The role of protein oxidation in the development of diabetic microvascular complications

Mertoglu, Cuma; Siranli, Gulsah; Coban, T. Abdulkadir; Karakurt, Yucel; Ersoy, Alevtina; Ozcicek, Adalet; Arslan, Yusuf Kemal; Gok, Gamze; Erel, Ozcan

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The role of protein oxidation in the development of diabetic microvascular complications [North Clin Istanb]

North Clin Istanb. 2021; 8(5): 500-506 | DOI: 10.14744/nci.2021.33341

The role of protein oxidation in the development of diabetic microvascular complications

Cuma Mertoglu¹, Gulsah Siranli², T. Abdulkadir Coban², Yucel Karakurt³, Alevtina Ersoy⁴, Adalet Ozcicek⁵, Yusuf Kemal Arslan⁶, Gamze Gok⁷, Ozcan Erel⁷
¹Department of Clinical Biochemistry, Erzincan Binali Yildirim University Faculty of Medicine, Erzincan, Turkey; Department of Clinical Biochemistry, Inonu University Faculty of Medicine, Malatya, Turkey
²Department of Clinical Biochemistry, Erzincan Binali Yildirim University Faculty of Medicine, Erzincan, Turkey
³Department of Ophthalmology, Erzincan Binali Yildirim University Faculty of Medicine, Erzincan, Turkey
⁴Department of Neurology, Erzincan Binali Yildirim University Faculty of Medicine, Erzincan, Turkey
⁵Department of Internal Medicine, Erzincan Binali Yildirim University Faculty of Medicine, Erzincan, Turkey
⁶Department of Biostatistics, Erzincan Binali Yildirim University Faculty of Medicine, Erzincan, Turkey
⁷Department of Clinical Biochemistry, Yildirim Beyazit University Faculty of Medicine, Ankara, Turkey

OBJECTIVE: The role of protein oxidation in the development of diabetic microvascular complications was investigated.
METHODS: In total, 266 participants were split into five groups: Group 1; diabetes mellitus for at least 10 years without any complications, Group 2; diabetic nephropathy, Group 3; diabetic neuropathy, Group 4; diabetic retinopathy, and Group 5; control group. Thiol, disulfide, ferroxidase, and ischemia-modified albumin (IMA) levels were analyzed in the serum.
RESULTS: Native thiol, total thiol, and native thiol/total thiol were lower in Group 4 than Groups 1, 3, and 5 (p<0.001). However, disulfide/native thiol and disulfide/total thiol were higher in Group 4 than all other groups (p<0.001). IMA was higher in Groups 3 and 4 than all other groups (p<0.001). Ferroxidase was lower in Groups 3 and 4 than Group 2 (p<0.001).
CONCLUSION: Thiol-disulfide homeostasis impairment in favor of disulfide may have a function in the progress of diabetic retinopathy. Furthermore, the disruptions of IMA and ferroxidase levels involve in the development of diabetic retinopathy and neuropathy.

Keywords: Diabetes mellitus, microvascular complications; neuropathy; retinopathy; thiol-disulfide.

Diyabetik mikrovask�ler komplikasyonlar�n geli�iminde protein oksidasyonunun rol�

Cuma Mertoglu¹, Gulsah Siranli², T. Abdulkadir Coban², Yucel Karakurt³, Alevtina Ersoy⁴, Adalet Ozcicek⁵, Yusuf Kemal Arslan⁶, Gamze Gok⁷, Ozcan Erel⁷
¹Erzincan Binali Y�ld�r�m �niversitesi T�p Fak�ltesi, Klinik Biyokimya Anabilim Dal�, Erzincan; �n�n� �niversitesi T�p Fak�ltesi Klinik Biyokimya Anabilim Dal�, Malatya
²Erzincan Binali Y�ld�r�m �niversitesi T�p Fak�ltesi, Klinik Biyokimya Anabilim Dal�, Erzincan
³Erzincan Binali Y�ld�r�m �niversitesi T�p Fak�ltesi, G�z Hastal�klar� Anabilim Dal�, Erzincan
⁴Erzincan Binali Y�ld�r�m �niversitesi T�p Fak�ltesi, N�roloji Anabilim Dal�, Erzincan
⁵Erzincan Binali Y�ld�r�m �niversitesi T�p Fak�ltesi, Dahiliye Anabilim Dal�, Erzincan
⁶Erzincan Binali Y�ld�r�m �niversitesi T�p Fak�ltesi, Biyoistatistik Anabilim Dal�, Erzincan
⁷Y�ld�r�m Beyaz�t �niversitesi T�p Fak�ltesi, Klinik Biyokimya Anabilim Dal�, Ankara

AMA�: Diyabetik mikrovask�ler komplikasyonlar�n geli�iminde protein oksidasyonunun rol� ara�t�r�ld�.
Y�NTEMLER: Toplamda 266 kat�l�mc� 5 gruba ayr�ld�: Grup 1; en az 10 y�ld�r herhangi bir komplikasyon olmaks�z�n diabetes mellitus, Grup 2; diyabetik nefropati, Grup 3; diyabetik n�ropati, Grup 4; diyabetik retinopati, Grup 5; kontrol grubu. Serumda tiyol, dis�lfid, ferroksidaz ve iskemik modifiye edilmi� alb�min (�MA) d�zeyleri analiz edildi.
BULGULAR: Nativ tiyol, toplam tiyol ve nativ tiyol/toplam tiyol grup 4'te, grup 1, 3 ve 5'e g�re daha d��kt� (p <0,001). Fakat, dis�lfid/nativ tiyol ve dis�lfid/toplam tiyol, 4. grupta di�er t�m gruplardan daha y�ksekti (p <0.001). �MA, 3. ve 4. gruplarda di�er t�m gruplardan daha y�ksekti (p <0.001). Feroksidaz, 3. ve 4. gruplarda 2. gruptan daha d��kt� (p <0.001).
SONU�LAR: Dis�lfid lehine tiyol-dis�lfid homeostaz bozuklu�u, diyabetik retinopatinin geli�iminde i�lev g�rebilir. Ayr�ca, �MA ve feroksidaz seviyelerinin bozulmas�, diyabetik retinopati ve n�ropatinin geli�imine katk�da bulunur. (NCI-2020-0347.R1)

Anahtar Kelimeler: �eker hastal��, Mikrovask�ler komplikasyonlar; Tiyol-dis�lf�d, Retinopati, N�ropati

Corresponding Author: Cuma Mertoglu
Manuscript Language: English

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