Deneysel beyin travmas� olu�turulan s��anlarda erken tan� i�in sell�ler prion protein(PrPC)�nin de�erlendirilmesi

Kural, Alev; Tekin Neijmann, Sebnem; Toker, Aysun; Do�an, Halil; Sever, Nurten; Sar�kaya, Sezgin

Cilt : 26 Say� : 1 Y�l : 2024

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Deneysel beyin travmas� olu�turulan s��anlarda erken tan� i�in sell�ler prion protein(PrPC)�nin de�erlendirilmesi [Ulus Travma Acil Cerrahi Derg]

Ulus Travma Acil Cerrahi Derg. 2020; 26(1): 1-8 | DOI: 10.5505/tjtes.2018.46923

Deneysel beyin travmas� olu�turulan s��anlarda erken tan� i�in sell�ler prion protein(PrPC)�nin de�erlendirilmesi

Alev Kural¹, Sebnem Tekin Neijmann¹, Aysun Toker², Halil Do�an³, Nurten Sever⁴, Sezgin Sar�kaya⁵
¹Bak�rk�y Dr. Sadi Konuk E�itim ve Ara�t�rma Hastanesi, Biyokimya B�l�m�, �stanbul
²Karaman �zel Hastanesi, Biyokimya B�l�m�, Karaman
³Bak�rk�y Dr. Sadi Konuk E�itim ve Ara�t�rma Hastanesi, Acil T�p B�l�m�, �stanbul
⁴Bak�rk�y Dr. Sadi Konuk E�itim ve Ara�t�rma Hastanesi, Patoloji B�l�m�, �stanbul
⁵Yeditepe �niversitesi, Acil T�p Anabilim Dal�,�stanbul

AMA�: Travmatik beyin yaralanmas� �nemli bir problem olmas�na ra�men, tan�da yard�mc� olan yayg�n kullan�ml� bir n�ro-biyobelirte� yoktur. Bu �al��ma, S100B ve prion protein (PrPC) d�zeylerini travmatik beyin yaralanmas� olu�turulan s��anlarda de�erlendirmeyi ama�lamaktad�r.
GERE� VE Y�NTEM: On be� albino cinsi s��an; sham (1), kontrol (6) ve travma (8) olarak �� gruba ayr�ld�. Travmatik beyin yaralanmas� modifiye serbest d��me modeli ile olu�turuldu. S100B, PrPC d�zeyleri ELISA y�ntemi ile �l��ld�. Beyin �rnekleri patolojik inceleme i�in ��kar�ld�.
BULGULAR: Serum S100B ve PrPc d�zeyleri travma grubunda, travmadan sonraki 2. ve 24. saatlerde y�ksek bulundu (s�ras�yla, p<0.002, p<0.002). Ayr�ca travma grubundan al�nan beyin �rneklerinde histopatolojik yaralanma skoru y�ksek bulundu. Sadece serum PrPc d�zeyleri ile ��kar�lan beyin dokusundaki yaralanma skoru aras�nda pozitif korelasyon vard� (p=0.039, r= 0.731). ROC analizi ile iki parametre incelendi�inde travmatik beyin yaralanmas�n�n tan�s�nda sensitivite ve spesifitesi ayn� bulundu.
TARTI�MA: S100B ve PrPc d�zeyleri bizim deneysel modelimizde tan�da iyi sensitiviteye sahiplerdi. PrPc travmatik beyin yaralanmas� ile gelen hastalarda g�venilir bir belirte� olarak kullan�labilir. Bu biyo-belirte�in tan�sal de�erini g�sterecek klinik �al��malara ihtiya� vard�r.

Anahtar Kelimeler: S100B, sell�ler prion protein (PrPC), travmatik beyin hasar�.

Evaluation of rat major celluler prion protein for early diagnosis in experimental rat brain trauma model

Alev Kural¹, Sebnem Tekin Neijmann¹, Aysun Toker², Halil Do�an³, Nurten Sever⁴, Sezgin Sar�kaya⁵
¹Department of Biochemistry, Bak�rk�y Dr. Sadi Konuk Training and Research Hospital, �stanbul-Turkey
²Department of Biochemistry, Karaman Private Hospital, Karaman-Turkey
³Department of Emergency Medicine, Bak�rk�y Dr. Sadi Konuk Training and Research Hospital, �stanbul-Turkey
⁴Department of Pathology, Bak�rk�y Dr. Sadi Konuk Training and Research Hospital, �stanbul-Turkey
⁵Department of Emergency Medicine, Yeditepe University Faculty of Medicine, �stanbul-Turkey

BACKGROUND: Although traumatic brain injury (TBI) is an important problem, there has been no widespread utilization of neuro-biomarkers to aid the diagnosis of TBI. This study was conducted to evaluate serum S100B and prion protein (PrPC) levels in rats with TBI.
METHODS: In this study, 15 albino rats were categorized into three groups as follows: sham-operated (1), control (6) and trauma (8) groups. The TBI model was based on the modified free falling model. S100B, PrPC levels were measured using ELISA. Brain specimens were obtained for the pathological examination.
RESULTS: Serum S100B and PrPC levels were found to increase in T group at both 2h and 24h after trauma (p<0.002, p<0.002, respectively). We also found higher histopathological injury scores of brain tissues in the T group. Only a positive correlation was found between serum PrPC levels and the extent of brain injury (p=0.039, r=0.731). Using ROC analysis, among the two serum markers investigated, both of them revealed the same sensitivity and specificity for diagnosing TBI.
CONCLUSION: The changes in serum S100B and PrPC levels showed good sensitivity in our experimental model. Therefore, PrPC could be helpful in the early prognostic prediction in patients with TBI. Further studies are needed to test our findings in humans following TBI (penetrating bodies, blunt trauma) to definitively acknowledge it as a reliable biomarker and its subsequent diagnostic utility.

Keywords: Major cellular protein prion (PrPC), S100B; traumatic brain injury.

Sorumlu Yazar: Alev Kural, T�rkiye
Makale Dili: �ngilizce

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