Evaluation of hepatic and remote organ injury in an experimental liver ischemia-reperfusion model in rats and the effects of quercetin on this damage

Ar�, Neziha Senem; Yulu�, Esin; Ar�, B�nyamin; KAYA, Cansu; Reis K�se, G�k�en Derya; Zengin, Tu�ba; Keskin, O�uzhan; Ar�c�, Tu�ba; Yenilmez, Engin

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Evaluation of hepatic and remote organ injury in an experimental liver ischemia-reperfusion model in rats and the effects of quercetin on this damage [Ulus Travma Acil Cerrahi Derg]

Ulus Travma Acil Cerrahi Derg. 2025; 31(9): 823-830 | DOI: 10.14744/tjtes.2025.61423

Evaluation of hepatic and remote organ injury in an experimental liver ischemia-reperfusion model in rats and the effects of quercetin on this damage

Neziha Senem Ar�¹, Esin Yulu�², B�nyamin Ar�³, Cansu KAYA⁴, G�k�en Derya Reis K�se⁵, Tu�ba Zengin⁶, O�uzhan Keskin⁷, Tu�ba Ar�c�⁸, Engin Yenilmez²
¹Department of Histology and Embryology, Kutahya Health Sciences University Faculty of Medicine, Kutahya-Türkiye
²Department of Histology and Embryology, Karadeniz Technical University Faculty of Medicine, Trabzoc-Türkiye
³Department of Orthopedics and Traumatology, Kütahya Health Sciences University Faculty of Medicine, Kutahya-Türkiye
⁴Department of Medical Biology, Karadeniz Technical University Faculty of Medicine, Trabzon-Türkiye
⁵Ivf Center, Zeynep Kamil Women and Children Diseases Traning and Research Hospital, �stanbul-Türkiye
⁶Ivf Center, Trabzon Kanuni Training and Research Hospital, Trabzon-Türkiye
⁷Department of Pulmonary Disease, �anakkale University Faculty of Medicine, �anakkale-Türkiye
⁸IVF Center, �stanbul �am and Sakura City Hospital, �stanbul-Türkiye

BACKGROUND: This study aims to show the changes in the liver, lung, kidney, and heart in the liver ischemia-reperfusion model in rats and the effect of quercetin on these changes histopathologically and immunohistochemically.
METHODS: Eighteen Sprague Dawley rats were classified into three groups: Group 1 sham, Group 2 ischemia-reperfusion (IR), Group 3 ischemia-reperfusion + quercetin (IR+Q). For three days, distilled water was given to Group 1, and quercetin was given to Group 3 via gavage. At the end of the third day, abdominal opening-closing was applied to Group 1, and 4 hours of reperfusion was applied to Groups 2 and 3 after 1 hour of ischemia by clamping the hepatoduodenal ligament, and all rats were euthanized. Liver, lung, kidney, and heart tissue samples were stained with Hematoxylin Eosin (HE), Masson Trichrome, Periodic Acid-Schiff (PAS), and TUNEL (Terminal deoxynucleotidyl transferase (TdT) deoxyuridine triphosphate nick end labeling assay) to assess apoptosis and examined histopathologically and immunohistochemically under a light microscope.
RESULTS: In the liver, the damage score was significantly higher in the IR group than in the sham group, while it was significantly lower in the IR+Q group than in the IR group. While there was no significant difference between the groups in semi-quantitative scoring parameters, the Apoptotic Index was significantly higher in the IR group than in the sham group and significantly lower in the IR+Q group than in the IR group. In the lung, no significant difference in lung damage scores between the groups was observed. While the Apoptotic Index was significantly higher in the IR group than in the sham group, it was significantly lower in the IR+Q group than in the IR group. In the kidneys, tubular cell degeneration and intertubular vascular congestion were significantly higher in the IR group than in the sham group. While the Apoptotic Index was higher in the IR group than in the sham and IR+Q groups, it was higher in the IR+Q group than in the sham group. In the heart, there was no difference between the groups in terms of myocardial cell degeneration and vascular damage. The apoptotic index was significantly higher in the IR group than in the sham and IR+Q groups.
CONCLUSION: Our results indicate that histopathological damage occurs in the liver, lung, kidney, and heart in the experimentally created IR model, and quercetin application decreases IR-related damage and apoptosis in these organs.

Keywords: Ischemia-reperfusion injury, liver, quercetin, remote organ.

S��anlarda deneysel karaci�er iskemi-reperf�zyon modelinde karaci�er ve uzak organ hasar�n�n de�erlendirilmesi ve bu hasara quercetin'in etkileri

Neziha Senem Ar�¹, Esin Yulu�², B�nyamin Ar�³, Cansu KAYA⁴, G�k�en Derya Reis K�se⁵, Tu�ba Zengin⁶, O�uzhan Keskin⁷, Tu�ba Ar�c�⁸, Engin Yenilmez²
¹K�tahya Sa�l�k Bilimleri �niversitesi T�p Fak�ltesi, Histoloji Ve Embriyoloji Ana Bilim Dal�, K�tahya
²Karadeniz Teknik �niversitesi T�p Fak�ltesi, Histoloji Ve Embriyoloji Ana Bilim Dal�, Trabzon, Türkiye
³K�tahya Sa�l�k Bilimleri �niversitesi T�p Fak�ltesi, Ortopedi Ve Travmotoloji Ana Bilim Dal�, K�tahya, Türkiye
⁴Karadeniz Teknik �niversitesi T�p Fak�ltesi, T�bbi Biyoloji Ana Bilim Dal�, Trabzon, Türkiye
⁵Zeynep Kamil Kad�n Do�um Ve �ocuk Hastal�klar� Hastanesi, Ivf Merkezi, �stanbul, Türkiye
⁶Trabzon Kanuni E�itim Ve Ara�t�rma Hastanesi, Ivf Merkezi, Trabzon, Türkiye
⁷�anakkale �niversitesi T�p Fak�ltesi, G��s Hastal�klar� Ana Bilim Dal�, �anakkale, Türkiye
⁸Ivf Merkezi, �stanbul �am and Sakura �ehir Hastanesi, �stanbul, Türkiye

AMA�: Bu �al��ma, s��anlarda karaci�er iskemi-reperf�zyon modelinde karaci�er, akci�er, b�brek ve kalpte meydana gelen de�i�iklikleri ve quercetin'in bu de�i�iklikler �zerindeki etkisini histopatolojik ve imm�nohistokimyasal olarak g�stermeyi ama�lamaktad�r.
GERE� VE Y�NTEM: On sekiz Sprague Dawley s��an 3 gruba ayr�ld�: Grup 1 sham, Grup 2 iskemi-reperf�zyon, Grup 3 iskemi-reperf�zyon + quercetin. 3 g�n boyunca Grup 1'e distile su, Grup 3'e ise quercetin gavaj yoluyla verildi. 3. g�n�n sonunda Grup 1'e abdominal a�ma-kapama, Grup 2 ve 3'e ise hepatoduodenal ligament klemplenerek 1 saatlik iskeminin ard�ndan 4 saatlik reperf�zyon uyguland� ve t�m s��anlar sakrifiye edildi. Karaci�er, akci�er, b�brek ve kalp doku �rnekleri hematoksilen eozin (HE), Masson Trikrom, Periyodik Asit-Schiff (PAS) ve apoptozu de�erlendirmek i�in TUNEL (Terminal deoksin�kleotidil transferaz (TdT) deoksi�ridin trifosfat nick end labeling assay) ile boyand� ve ��k mikroskobu alt�nda histopatolojik ve imm�nohistokimyasal olarak incelendi.
BULGULAR: Karaci�erde hasar skoru; IR grubunda sham grubuna g�re anlaml� derecede y�ksek iken, IR+Q grubunda IR grubuna g�re anlaml� derecede d��kt�. Yar� kantitatif skorlama parametrelerinde gruplar aras�nda anlaml� bir fark bulunmazken, apoptotik indeks �R grubunda sham grubuna g�re anlaml� derecede y�ksek, �R+Q grubunda ise �R grubuna g�re anlaml� derecede d��kt�. Akci�erde, akci�er hasar� skorlar�nda gruplar aras�nda anlaml� bir fark g�zlenmedi. Apoptotik indeks IR grubunda sham grubuna g�re anlaml� derecede y�ksekken, IR+Q grubunda IR grubuna g�re anlaml� derecede d��kt�. B�breklerde, t�b�ler h�cre dejenerasyonu ve intert�b�ler vask�ler konjesyon IR grubunda sham grubuna g�re anlaml� derecede y�ksekti. Apoptotik indeks IR grubunda sham ve IR+Q gruplar�na g�re daha y�ksek iken, IR+Q grubunda sham grubuna g�re daha y�ksekti. Kalpte, miyokardiyal h�cre dejenerasyonu ve vask�ler hasar a��s�ndan gruplar aras�nda fark yoktu. Apoptotik indeks IR grubunda sham ve IR+Q gruplar�na g�re anlaml� olarak daha y�ksekti.
SONU�: Sonu�lar�m�z, deneysel olarak olu�turulan IR modelinde karaci�er, akci�er, b�brek ve kalpte histopatolojik hasar olu�tu�unu ve quercetin uygulamas�n�n bu organlarda IR ile ili�kili hasar� ve apoptozisi azaltt��n� g�stermektedir.

Anahtar Kelimeler: �skemi-reperf�zyon hasar�, karaci�er, quercetin, uzak organ hasar�.

Corresponding Author: Neziha Senem Ar�, T�rkiye
Manuscript Language: English

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