and 13.0% respectively. No significant
difference was observed in the distribution of these polymorphisms among the
groups. Heterozygotes and homozygotes for the d3 allele were considered together
(d3-GHR) in the patients and compared with fl/fl-GHR group. d3-GHR and fl/fl-
GHR patients showed similar anthropometric measures. Baseline GH and IGF-1
levels did not differ between the groups. Both groups showed similar adenoma
features (size and the presence of cavernous sinus invasion). Moreover, treatment
modalities did not show any difference. The prevalence of comorbidities such as
coronary artery disease, hypertension, hyperlipidemia, Type 2 diabetes mellitus and
multinodular goiter were similar in both groups. There were 24 cancer patients
(20.3%) and there was no significant difference in the prevalence of cancer among
d3-GHR and fl/fl-GHR patients (n:7, 14.9 % vs n:17, 23.9%; p: 0.23).
A significant correlation between basal GH and IGF-1 levels (R²: 0.227, p<0.001)
was observed in fl/fl-GHR group whereas no significant association was found in d3-
GHR group (R²: 0.081, p: 0.08).
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Conclusion: The distribution of the genotype for d3GHR in this study was similar to
previous studies in acromegaly. Our study supports that the genotype of d3GHR
variant seems to have no impact on clinical features and comorbidities of
acromegalic patients, but may play role in the GH/IGF-1 disassociation in
acromegaly. | tr_TR |
| dc.language.iso | tur | tr_TR |
| dc.publisher | Tıp Fakültesi | tr_TR |
| dc.subject | Acromegaly | tr_TR |
| dc.title | D3-Büyüme Hormon Reseptör Polimorfizminin Akromegalı Hastalarında Klinik, Metabolik ve Kardiyovasküler Etkileri | tr_TR |
| dc.type | info:eu-repo/semantics/doctoralThesis | en |
| dc.callno | 2013/684 | tr_TR |
| dc.contributor.departmentold | İç Hastalıkları Ana Bilim Dalı | tr_TR |
| dc.description.ozet | Amaç: Büyüme hormon reseptör (GHR) geninin sik görülen polimorfik
varyantlarindan birisi ekzon 3 içeren "fl-GHR" ve içermeyen "d3-GHR"
izoformlaridir. d3-GHR tasiyanlarda egzojen GH’nun indükledigi sinyal
transdüksiyon hizi artmistir. Bu çalismada d3-GHR polimorfizminin akromegali
hastalarinin klinik bulgulari ve komorbiditeleri ile iliskisini ortaya koymak
amaçlanmistir.
Yöntem: Çalismaya akromegali tanisi alan 118 hasta (61 K/57 E, ortalama yas:
50.3±12.2 yil) ve 108 saglikli kontrol (94 K/14 E, ortalama yas: 41.1±11.1 yil) dahil
edildi. Genotip analizi periferik kan DNA’sinda PCR yöntemi ile yapildi. Hastalarin
ve kontrollerin d3-GHR polimorfizm prevalanslari karsilastirildi. Akromegalik
hastalarin demografik özellikleri, tani sirasindaki GH ve IGF-1 düzeyleri,
adenomunun özellikleri, tedavi yöntemleri ve komorbiditeleri degerlendirildi. Bu
parametreler ile d3-GHR polimorfizmi arasindaki iliski incelendi.
Bulgular: Akromegalik hastalarin %60.2’sinde (n:71) fl/fl-GHR, %33.9’unda (n:40)
d3-GHR heterozigot (fl/d3-GHR) ve %5.9’unda (n:7) d3-GHR homozigot (d3/d3-
GHR) polimorfizmi saptandi. Kontrollerin ise %57.4’ünde (n:62) fl/fl-GHR,
%29.6’sinda (n:32) fl/d3-GHR ve %13.0’ünde (n:14) d3/d3-GHR polimorfizmi
bulundu. Polimorfizm sikliklari açisindan hasta ve kontrol grubu arasinda fark
saptanmadi. Heterozigot ve homozigot d3 aleli tasiyan akromegalik hastalar birlikte
gruplandirildi (d3-GHR) ve fl/fl-GHR grubu ile karsilastirildi. Demografik özellikler
açisindan gruplar arasinda fark bulunmadi. Hastalarin tani aninda GH ve IGF-1
düzeyleri benzer bulundu. Adenom özellikleri (boyut, patolojik özellikleri ve
kavernöz sinüs invazyon varligi) her iki grupta benzerdi. Tedavi yöntemleri gruplar
arasinda farklilik göstermemekteydi. Koroner arter hastaligi, hipertansiyon,
hiperlipidemi, Tip 2 diabetes mellitus prevalansi açisindan gruplar arasinda fark
saptanmadi. Multinodüler guatr prevalansi gruplar arasinda benzer bulundu. Yirmi
dört hastada kanser tespit edildi (%20.3) ve kanser riski üzerinde d3-GHR
polimorfizminin bir etkisi gözlenmedi (d3-GHR, n:7; %14.9 vs. fl/fl-GHR, n:17;
%23.9, p: 0.23). fl/fl-GHR grubunda tedavi öncesi GH ve IGF-1 düzeyleri arasinda
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anlamli iliski saptanirken (R²: 0.227, p<0.001), bu iliski d3-GHR grubunda (R²:
0.081, p:0.08) bulunmadi.
Sonuç: Akromegalik hastalarda d3-GHR polimorfizm sikligi daha önce yapilan
çalismalarla benzer bulunmustur. Bizim çalışmamız, d3-GHR genotipinin,
akromegali hastalarının klinik bulguları ve komorbiditeleri üzerinde belirgin etkisi
olmadigini destekler niteliktedir ancak bu polimorfizmin, GH ile IGF-1
disasosiasyonunda rol oynayabilecegi düsünülebilir. | tr_TR |
| dc.subtype | medicineThesis | |
