Shivers R R, Edmonds C L, Del Maestro R F
Acta Neuropathol. 1984;64(3):192-202. doi: 10.1007/BF00688109.
Brain tumors, benign and malignant, are characteristically more permeable to various types of tracer molecules than the neuropil in which they are embedded. Impermeability of brain neuropil capillaries is imparted by the blood-brain barrier, the anatomic basis of which is the network of interendothelial zonulae occludentes that seal capillary endothelial cells. To explore both the vascular elements of brain neoplasms and the route of tracer extravasation from them, as well as the possible effects of brain tumors on the permeability of peritumoral neuropil capillaries, brain tumors were induced in newborn Wistar rats by intracerebral (i.c.) injection of C-6 astrocytoma cells. The protein tracer horseradish peroxidase (HRP) was injected systemically into both normal and tumor-bearing rats to mark the pathway along which it flowed into the tumor parenchyma tissue spaces, and to signal any concomitant tracer loss from the tumor extracellular compartment or peritumoral brain capillaries, into the neuropil extracellular milieu. Electron-microscopic examination of thin plastic sections of tumor and peritumoral neuropil revealed massive extravasation of tracer into the tumor tissue spaces, but none was seen outside of the capillaries in the surrounding brain neuropil. Zonulae occludentes of both tumor capillary endothelium and brain capillary endothelium were devoid of tracer and judged tight (sealed). Tracer was seen in pinocytotic vesicles in the highly attenuated endothelium of tumor capillaries and also in cytoplasmic vesicles within the tumor cells. The peritumoral and contralateral neuropil capillary endothelium exhibited reaction product-filled pinocytotic vesicles and vesiculo-tubular conduits. Often, one end of a HRP-filled vesiculo-tubular channel appeared continuous with either the luminal or abluminal plasmalemma. High-voltage electron microscopy of these conduits often showed them to be continuous with both luminal and abluminal surfaces of the endothelium, thus forming a continuum across the capillary wall. In addition, these transendothelial channels, clearly constituted as chains of fused vesicles, were often seen in close proximity to, or fused with, dense bodies in the endothelial cytoplasm. In spite of the presence of HRP-filled structures in the peritumoral neuropil capillary endothelium of tumor-bearing rats, no evidence of tracer extravasation from these vessels was apparent. These results suggest that although peritumoral and contralateral neuropil capillaries possess the machinery for extravasation of tracer, likely as a response to the presence of the neoplasm, tracer is not lost but, instead, is degraded by endothelial enzymes.(ABSTRACT TRUNCATED AT 400 WORDS)
良性和恶性脑肿瘤的特征是,相较于其所处的神经纤维,它们对各种示踪分子的渗透性更强。血脑屏障赋予了脑内神经纤维毛细血管不渗透性,其解剖学基础是封闭小带网络,该网络封闭了毛细血管内皮细胞。为了探究脑肿瘤的血管成分、示踪剂从肿瘤渗出的途径,以及脑肿瘤对肿瘤周围神经纤维毛细血管渗透性可能产生的影响,通过脑内(i.c.)注射C-6星形细胞瘤细胞,在新生Wistar大鼠中诱导产生脑肿瘤。将蛋白质示踪剂辣根过氧化物酶(HRP)全身注射到正常大鼠和荷瘤大鼠体内,以标记其流入肿瘤实质组织间隙的途径,并标记肿瘤细胞外间隙或肿瘤周围脑毛细血管中示踪剂的任何伴随损失,以及向神经纤维细胞外环境中的损失。对肿瘤和肿瘤周围神经纤维的超薄塑料切片进行电子显微镜检查发现,示踪剂大量渗入肿瘤组织间隙,但在周围脑内神经纤维的毛细血管外未见示踪剂。肿瘤毛细血管内皮和脑毛细血管内皮的封闭小带均未发现示踪剂,判定为紧密(封闭)。在肿瘤毛细血管高度变薄的内皮细胞的吞饮小泡中以及肿瘤细胞内的胞质小泡中可见示踪剂。肿瘤周围和对侧神经纤维毛细血管内皮表现出充满反应产物的吞饮小泡和囊泡管状通道。通常,一个充满HRP的囊泡管状通道的一端似乎与管腔或管腔外质膜连续。对这些通道进行高压电子显微镜检查时,常常显示它们与内皮的管腔和管腔外表面均连续,从而在毛细血管壁上形成一个连续体。此外,这些跨内皮通道显然由融合的小泡链构成,经常可见它们靠近内皮细胞质中的致密体或与之融合。尽管在荷瘤大鼠的肿瘤周围神经纤维毛细血管内皮中存在充满HRP的结构,但未发现这些血管有示踪剂外渗的明显证据。这些结果表明,尽管肿瘤周围和对侧神经纤维毛细血管具备示踪剂外渗的机制,这可能是对肿瘤存在的一种反应,但示踪剂并未丢失,而是被内皮酶降解。(摘要截选至400字)
