Hyperglycemia with or without insulin resistance triggers different structural changes in brain microcirculation and perivascular matrix
Tarih
2023Yazar
Yigit, Buket
Gursoy-Ozdemir, Yasemin
Karahuseyinoglu, Sercin
Zeybel, Mujdat
Yapici-Eser, Hale
Pekmez, Murat
Kizilirmak, Ali B.
Kesibi, Judy
Ozler, Ceyda
Sapanci, Selin
Shomalizadeh, Narges
Ozkan, Esra
Cetin-Tas, Yagmur
Sekerdag, Emine
Üst veri
Tüm öğe kaydını gösterÖzet
Both type-1 and type-2 DM are related to an increased risk of cognitive impairment, neurovascular complications, and dementia. The primary triggers for complications are hyperglycemia and concomitant insulin resistance in type-2 DM. However, the diverse mechanisms in the pathogenesis of diabetes-related neurovascular complications and extracellular matrix (ECM) remodeling in type-1 and 2 have not been elucidated yet. Here, we investigated the high fat-high sucrose (HFHS) feeding model and streptozotocin-induced type-1 DM model to study the early effects of hyperglycemia with or without insulin resistance to demonstrate the brain microcirculatory changes, perivascular ECM alterations in histological sections and 3D-reconstructed cleared brain tissues. One of the main findings of this study was robust rarefaction in brain microvessels in both models. Interestingly, the HFHS model leads to widespread non-functional angiogenesis, but the type-1 DM model predominantly in the rostral brain. Rarefaction was accompanied by basement membrane thickening and perivascular collagen accumulation in type-1 DM; more severe blood-brain barrier leakage, and disruption of perivascular ECM organization, mainly of elastin and collagen fibers' structural integrity in the HFHS model. Our results point out that the downstream mechanisms of the long-term vascular complications of hyperglycemia models are structurally distinctive and may have implications for appropriate treatment options.
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- Makale [92796]