Abstract
Lesions to the nervous system often produce hemorrhage and tissue loss that are difficult, if not impossible, to repair. Therefore, scar formation, inflammation and cavitation take place, expanding the lesion epicenter. This significantly worsens the patient conditions and impairment, increasing neuronal loss and glial reaction, which in turn further decreases the chances of a positive outcome. The possibility of using hemostatic substances that also function as a scaffold, such as the fibrin sealant, reduces surgical time and improve postoperative recovery. To date, several studies have demonstrated that human blood derived fibrin sealant produces positive effects in different interventions, becoming an efficient alternative to suturing. To provide an alternative to homologous fibrin sealants, the Center for the Study of Venoms and Venomous Animals (CEVAP, Brazil) has proposed a new bioproduct composed of certified animal components, including a thrombin-like enzyme obtained from snake venom and bubaline fibrinogen. Thus, the present review brings up to date literature assessment on the use of fibrin sealant for nervous system repair and positions the new heterologous bioproduct from CEVAP as an alternative to the commercial counterparts. In this way, clinical and pre-clinical data are discussed in different topics, ranging from central nervous system to peripheral nervous system applications, specifying positive results as well as future enhancements that are necessary for improving the use of fibrin sealant therapy.
Similar content being viewed by others
Background
The nervous system is immensely complex and responsible for most of the biological responses and maintenance of homeostasis. It is, however, subject to injuries and pathologies that usually require surgical intervention. Due to its cellular organization, high vascularization and the presence of the blood–brain barrier, to interfere in the nervous tissue parenchyma constitutes a major challenge. The possibility of using a biological scaffold to provide hemostasis, reestablishment of subarachnoid space tightness as well as a vehicle for drug and stem cell delivery opened a new and promising field of research.
The use of homologous commercial fibrin sealants (FS) in a number of surgical procedures is now consolidated as an efficient method to avoid suturing, enhancing success ratio and reducing patient recovery time. To provide an alternative to human blood derived fibrin sealants, the Center for the Study of Venoms and Venomous Animals (CEVAP – UNESP) has proposed a new heterologous bioproduct composed of certified animal components, including a thrombin-like enzyme obtained from snake venom and a buffalo-cryoprecipitate rich in fibrinogen [1–4]. After more than 20 years of efforts, this study is now under clinical trials [5–10].
The present review positions CEVAP heterologous fibrin sealant (HFS) in the context of nervous system repair following trauma and diseases, indicating a possible advantageous use in different instances. Recent literature is provided and discussed in different topics, ranging from central nervous system (CNS) to peripheral nervous system (PNS) applications, specifying positive results as well as future enhancements that are necessary for improving the use of fibrin sealant therapy.
Brain
The use of FS in brain lesions is not restricted to its common use in the treatment and prevention of cerebrospinal fluid (CSF) leaks [11]. It has expanded to a wide range of surgical interventions including as a hemostatic agent following the total or partial extraction of brain tumors and for coaptation of nerves and brain vessels, replacing conventional sutures [11–13]. There are also promising results from combining this valuable adjunct with various drugs and other agents to enhance regenerative and therapeutic effects after a wide spectrum of brain traumas whether accidental, surgical or even congenital [14–17]. Since the early 20th century, fibrin has been used for stopping cerebral hemorrhage and it is currently being employed through the sealant in various reparative procedures [2, 18].
A cerebrospinal fluid fistula is a condition in which there is a leak of CSF to the nasal cavity, due to fracture of the skull, resulting from traumatic causes (accidental or surgical) and non-traumatic causes, also known as spontaneous fistulas [11, 19]. In both cases, the persistent leakage of CSF might cause complications that are responsible for significant mortality and morbidity [20]. Most leaks provoked by head trauma will seal without intervention; however, spontaneous or surgically-induced leaks often require operative repair [20].
Some authors described treatment by FS of acute (intraoperative) cerebrospinal fluid leaks [21, 22]. Green et al. [21] evaluated FS as an adjunct to sutured dural repair to obtain intraoperative watertight closure in patients undergoing elective cranial surgery. The study demonstrated the superiority of FS over sutures in establishing intraoperative tight closure of a dural incision. Furthermore, Hobbs et al. [22] demonstrated the effectiveness of FS in 120 patients undergoing pituitary surgery procedures with intraoperative CSF leaks. All intraoperative leaks were managed using the FS with different materials, resulting in a low incidence of postoperative CSF leakage.
Other authors described FS as preventing postoperative cerebrospinal fluid leaks [23, 24]. Its use was predominantly in cranial procedures with low incidences of postoperative CSF leaks [11]. Many cases involving patients undergoing transsphenoidal surgery in which postoperative CSF leaks significantly decreased were reported [11]. For example, Yoshimoto et al. [23] evaluated a FS for prevention of postoperative extra dural fluid collection through the dural sutures in patients undergoing craniotomy for an unruptured aneurysm. Once again, the study demonstrated the superiority of the fibrin sealant over sutures. Furthermore, a retrospective (historical) study by Kassam et al. [24] evaluated the efficacy and cost-effectiveness of fibrin in patients with intracranial pathological lesions. The incidence of CSF leaking in matched groups treated with FS or without it were compared. There were no cases of CSF leak in the group of patients receiving FS. Thus, the authors conclude that the FS reduces the incidence of postoperative CSF leaks.
Recent studies in animal models are corroborating the hypothesis that FS prevents CSF leakage. Hutchinson et al. [25] compared two available FS with a synthetic polyethylene glycol (PEG) hydrogel sealant in a canine durotomy repair model. This well-characterized model employed 27 mongrel dogs to assess the ability of sealants to achieve intraoperative tight seals of the dura mater, as well as long-term safety and efficacy. The application of these sealants was 100% effective in preventing CSF leakage.
Finally, a few authors described FS as a treatment for persistent CSF leaks. Cappabianca et al. [26] locally injected FS in patients following different neurosurgical procedures. The injection of FS has proven to be effective in filling or sealing postoperative recesses and treating minor or initial CSF leaks, adding another possibility for threatening postoperative leaks.
Besides CSF leaks, postoperative subdural fluid collection (SFC) is another complication of craniotomy, being most frequently employed after aneurysm surgery [27]. Most SFC cases eventually disappear or are clinically asymptomatic. However, some SFCs enlarge, leading to hygromas or subdural hematomas, which require surgical treatment [27]. In this sense, arachnoid plasty has been demonstrated to be effective for preventing SFC. Several arachnoid plasty methods have been reported including its sealing with FS or covering with appropriate materials and FS. Thus, Abe et al. [27] examined the efficacy of arachnoid plasty with collagen sheet and FS after the clipping of unruptured aneurysms. The procedure achieved favorable outcomes with zero incidence of SFC or complications such as surgical infection.
Lee et al. [12] described a series of 26 patients who underwent microneurosurgical operations in which FS was used. The patients had various neurological disorders: 11 had cerebral aneurysms, 11 had brain tumors, two had lipomyelomeningoceles, one had cerebral arteriovenous malformation and one had torn dura resulting from a mastoidectomy. The FS was tested and effective in the following procedures: reinforcement of aneurysmal clipping; local hemostasis; protection of cerebral veins and sealing of CSF leakage.
Fujimura et al. [13] studied the incidence of chronic hydrocephalus by analyzing a series of 39 patients with subarachnoid hemorrhage, who underwent perivascular coating with FS of cerebral arteries after clipping of an aneurysm. The authors concluded that there were no complications caused by FS and that it protected the cerebral arteries during the acute phase.
Furthermore, there are also promising results associating fibrin sealants with other components, even in cell therapy. An example of this association is the combination of collagen foil or fleece with FS. It is known that the collagen has been successfully employed as a dural graft for years, but when used in combination with fibrin sealant, it enhances sealing and tissue regeneration properties, positively reflecting on hemostasis and stimulation of tissue repair. Besides, such combination prevents fibrin sealant to be washed away in cases of CSF leakage. Thus, a combination of collagen and FS is effective, safe and biocompatible. No further adverse events, complications or toxicity were reported [14–16, 28, 29].
Another example is the FS association with stem cells. Chen et al. [17] investigated the therapeutic effects of subdural transplantation of inducible pluripotent stem cells (iPS) mixed with fibrin sealant (iPS-FS) on rats with cerebral ischemia induced by middle cerebral artery occlusion (MCAO). They demonstrated that subdural iPS-FS enhances recovery from induced stroke and is able to avoid iatrogenic injury to brain parenchyma, thus comprising a safer alternative approach. In this respect, due to the feasibility of obtaining formulations with varying characteristics (customization), the use of the derived snake venom sealant enables an association with potentially different compounds beneficial for the regeneration process of the nervous system.
Thus, it is evident that the FS is a valuable adjuvant to various microneurosurgical procedures, and potentially useful by contributing to the improvement of surgical techniques related to different disorders and adversities in the brain and surrounding environment.
Spinal cord
Spinal cord injury (SCI) by compression or spondylolisthesis usually results in cavitation and glial scar formation. Biomatrices with immunomodulatory properties are of interest since they may be used to bridge the lesion, reducing the formation of scar tissue, as well as facilitating axonal growth. In this context, FS could act as a carrier for therapeutic agents, such as neurotrophic factors and stem cells [30–32].
Guest et al. [33] combined fibroblast growth factor (FGF) and FS to human Schwann-cell grafts which were engrafted to transected rat spinal cords. Such therapy reduced retrograde axonal degeneration stimulating fiber regeneration throughout the implant. In human patients, a therapeutic combination of FGF and FS was applied to the injured spinal segment and used to prevent postoperative CSF leakage. The treatment resulted in significant motor and sensory improvements [34].
FS can be complexed with FGF and nerve grafts as well. Kuo et al. [35] used autologous peripheral intercostal nerve segments combined with FGF in an FS scaffold, implanted to bridge the 5 mm gap in transected rat spinal cords. FGF treatment induced IL-4 expression while nerve grafts induced nerve grow factor (NGF) and brain-derived neurotrophic factor (BDNF) expression. This combined treatment has also been applied to animals with chronic complete SCI by the removal of scar tissue to expose fresh tissue at the surface of the spinal cord stumps [36]. Such approach restored a degree of hind-limb function [36, 37]. Tsai et al. [38] also treated spinal cord transection with peripheral nerve grafts and spinal cord anastomosis, both including FGF1 in an FS scaffold. Rats recovered both motor-evoked potentials, recorded at the lumbar level and locomotor function due to long tract regeneration.
Proteins can be complexed with fibrin matrix. Lord-Fontaine et al. [39] used rat contusion model and topical application of the protein BA-210 onto the spinal cord using an FS formulation. BA-210 inactivates Rho, which activation is a conserved response in various types of central injuries, thus significantly reducing tissue loss in the perilesional area and rostrocaudal spreading of lesion cavity. Significant walking abilities were regained more rapidly and more consistently in rats treated with BA-210 [39]. Although a previous work has shown a potential scaffold role for FS, which enhanced FGF and BA-210 treatments, FS action itself has not been fully evaluated [39].
FS is already applied by neurosurgeons as a hemostatic agent and for the control of cerebrospinal fluid (CSF) leaks [15, 32, 40–42]. In this sense, postoperative CSF leakage is a known complication of spinal surgery. The ideal material to be used in the dural closure is still a matter of debate [43]. Prompt surgery is recommended to prevent the complications such as meningitis, CSF fistulas, and pseudocyst formation with potential nerve compression [44]. In this regard, FS has been considered effective for prevention of CSF leakage in the field of neurosurgery and spinal surgery [45]. Frequently, durotomy margin is uneven, and watertight dural closure cannot be achieved only by single sutures. In such cases, the use of a sealant is helpful [45–49].
Many authors recommend FS to reinforce the site of durotomy and have reported that the FS-treated patients presented a significantly higher rate of tight closure than controls as well as decreased postoperative drainage output and time spent at the hospital [45, 48–51]. Percutaneous therapy of FS in humans with postoperative CSF leaks generated a 50% success rate, similar to the 56% success rate in rats with direct application of FS alone, after experimental induction of CSF rhinorrhea [44, 52]. Patel et al. [44] recommend autologous cryoprecipitate use whenever possible to avoid the risk of blood-borne pathogens, including hepatitis C. The preparation of cryoprecipitate from autologous blood requires three days, and 500 mL of whole blood generates 20 to 25 mL of cryoprecipitate [44].
An autologous FS has also been used by Nakamura et al. [45] – in comparison to commercial FS – in patients undergoing spinal surgery. No complications such as infection or continuous CSF leak were observed in any case. The volume of drainage fluid was significantly reduced in the group subjected to either autologous or commercial FS, when compared to the group without FS. As to safety, the autologous adhesive was equal to the commercial counterpart. The preventive effects of both adhesives were equivalent, but the autologous adhesive is much cheaper and provides the advantage of being risk-free of transfusion infection.
As a treatment for sacral meningeal cysts, Paulsen et al. [53] determined whether placement of FS after aspiration could offer a more definitive therapy. The use of FS resulted in marked improvement in all patients, with no evidence of pathology recurrence [54].
Although FS use has produced positive results, there are reports of inconsistent outcomes. Thus, in a retrospective analysis done by Balasubramaniam et al. [43], evaluating children submitted to surgery for various spinal pathologies, FS had no effect, though the numbers were statistically too small. Jankowitz et al. [55] reached a similar conclusion that the use of FS did not significantly decrease the incidence of subsequent CSF leakage while studying the potential efficacy of FS TISSEEL® (Baxter) for enhancing dural repair after lumbar spine surgery. Considering the risk of healing inhibition, the findings did not support the prophylactic use of FS when a primary repair is deemed adequate. Augmentation with muscle, fat, FS, or graft should be considered when the dural closure is suboptimal.
When used to fill the lesion gap after SCI, FS provided neuroprotective effects. Tissucol® (Baxter) FS was used by Petter-Puchner et al. [32] after thoracic spinal cord hemisection in rats. Three and seven days after lesion, histology showed a more pronounced inflammatory response triggered by macrophages in the FS-treated group. This difference did not impair behavioral or reflex tests performed at the same time points. At day 28, recruitment of macrophages and microglia had substantially decreased and no intergroup difference was detectable. Substantial benefits were found in relation to motor function and proprioceptive recovery in the FS-treated group [32]. A similar result was achieved after intramedullary axotomy and a new heterologous fibrin sealant (HFS) treatment. The HFS-treated group displayed improved motoneuronal survival after lesion and showed upregulation of iNOS2 and arginase1 genes, proinflammatory (TNFα and IL1β) and antiinflammatory cytokines (IL10, IL4, and IL13). Thus, HFS enhanced early macrophage recruitment and proinflammatory cytokine expression, which contributed to an acceleration of inflammation resolution, shown by the increased expression of M2 macrophage markers and antiinflammatory cytokines. The greater inflammation was coupled with better motor performance in the walking track test [56].
Spinal cord ventral and dorsal roots
Spinal motoneurons are located in the spinal cord ventral horn and send their axon towards the periphery to innervate skeletal muscles. These efferent fibers, among other functions, control the voluntary movements in response to central brain stimulation and/or sensory feedback. Afferent fibers bring sensorial information (touch, temperature, pressure, pain and proprioception) from the periphery to the CNS through the dorsal roots. Sensorial feedback and motor control are crucial in our everyday life, given their roles in the controlling and adjusting of movements and in adaption to environmental changes [57]. Unfortunately, nerve roots can be damaged, thereby disrupting complex and highly specialized neural networks, impairing neural signal transmission.
A schematic view of dorsal and ventral nerve roots, as well as structures of gray and white matter, are represented in Fig. 1. It also illustrates the ventral root avulsion and dorsal root section lesions. Axons in the white matter are highlighted with the program AxonSeg, available online [58].
Schematic view of dorsal and ventral nerve roots. Sensory neurons bring sensory inputs through the dorsal roots, which are transmitted to the motoneurons via interneurons. Motoneurons send their axons through ventral roots that innervate target muscles. Dorsal root lesion and ventral root avulsion have been used to evaluate the efficacy of the CEVAP heterologous fibrin sealant (HFS) for CNS repair and regeneration. The inset shows presynaptic terminals in apposition to motoneurons that retract after injury (synapse pruning). Myelinated axons located in the white matter are highlighted (top left) by using AxonSeg, an open source software for axon morphometry [58]
Proximal root injury, differently from peripheral nerve lesion, results in extensive degeneration of adult motoneurons and loss of sensory feedback since axons cannot regenerate into the spinal cord [59, 60]. When this injury happens in an abrupt traction, it is called avulsion [61, 62]. Such lesion or damage frequently occurs in severe brachial plexus injuries due to the high impact of the trauma [61]. In cats and dogs, avulsion is normally associated with being hit by vehicles [63, 64]. Nevertheless, in humans, it often happens in vehicle or sport accidents with limb traction or shoulder depression. In such accidents, the brachial plexus can be damaged when the head is pushed away from the shoulder [57, 65]. Compression or crushing, industrial trauma, and iatrogenic injury are mechanisms that can also produce root avulsion [61, 62]; and a similar lesion can also happen in the newborn during childbirth [57].
The disconnection of spinal motoneurons from the muscle fibers interrupts the anterograde flow of neurotrophic factors, leading to neuronal degeneration and skeletal muscle paralysis. On the contrary, deafferentation after dorsal root disconnection does not result in significant dorsal root ganglia neuronal death, although it leads to loss of sensory feedback [66, 67]. Overall, root lesions trigger several long-lasting structural changes in the CNS, affecting not only local spinal cord circuits but also the entire motor pathway, including the motor cortex [68, 69].
Extensive synaptic plasticity occurs in the motoneuron cell body in response to ventral root avulsion, with preferential loss of excitatory inputs [70, 71]. In turn, such imbalance of synaptic connections impairs voluntary movements and may cause neuropathic pain and/or hyperalgesia. Additionally, proximal lesions also break the blood–brain barrier, facilitating the influx of blood-borne cells, increasing inflammation and glial reaction [65, 72–76]. Reactive astrocytes participate in presynaptic terminal retraction from the surface of injured motoneurons, so that reducing inflammation usually preserves spinal cord circuits and facilitates regeneration [74, 77].
The clinical effect of root injury is not only restricted the loss of limb function ipsilateral to the lesion, but also several other subsequent clinical complications, such as meningeal cysts, intractable pain, impaired blood circulation, herniation and monoplegia [57, 62]. From the point of view of the patient, brachial plexus injury is devastating, leading to unemployment, economic hardship, and depression.
Poor recovery of function after brachial plexus avulsion can occur due to considerable distances through which motoneuron axons must regenerate to reconnect with the target muscles and the slow growth velocity of the regenerating axons, which cannot reach muscles before irreversible atrophy [78–80]. Also, when regenerating, afferent axons from the dorsal root ganglia reach the inhibitory environment of the spinal cord, being unable to reenter the CNS and reestablish functional connections [81]. On this matter, various attempts to promote regeneration after root lesion have been reported. Previous efforts to repair ventral roots were performed in rats by Carlstedt et al. [82] followed by Cullheim et al. in cats [83]. In these studies, the avulsed ventral roots were reimplanted on the surface of spinal cord lateral funiculus. A similar technique was applied to humans; however, with limited success [57, 84]. Further experimental ventral root implant approaches were carried out using 9/0 non-absorbable sutures (EthilonH®), lithium chloride, tissue glue (TisseelH®), fibrin sealant (TissueCol®; Baxter BVUtrecht, the Netherlands), nerve grafting, biodegradable scaffolds and nerve transfer [79, 85–91]. For dorsal root repair, some promising results towards regeneration were obtained by using inhibitors of chondroitin sulfate proteoglycans, myelin associated proteins, and by knocking down neurotrophin receptors [92–103].
The heterologous fibrin sealant derived from snake venom (HFS), alone or in association with cell therapy, has already shown promising results in the treatment of dorsal and ventral root injuries [67, 104]. Figure 1 shows the dorsal root rhizotomy. The HFS usage to reconnect ventral and dorsal roots also resulted in the statistically significant preservation of injured motoneurons, improved synaptic circuitry recovery, upregulation of trophic factors, and substantial recovery of sensory and motor function [67, 104–107]. Such studies provide a novel approach for treating spinal cord root lesions, aiming at restoring CNS/PNS interface integrity.
Vidigal de Castro et al. [107] showed a significant restoration of weight-bearing capacity following ventral root avulsion (VRA) and reimplantation with the heterologous (HFS) and commercial fibrin sealant (FS), showed by the overview of CatWalk System (Fig. 2) and Additional file 1 (VRA only), Additional file 2 (VRA + HFS) and Additional file 3 (VRA + FS).
Paw prints and walking profile after ventral root avulsion and treatment with two different fibrin sealants, obtained with the CatWalk System (Noldus®). a-c Preoperative; d-f ventral root avulsion (VRA) only; g-i VRA followed by reimplantation with new heterologous fibrin sealant derived from snake venom (VRA + HFS); j-l VRA followed by reimplantation with commercial fibrin sealant (VRA + FS). It is possible to observe that (h and k) root reimplantation results in paw print partial recovery, whereas (e) avulsion alone leads to permanent paralysis
Peripheral nervous system
Peripheral nerve injuries lead to the disconnection of the nervous system with target organs, resulting in paralysis and numbness. Incomplete injuries usually cause pharmacologically resistant neuropathic pain [108]. Thus, the primary concern after nerve lesion is to secure the anatomical continuity, allowing regeneration of the axons towards the periphery.
End-to-end coaptation, with or without grafting is the gold-standard technique used to repair a sectioned peripheral nerve [109, 110]. Thus, the surgical approach depends on the degree of the lesion. Direct nerve repair with epineural suturing is possible when a tension-free adjustment and adequate vascularization can be achieved. When there is a gap between the stumps, generating significant tension for direct epineural repair, the interposition of autologous nerve grafts is required. In acute and clean nerve transection, the primary repair should be performed as soon as possible to improve neuronal survival and decrease fibrosis of the distal stump.
Minimizing the number of sutures can also decrease iatrogenic nerve tissue trauma. In this sense, alternative repair techniques have been studied in order to improve the stability of end-to-end coaptation. Tissue adhesives, such as the fibrin sealant, can either supplement or replace sutures and present advantages including reduction of surgery time [111, 112]. Besides, the FS may reduce suture-associated inflammation and enhance axonal regeneration [113].
A study comparing the use of FS alone, suturing and the combination of both techniques after sciatic nerve injury showed that fibrin sealant presented better results than suturing considering recovery of evoked motor action potential [114]. Other studies comparing the use of FS associated with peroneal nerve tubulization demonstrate that FS allows nerve regeneration and functional recovery without formation of neuroma [115, 116].
End-to-side coaptation has been proposed to repair peripheral nerves in the absence of the proximal stump. When associated with FS in rats, a greater number of regenerating fibers and improved motor recovery were observed [117].
Additional to FS coaptation, the use of neuroprotective and pro-regenerative substances, such as atorvastatin, was analyzed after sciatic nerve lesion demonstrating beneficial effects on muscle strength [118–121].
Wood et al. [122] evaluated the effects of glial cell-derived neurotrophic factor (GDNF) microspheres associated with FS, showing improvement in axonal regeneration and size of regrown axons. Tubular conduits prepared from FS can also improve short- and long-term regeneration following peripheral nerve injury, with regard to axonal sprouting and muscle weight recovery [123, 124]. Also, the evaluation of FS with bone marrow mononuclear stem cells on sciatic nerve injury demonstrated better results compared with FS alone as to morphometric parameters [125].
Importantly, the better understanding of nerve regeneration approaches requires careful evaluation of motor and sensory behavior. Such functional recovery is crucial for validation of morphological and molecular (e.g. gene expression) data [126]. In this sense, our group has dedicated much effort to combine reparative approaches with histological and molecular analyses and behavioral tests in order to improve the completeness of the results and findings [127, 128].
The fibrin sealant derived from snake venom (HFS) has been used for rat neonatal sciatic nerve coaptation facilitating the regenerative process. Furthermore, the comparison between HFS with another commercially available sealant (FS) revealed that both present similar performance in peripheral nerve repair [127]. Additional files 4, 5 and 6 illustrate normal gait pattern, evaluation after neonatal sciatic nerve axotomy and following coaptation, respectively.
An early study comparing HFS with other commercially available sealants showed that the new sealant promoted adequate sciatic nerve adherence and repair, highlighting that the nerve without repair showed extensive fibrosis and absence of nerve fibers [129]. More recently, another study using HFS, performed to evaluate functional recovery following sciatic nerve coaptation, showed improved recovery of neurophysiological parameters relative to action potential and muscle reinnervation [130]. The use of low-level laser therapy (LLLT) was also tested with HFS to observe the collateral repair of axons originating from the vagus nerve to the interior of a sural nerve graft, demonstrating that the HFS supports axonal regeneration [131]. Cartarozzi et al. [128] also observed sciatic nerve regeneration after combining mesenchymal stem cells and HFS in a polycaprolactone-based tubular prosthesis after nerve transection. CEVAP heterologous fibrin sealant scaffold combined with cell therapy improved Schwann cell reactivity, myelination and gait recovery.
Conclusions
Biological sealants have long been used in research to provide a scaffold for substances and regrowth of axons and have been employed in neurosurgery for over 20 years without inducing damage to the nervous system [86, 101, 102, 132]. Sealant efficacy is similar or even better when compared to sutures in most of the cases [133–137]. However, commercial sealants have the disadvantage of using human blood that can lead to eventual transmission of infectious diseases, necrosis, and seroma formation [2].
As to the repair of nerves, the ideal sealant must possess specific biological, mechanical and structural properties, while presenting minimal risk of disease transmission, antigenicity, and toxicity. Furthermore, the sealant should not induce fibrosis, that can lead to nerve compression, and should not act as a barrier to axon regeneration, thereby preserving normal axon architecture. Adherence produced by the sealant should provide adequate mechanical strength to avoid nerve rupture, providing a stable scaffold for axonal growth. Additionally, it should be easy to handle, reducing operative time.
Taking all the above into account, the new heterologous fibrin sealant from snake venom (HFS) represents a consistent alternative, since it is produced without human blood to avoid transmission of infectious diseases. Its formulation can be customized to surgical needs; the clotting time can be adjusted and degradation time can be controlled. Moreover, HFS prevents fluid loss, promotes tissue adhesion, reduces surgery time and decreases hemorrhage [2, 127]. In addition, it is cheaper than commercial heterologous sealants, since the technology and production processes have been optimized [2, 4].
Abbreviations
- BDNF:
-
Brain-derived neurotrophic factor
- CEVAP:
-
Center for the Study of Venoms and Venomous Animals (Brazil)
- CNS:
-
Central nervous system
- CSF:
-
Cerebrospinal fluid
- FGF:
-
Fibroblast growth factor
- FS:
-
Fibrin sealant
- GDNF:
-
Glial cell-derived neurotrophic factor
- HFS:
-
CEVAP heterologous fibrin sealant
- IL10:
-
Interleukin 10
- IL13:
-
Interleukin 13
- IL-1β:
-
Interleukin 1-beta
- IL4:
-
Interleukin 4
- iPS:
-
Inducible pluripotent stem cells
- iPS-FS:
-
Inducible pluripotent stem cells mixed with fibrin sealant
- LLLT:
-
Low-level laser therapy
- MCAO:
-
Middle cerebral artery occlusion
- NGF:
-
Nerve growth factor
- PEG:
-
Polyethylene glycol
- PNS:
-
Peripheral nervous system
- SCI:
-
Spinal cord injury
- SFC:
-
Subdural fluid collection
- TNF:
-
Tumor necrosis factor
- VRA:
-
Ventral root avulsion
References
Ferreira Junior RS, Barros LC, Abbade LF, Barraviera SS, Silvares MC, Pontes LG, et al. Heterologous fibrin sealant derived from snake venom: from bench to the bedside - an overview. J Venom Anim Toxins incl Trop Dis. 2017.
Barros LC, Ferreira Junior RS, Barraviera SR, Stolf HO, Thomazinni-Santos IA, Mendes-Giannini MJ, et al. A new fibrin sealant from Crotalus durissus terrificus venom: applications in medicine. J Toxicol Environ Health B Crit Rev. 2009;12(8):553–71. doi:10.1080/10937400903442514.
Barros LC AMS, Costa FL, Rodrigues VM, Fuly AL, Giglio JR, et al. Biochemical and biological evaluation of gyroxin isolated from Crotalus durissus terrificus venom. J Venom Anim Toxins incl Trop Dis. 2011;17(1):10.
Ferreira Junior RS. Autologous or heterologous fibrin sealant scaffold: which is the better choice? J Venom Anim Toxins incl Trop Dis. 2014;20:31. doi:10.1186/1678-9199-20-31.
Stolf HO. The use of fibrin adhesive derived from snake venom and the evaluation of skin grafting using skin from the patient’s nasolabial fold. J Venom Anim Toxins. 1999;5(2):227.
Barbosa MD, Gregh SL, Passanezi E. Fibrin adhesive derived from snake venom in periodontal surgery. J Periodontol. 2007;78(10):2026–31. doi:10.1902/jop.2007.070005.
Barbosa MD, Stipp AC, Passanezi E, Greghi SL. Fibrin adhesive derived from snake venom in periodontal surgery: histological analysis. J Appl Oral Sci. 2008;16(5):310–5.
Chiquito GCM. Comparison between suture and fibrin adhesive derived from snake venom for fixation of connective tissue graft in correction of marginal tissue recession. J Venom Anim Toxins incl Trop Dis. 2007;13(2):559.
Gatti MAN, Vieira LM, Barraviera B, Barraviera SRCS. Treatment of venous ulcers with fibrin sealant derived from snake venom. J Venom Anim Toxins incl Trop Dis. 2011;17(2):4.
Abbade LPF, Barraviera SRCS, Silvares MRC, Carneiro MTR, Medolago NB, Ferreira Jr RS, et al. A new fibrin sealant derived from snake venom candidate to treat chronic venous ulcers. J Am Acad Dermatol. 2015;72(5 Supplement 1):AB271.
Esposito F, Angileri FF, Kruse P, Cavallo LM, Solari D, Esposito V, et al. Fibrin sealants in dura sealing: a systematic literature review. PLoS One. 2016;11(4), e0151533. doi:10.1371/journal.pone.0151533.
Lee KC, Park SK, Lee KS. Neurosurgical application of fibrin adhesive. Yonsei Med J. 1991;32(1):53–7.
Fujimura M, Sugawara T, Seki H, Oku T, Niimura K, Otawara Y, et al. Perivascular coating with fibrin glue of cerebral arteries in patients with aneurysmal subarachnoid hemorrhage; incidence of chronic hydrocephalus. Tohoku J Exp Med. 1996;179(4):267–72.
Cappabianca P, Cavallo LM, Valente V, Romano I, D’Enza AI, Esposito F, et al. Sellar repair with fibrin sealant and collagen fleece after endoscopic endonasal transsphenoidal surgery. Surg Neurol. 2004;62(3):227–33. doi:10.1016/j.surneu.2004.01.016. discussion 233.
Cappabianca P, Esposito F, Cavallo LM, Messina A, Solari D, di Somma LG, et al. Use of equine collagen foil as dura mater substitute in endoscopic endonasal transsphenoidal surgery. Surg Neurol. 2006;65(2):144–8. doi:10.1016/j.surneu.2005.08.023. discussion 149.
Parlato C, di Nuzzo G, Luongo M, Parlato RS, Accardo M, Cuccurullo L, et al. Use of a collagen biomatrix (TissuDura) for dura repair: a long-term neuroradiological and neuropathological evaluation. Acta Neurochir (Wien). 2011;153(1):142–7. doi:10.1007/s00701-010-0718-2.
Chen SJ, Chang CM, Tsai SK, Chang YL, Chou SJ, Huang SS, et al. Functional improvement of focal cerebral ischemia injury by subdural transplantation of induced pluripotent stem cells with fibrin glue. Stem Cells Dev. 2010;19(11):1757–67. doi:10.1089/scd.2009.0452.
Grey EG. Fibrin as a hemostatic in cerebral surgery. Surg Gynecol Obstet. 1915;21:452–4.
Al-Sebeih K, Karagiozov K, Elbeltagi A, Al-Qattan F. Non-traumatic cerebrospinal fluid rhinorrhea: diagnosis and management. Ann Saudi Med. 2004;24(6):453–8.
Rock JP, Sierra DH, Castro-Moure F, Jiang F. Skull base cerebrospinal fluid leakage control with a fibrin-based composite tissue adhesive. Skull Base Surgery. 1996;6(3):137–40.
Green AL, Arnaud A, Batiller J, Eljamel S, Gauld J, Jones P, et al. A multicentre, prospective, randomized, controlled study to evaluate the use of a fibrin sealant as an adjunct to sutured dural repair. Br J Neurosurg. 2014:1–7. doi:10.3109/02688697.2014.948808.
Hobbs CGL, Darr A, Carlin WV. Management of intra-operative cerebrospinal fluid leak following endoscopic trans-sphenoidal pituitary surgery. J Laryngol Otol. 2011;125(3):311–3. doi:10.1017/S0022215110002483.
Yoshimoto T, Sawamura Y, Houkin K, Abe H. Effectiveness of fibrin glue for preventing postoperative extradural fluid leakage. Neurol Med Chir (Tokyo). 1997;37(12):886–9. discussion 889–90.
Kassam A, Horowitz M, Carrau R, Snyderman C, Welch W, Hirsch B, et al. Use of Tisseel fibrin sealant in neurosurgical procedures: incidence of cerebrospinal fluid leaks and cost-benefit analysis in a retrospective study. Neurosurgery. 2003;52(5):1102–5. discussion 1105.
Hutchinson RW, Mendenhall V, Abutin RM, Muench T, Hart J. Evaluation of fibrin sealants for central nervous system sealing in the mongrel dog durotomy model. Neurosurgery. 2011;69(4):921–8. doi:10.1227/NEU.0b013e318222ad63. discussion 929.
Cappabianca P, Esposito F, Magro F, Cavallo LM, Solari D, Stella L, et al. Natura abhorret a vacuo--use of fibrin glue as a filler and sealant in neurosurgical “dead spaces”. Technical note. Acta Neurochir (Wien). 2010;152(5):897–904. doi:10.1007/s00701-009-0580-2.
Abe J, Ichinose T, Terakawa Y, Tsuyuguchi N, Tsuruno T, Ohata K. Efficacy of arachnoid plasty with collagen sheets and fibrin glue: An in vitro experiment and a case review. Surg Neurol Int. 2015;6:90. doi:10.4103/2152-7806.157792.
Cho JM, Ahn JY, Chang JH, Kim SH. Prevention of cerebrospinal fluid rhinorrhea after transsphenoidal surgery by collagen fleece coated with fibrin sealant without autologous tissue graft or postoperative lumbar drainage. Neurosurgery. 2011;68(1 Suppl Operative):130–6; discussion 136–7. doi:10.1227/NEU.0b013e318207b4ea.
Reddy M, Schöggl A, Reddy B, Holzer A, Saringer W, Steiger C, et al. Watertightness and effectiveness of a fibrinogen-based collagen fleece (TachoComb®) in neurosurgery. Eur Surg. 2003;35(5):278–81. doi:10.1007/s10353-003-0027-6.
Iwakawa M, Mizoi K, Tessler A, Itoh Y. Intraspinal implants of fibrin glue containing glial cell line-derived neurotrophic factor promote dorsal root regeneration into spinal cord. Neurorehabil Neural Repair. 2001;15(3):173–82.
Cheng H, Huang SS, Lin SM, Lin MJ, Chu YC, Chih CL, et al. The neuroprotective effect of glial cell line-derived neurotrophic factor in fibrin glue against chronic focal cerebral ischemia in conscious rats. Brain Res. 2005;1033(1):28–33. doi:10.1016/j.brainres.2004.10.067.
Petter-Puchner AH, Froetscher W, Krametter-Froetscher R, Lorinson D, Redl H, van Griensven M. The long-term neurocompatibility of human fibrin sealant and equine collagen as biomatrices in experimental spinal cord injury. Exp Toxicol Pathol. 2007;58(4):237–45. doi:10.1016/j.etp.2006.07.004.
Guest JD, Hesse D, Schnell L, Schwab ME, Bunge MB, Bunge RP. Influence of IN-1 antibody and acidic FGF-fibrin glue on the response of injured corticospinal tract axons to human Schwann cell grafts. J Neurosci Res. 1997;50(5):888–905. doi:10.1002/(SICI)1097-4547(19971201)50:5<888::AID-JNR24>3.0.CO;2-W.
Wu JC, Huang WC, Chen YC, Tu TH, Tsai YA, Huang SF, et al. Acidic fibroblast growth factor for repair of human spinal cord injury: a clinical trial. J Neurosurg Spine. 2011;15(3):216–27. doi:10.3171/2011.4.SPINE10404.
Kuo HS, Tsai MJ, Huang MC, Chiu CW, Tsai CY, Lee MJ, et al. Acid fibroblast growth factor and peripheral nerve grafts regulate Th2 cytokine expression, macrophage activation, polyamine synthesis, and neurotrophin expression in transected rat spinal cords. J Neurosci. 2011;31(11):4137–47. doi:10.1523/JNEUROSCI.2592-10.2011.
Olson L. Combinatory treatments needed for spinal cord injury. Exp Neurol. 2013;248:309–15. doi:10.1016/j.expneurol.2013.06.024.
Fraidakis MJ. Lugaro’s forgotten legacy: the hypothesis of negative neurotropism. J Hist Neurosci. 2010;19(3):239–52. doi:10.1080/09647040903148621.
Tsai EC, Krassioukov AV, Tator CH. Corticospinal regeneration into lumbar grey matter correlates with locomotor recovery after complete spinal cord transection and repair with peripheral nerve grafts, fibroblast growth factor 1, fibrin glue, and spinal fusion. J Neuropathol Exp Neurol. 2005;64(3):230–44.
Lord-Fontaine S, Yang F, Diep Q, Dergham P, Munzer S, Tremblay P, et al. Local inhibition of Rho signaling by cell-permeable recombinant protein BA-210 prevents secondary damage and promotes functional recovery following acute spinal cord injury. J Neurotrauma. 2008;25(11):1309–22. doi:10.1089/neu.2008.0613.
Novikova LN, Novikov LN, Kellerth JO. Biopolymers and biodegradable smart implants for tissue regeneration after spinal cord injury. Curr Opin Neurol. 2003;16(6):711–5. doi:10.1097/01.wco.0000102620.38669.3e.
Kataoka K, Suzuki Y, Kitada M, Hashimoto T, Chou H, Bai H, et al. Alginate enhances elongation of early regenerating axons in spinal cord of young rats. Tissue Eng. 2004;10(3–4):493–504. doi:10.1089/107632704323061852.
Woerly S, Doan VD, Evans-Martin F, Paramore CG, Peduzzi JD. Spinal cord reconstruction using NeuroGel implants and functional recovery after chronic injury. J Neurosci Res. 2001;66(6):1187–97. doi:10.1002/jnr.1255.
Balasubramaniam C, Rao SM, Subramaniam K. Management of CSF leak following spinal surgery. Childs Nerv Syst. 2014;30(9):1543–7. doi:10.1007/s00381-014-2496-2.
Patel MR, Louie W, Rachlin J. Postoperative cerebrospinal fluid leaks of the lumbosacral spine: management with percutaneous fibrin glue. AJNR Am J Neuroradiol. 1996;17(3):495–500.
Nakamura H, Matsuyama Y, Yoshihara H, Sakai Y, Katayama Y, Nakashima S, et al. The effect of autologous fibrin tissue adhesive on postoperative cerebrospinal fluid leak in spinal cord surgery: a randomized controlled trial. Spine (Phila Pa 1976). 2005;30(13):E347–51.
Kim KD, Wright NM. Polyethylene glycol hydrogel spinal sealant (DuraSeal Spinal Sealant) as an adjunct to sutured dural repair in the spine: results of a prospective, multicenter, randomized controlled study. Spine (Phila Pa 1976). 2011;36(23):1906–12. doi:10.1097/BRS.0b013e3181fdb4db.
Tan LA, Takagi I, Straus D, O’Toole JE. Management of intended durotomy in minimally invasive intradural spine surgery: clinical article. J Neurosurg Spine. 2014;21(2):279–85. doi:10.3171/2014.3.SPINE13719.
Yeom JS, Buchowski JM, Shen HX, Liu G, Bunmaprasert T, Riew KD. Effect of fibrin sealant on drain output and duration of hospitalization after multilevel anterior cervical fusion: a retrospective matched pair analysis. Spine (Phila Pa 1976). 2008;33(16):E543–7. doi:10.1097/BRS.0b013e31817c6c9b.
Won YI, Kim CH, Chung CK, Jahng TA, Park SB. The use fibrin sealant after spinal intradural tumor surgery: is it necessary? Korean J Spine. 2016;13(1):24–9. doi:10.14245/kjs.2016.13.1.24.
Dafford EE, Anderson PA. Comparison of dural repair techniques. Spine J. 2015;15(5):1099–105. doi:10.1016/j.spinee.2013.06.044.
Wright NM, Park J, Tew JM, Kim KD, Shaffrey ME, Cheng J, et al. Spinal sealant system provides better intraoperative watertight closure than standard of care during spinal surgery: a prospective, multicenter, randomized controlled study. Spine (Phila Pa 1976). 2015;40(8):505–13. doi:10.1097/BRS.0000000000000810.
Nishihira S, McCaffrey TV. The use of fibrin glue for the repair of experimental CSF rhinorrhea. Laryngoscope. 1988;98(6 Pt 1):625–7. doi:10.1288/00005537-198806000-00009.
Paulsen RD, Call GA, Murtagh FR. Prevalence and percutaneous drainage of cysts of the sacral nerve root sheath (Tarlov cysts). AJNR Am J Neuroradiol. 1994;15(2):293–7. discussion 298–9.
Patel MR, Louie W, Rachlin J. Percutaneous fibrin glue therapy of meningeal cysts of the sacral spine. AJR Am J Roentgenol. 1997;168(2):367–70. doi:10.2214/ajr.168.2.9016209.
Jankowitz BT, Atteberry DS, Gerszten PC, Karausky P, Cheng BC, Faught R, et al. Effect of fibrin glue on the prevention of persistent cerebral spinal fluid leakage after incidental durotomy during lumbar spinal surgery. Eur Spine J. 2009;18(8):1169–74. doi:10.1007/s00586-009-0928-6.
Spejo A, Chiarotto G, Ferreira Junior RS, Barraviera B, Oliveira ALR. Neuroprotection and functional recovery after spinal cord injury followed by mesenchymal stem cell and fibrin sealant treatment. Annals of 2nd FALAN (Federation of Latin American and Caribbean Neuroscience Socities) Congress 2016. p. 127.
Carlstedt T. Nerve root replantation. Neurosurg Clin N Am. 2009;20(1):39–50. doi:10.1016/j.nec.2008.07.020.
Zaimi A, Duval T, Gasecka A, Côté D, Stikov N, Cohen-Adad J. AxonSeg: open source software for axon and myelin segmentation and morphometric analysis. Front Neuroinform. 2016;10:37. doi:10.3389/fninf.2016.00037.
Oliveira AL, Langone F. GM-1 ganglioside treatment reduces motoneuron death after ventral root avulsion in adult rats. Neurosci Lett. 2000;293(2):131–4.
Carlstedt T. Nerve fibre regeneration across the peripheral-central transitional zone. J Anat. 1997;190(Pt 1):51–6.
Teixeira MJ, da Paz MGS, Bina MT, Santos SN, Raicher I, Galhardoni R, et al. Neuropathic pain after brachial plexus avulsion - central and peripheral mechanisms. BMC Neurol. 2015;15:73. doi:10.1186/s12883-015-0329-x.
Thatte MR, Babhulkar S, Hiremath A. Brachial plexus injury in adults: diagnosis and surgical treatment strategies. Ann Indian Acad Neurol. 2013;16(1):26–33. doi:10.4103/0972-2327.107686.
Arias MVB, Stopiglia AJ. Avulsão do plexo braquial em cães. Aspectos clínicos e neurológicos. Brachial plexus avulsion in dogs. Clinical and neurological aspects. Cienc Rural. 1997;27(1):5.
Steinberg HS. Brachial plexus injuries and dysfunctions. Vet Clin North Am Small Anim Pract. 1988;18(3):565–80.
Fraher JP. The transitional zone and CNS regeneration. J Anat. 1999;194(Pt 2):161–82.
Oliveira AL, Hydling F, Olsson E, Shi T, Edwards RH, Fujiyama F, et al. Cellular localization of three vesicular glutamate transporter mRNAs and proteins in rat spinal cord and dorsal root ganglia. Synapse. 2003;50(2):117–29. doi:10.1002/syn.10249.
Benitez SU, Barbizan R, Spejo AB, Ferreira Jr RS, Barraviera B, Goes AM, et al. Synaptic plasticity and sensory-motor improvement following fibrin sealant dorsal root reimplantation and mononuclear cell therapy. Front Neuroanat. 2014;8:96. doi:10.3389/fnana.2014.00096.
Darian-Smith C. Monkey models of recovery of voluntary hand movement after spinal cord and dorsal root injury. ILAR J. 2007;48(4):396–410.
Chew DJ, Leinster VH, Sakthithasan M, Robson LG, Carlstedt T, Shortland PJ. Cell death after dorsal root injury. Neurosci Lett. 2008;433(3):231–4. doi:10.1016/j.neulet.2008.01.012.
Brännstrom T, Kellerth JO. Changes in synaptology of adult cat spinal alpha-motoneurons after axotomy. Exp Brain Res. 1998;118(1):1–13.
Linda H, Shupliakov O, Ornung G, Ottersen OP, Storm-Mathisen J, Risling M, et al. Ultrastructural evidence for a preferential elimination of glutamate-immunoreactive synaptic terminals from spinal motoneurons after intramedullary axotomy. J Comp Neurol. 2000;425(1):10–23.
Kozlova EN. Differentiation and migration of astrocytes in the spinal cord following dorsal root injury in the adult rat. Eur J Neurosci. 2003;17(4):782–90.
Scorisa JM, Zanon RG, Freria CM, de Oliveira AL. Glatiramer acetate positively influences spinal motoneuron survival and synaptic plasticity after ventral root avulsion. Neurosci Lett. 2009;451(1):34–9. doi:10.1016/j.neulet.2008.12.017.
Barbizan R, Oliveira ALR. Impact of acute inflammation on spinal motoneuron synaptic plasticity following ventral root avulsion. J Neuroinflammation. 2010;7:29. doi:10.1186/1742-2094-7-29.
Piehl F, Lundberg C, Khademi M, Bucht A, Dahlman I, Lorentzen JC, et al. Non-MHC gene regulation of nerve root injury induced spinal cord inflammation and neuron death. J Neuroimmunol. 1999;101(1):87–97.
Aldskogius H, Liu L, Svensson M. Glial responses to synaptic damage and plasticity. J Neurosci Res. 1999;58(1):33–41.
Aldskogius H, Kozlova EN. Central neuron-glial and glial-glial interactions following axon injury. Prog Neurobiol. 1998;55(1):1–26.
Höke A. Mechanisms of disease: what factors limit the success of peripheral nerve regeneration in humans? Nat Clin Pract Neurol. 2006;2(8):448–54. doi:10.1038/ncpneuro0262.
Fu R, Tang Y, Ling ZM, Li YQ, Cheng X, Song FH, et al. Lithium enhances survival and regrowth of spinal motoneurons after ventral root avulsion. BMC Neurosci. 2014;15:84. doi:10.1186/1471-2202-15-84.
Carlstedt T. Root repair review: basic science background and clinical outcome. Restor Neurol Neurosci. 2008;26(2–3):225–41.
Silver J, Miller JH. Regeneration beyond the glial scar. Nat Rev Neurosci. 2004;5(2):146–56. doi:10.1038/nrn1326.
Carlstedt T, Linda H, Cullheim S, Risling M. Reinnervation of hind limb muscles after ventral root avulsion and implantation in the lumbar spinal cord of the adult rat. Acta Physiol Scand. 1986;128(4):645–6. doi:10.1111/j.1748-1716.1986.tb08024.x.
Cullheim S, Carlstedt T, Linda H, Risling M, Ulfhake B. Motoneurons reinnervate skeletal muscle after ventral root implantation into the spinal cord of the cat. Neuroscience. 1989;29(3):725–33.
Fournier HD, Mercier P, Menei P. Repair of avulsed ventral nerve roots by direct ventral intraspinal implantation after brachial plexus injury. Hand Clin. 2005;21(1):109–18. doi:10.1016/j.hcl.2004.09.001.
Brunelli G, Brunelli F. Use of anterior nerves of cervical plexus to partially neurotize the avulsed brachial plexus. In: Brunelli G, editor. Textbook of microsurgery. Milan: Masson; 1988. p. 803–7.
Gu YD, Wu MM, Zhen YL, Zhao JA, Zhang GM, Chen DS, et al. Phrenic nerve transfer for brachial plexus motor neurotization. Microsurgery. 1989;10(4):287–9.
Seddon HJ. The use of autogenous grafts for the repair of large gaps in peripheral nerves. Br J Surg. 1947;35(138):151–67.
Gu YD, Zhang GM, Chen DS, Yan JG, Cheng XM, Chen L. Seventh cervical nerve root transfer from the contralateral healthy side for treatment of brachial plexus root avulsion. J Hand Surg Br. 1992;17(5):518–21.
Grahn PJ, Vaishya S, Knight A, Chen BK, Schmeichel A, Currier B, et al. Implantation of cauda equina nerve roots through a biodegradable scaffold at the conus medullaris in rat. Spine J. 2014;14(9):2172–7. doi:10.1016/j.spinee.2014.01.059.
Flores LP, Socolovsky M. Phrenic nerve transfer for reconstruction of elbow extension in severe brachial plexus injuries. J Reconstr Microsurg. 2016;32(7):546–50. doi:10.1055/s-0036-1583302.
Sinha S, Khani M, Mansoori N, Midha R. Adult brachial plexus injuries: surgical strategies and approaches. Neurol India. 2016;64(2):289–96. doi:10.4103/0028-3886.177597.
Steinmetz MP, Horn KP, Tom VJ, Miller JH, Busch SA, Nair D, et al. Chronic enhancement of the intrinsic growth capacity of sensory neurons combined with the degradation of inhibitory proteoglycans allows functional regeneration of sensory axons through the dorsal root entry zone in the mammalian spinal cord. J Neurosci. 2005;25(35):8066–76. doi:10.1523/JNEUROSCI.2111-05.2005.
Peng X, Zhou Z, Hu J, Fink DJ, Mata M. Soluble Nogo receptor down-regulates expression of neuronal Nogo-A to enhance axonal regeneration. J Biol Chem. 2010;285(4):2783–95. doi:10.1074/jbc.M109.046425.
Scott AL, Ramer MS. Schwann cell p75NTR prevents spontaneous sensory reinnervation of the adult spinal cord. Brain. 2010;133(Pt 2):421–32. doi:10.1093/brain/awp316.
Carlstedt T, Aldskogius H, Rosario C. Extension of dorsal horn neurons into the severed and implanted dorsal root. Restor Neurol Neurosci. 1991;3(4):205–9. doi:10.3233/RNN-1991-3405.
Tan CL, Andrews MR, Kwok JC, Heintz TG, Gumy LF, Fässler R, et al. Kindlin-1 enhances axon growth on inhibitory chondroitin sulfate proteoglycans and promotes sensory axon regeneration. J Neurosci. 2012;32(21):7325–35. doi:10.1523/JNEUROSCI.5472-11.2012.
Ramer MS, McMahon SB, Priestley JV. Axon regeneration across the dorsal root entry zone. Prog Brain Res. 2001;132:621–39. doi:10.1016/S0079-6123(01)32107-6.
Ramer MS, Duraisingam I, Priestley JV, McMahon SB. Two-tiered inhibition of axon regeneration at the dorsal root entry zone. J Neurosci. 2001;21(8):2651–60.
Kelamangalath L, Tang X, Bezik K, Sterling N, Son YJ, Smith GM. Neurotrophin selectivity in organizing topographic regeneration of nociceptive afferents. Exp Neurol. 2015;271:262–78. doi:10.1016/j.expneurol.2015.06.007.
Tang XQ, Heron P, Mashburn C, Smith GM. Targeting sensory axon regeneration in adult spinal cord. J Neurosci. 2007;27(22):6068–78. doi:10.1523/JNEUROSCI.1442-07.2007.
Tang XQ, Cai J, Nelson KD, Peng XJ, Smith GM. Functional repair after dorsal root rhizotomy using nerve conduits and neurotrophic molecules. Eur J Neurosci. 2004;20(5):1211–8. doi:10.1111/j.1460-9568.2004.03595.x.
Zhang Y, Dijkhuizen PA, Anderson PN, Lieberman AR, Verhaagen J. NT-3 delivered by an adenoviral vector induces injured dorsal root axons to regenerate into the spinal cord of adult rats. J Neurosci Res. 1998;54(4):554–62. doi:10.1002/(SICI)1097-4547(19981115)54:4<554::AID-JNR12>3.0.CO;2-M.
Fagoe ND, Attwell CL, Kouwenhoven D, Verhaagen J, Mason MR. Overexpression of ATF3 or the combination of ATF3, c-Jun, STAT3 and Smad1 promotes regeneration of the central axon branch of sensory neurons but without synergistic effects. Hum Mol Genet. 2015;24(23):6788–800. doi:10.1093/hmg/ddv383.
Barbizan R, Castro MV, Barraviera B, Ferreira Jr RS, Oliveira ALR. Influence of delivery method on neuroprotection by bone marrow mononuclear cell therapy following ventral root reimplantation with fibrin sealant. PLoS One. 2014;9(8), e105712. doi:10.1371/journal.pone.0105712.
Barbizan R, Castro MV, Rodrigues AC, Barraviera B, Ferreira RS, Oliveira AL. Motor recovery and synaptic preservation after ventral root avulsion and repair with a fibrin sealant derived from snake venom. PLoS One. 2013;8(5), e63260. doi:10.1371/journal.pone.0063260.
Spejo AB, Carvalho JL, Goes AM, Oliveira AL. Neuroprotective effects of mesenchymal stem cells on spinal motoneurons following ventral root axotomy: synapse stability and axonal regeneration. Neuroscience. 2013;250:715–32. doi:10.1016/j.neuroscience.2013.07.043.
Vidigal de Castro M, Barbizan R, Seabra Ferreira Jr R, Barraviera B, Leite Rodrigues de Oliveira A. Direct Spinal ventral root repair following avulsion: effectiveness of a new heterologous fibrin sealant on motoneuron survival and regeneration. Neural Plast. 2016;2016:2932784. doi:10.1155/2016/2932784.
Campbell WW. Evaluation and management of peripheral nerve injury. Clin Neurophysiol. 2008;119(9):1951–65. doi:10.1016/j.clinph.2008.03.018.
IJkema-Paassen J, Jansen K, Gramsbergen A, Meek MF. Transection of peripheral nerves, bridging strategies and effect evaluation. Biomaterials. 2004;25(9):1583–92.
Wu R, Wang L, Chen F, Huang Y, Shi J, Zhu X, et al. Evaluation of artificial nerve conduit and autografts in peripheral nerve repair in the rat model of sciatic nerve injury. Neurol Res. 2016;38(5):461–6. doi:10.1080/01616412.2016.1181346.
Isaacs J. Treatment of acute peripheral nerve injuries: current concepts. J Hand Surg [Am]. 2010;35(3):491–7. doi:10.1016/j.jhsa.2009.12.009. quiz 498.
Félix SP, Pereira Lopes FR, Marques SA, Martinez AM. Comparison between suture and fibrin glue on repair by direct coaptation or tubulization of injured mouse sciatic nerve. Microsurgery. 2013;33(6):468–77. doi:10.1002/micr.22109.
Koulaxouzidis G, Reim G, Witzel C. Fibrin glue repair leads to enhanced axonal elongation during early peripheral nerve regeneration in an in vivo mouse model. Neural Regen Res. 2015;10(7):1166–71.
Martins RS, Siqueira MG, da Silva CF, de Godoy BO, Plese JPP. Electrophysiologic assessment of regeneration in rat sciatic nerve repair using suture, fibrin glue or a combination of both techniques. Arq Neuro-Psiquiatr. 2005;63(3a):601–4.
Rafijah G, Bowen AJ, Dolores C, Vitali R, Mozaffar T, Gupta R. The effects of adjuvant fibrin sealant on the surgical repair of segmental nerve defects in an animal model. J Hand Surg [Am]. 2013;38(5):847–55. doi:10.1016/j.jhsa.2013.01.044.
Pertici V, Laurin J, Marqueste T, Decherchi P. Comparison of a collagen membrane versus a fibrin sealant after a peroneal nerve section and repair: a functional and histological study. Acta Neurochir (Wien). 2014;156(8):1577–90.
Nunes e Silva D, Coelho J, Frazílio FO, Odashiro AN, Carvalho PTC, Pontes ERJC, et al. End-to-side nerve repair using fibrin glue in rats. Acta Cir Bras. 2010;25(2):4.
Chen J, Zhang ZG, Li Y, Wang Y, Wang L, Jiang H, et al. Statins induce angiogenesis, neurogenesis, and synaptogenesis after stroke. Ann Neurol. 2003;53(6):743–51. doi:10.1002/ana.10555.
Paintlia AS, Paintlia MK, Singh I, Skoff RB, Singh AK. Combination therapy of lovastatin and rolipram provides neuroprotection and promotes neurorepair in inflammatory demyelination model of multiple sclerosis. Glia. 2009;57(2):182–93. doi:10.1002/glia.20745.
Déry MA, Rousseau G, Benderdour M, Beaumont E. Atorvastatin prevents early apoptosis after thoracic spinal cord contusion injury and promotes locomotion recovery. Neurosci Lett. 2009;453(1):73–6. doi:10.1016/j.neulet.2009.01.062.
Cloutier FC, Rouleau DM, Hébert-Davies J, Beaumont PH, Beaumont E. Atorvastatin is beneficial for muscle reinnervation after complete sciatic nerve section in rats. J Plast Surg Hand Surg. 2013;47(6):446–50.
Wood MD, Kim H, Bilbily A, Kemp SW, Lafontaine C, Gordon T, et al. GDNF released from microspheres enhances nerve regeneration after delayed repair. Muscle Nerve. 2012;46(1):122–4. doi:10.1002/mus.23295.
Kalbermatten DF, Pettersson J, Kingham PJ, Pierer G, Wiberg M, Terenghi G. New fibrin conduit for peripheral nerve repair. J Reconstr Microsurg. 2009;25(1):27–33. doi:10.1055/s-0028-1090619.
Pettersson J, Kalbermatten D, McGrath A, Novikova LN. Biodegradable fibrin conduit promotes long-term regeneration after peripheral nerve injury in adult rats. J Plast Reconstr Aesthet Surg. 2010;63(11):1893–9. doi:10.1016/j.bjps.2009.11.024.
Kurwale NS, Suri V, Srivastava A, Suri A, Mohanti S, Yadav P, et al. Role of bone marrow derived pluripotent stem cells in peripheral nerve repair in adult rats: a morphometric evaluation. J Neurosci Rural Pract. 2015;6(2):152–9. doi:10.4103/0976-3147.153218.
Navarro X. Functional evaluation of peripheral nerve regeneration and target reinnervation in animal models: a critical overview. Eur J Neurosci. 2016;43(3):271–86. doi:10.1111/ejn.13033.
Biscola NP, Cartarozzi LP, Ferreira Junior RS, Barraviera B, Oliveira ALR. Long-standing motor and sensory recovery following acute fibrin sealant based neonatal sciatic nerve repair. Neural Plast. 2016;2016:9028126. doi:10.1155/2016/9028126.
Cartarozzi LP, Spejo AB, Ferreira Jr RS, Barraviera B, Duek E, Carvalho JL, et al. Mesenchymal stem cells engrafted in a fibrin scaffold stimulate Schwann cell reactivity and axonal regeneration following sciatic nerve tubulization. Brain Res Bull. 2015;112:14–24. doi:10.1016/j.brainresbull.2015.01.005.
Juan FC, Thomazini IA, Gianini MJM, Viterbo F, Toscano E, Moraes RA, et al. Reparation of peripheral nerves with fibrin glue prepared from snake venom. Preliminary results. Sao Paulo Med J. 1995;113(5):1000–2.
Vicente EJD, Rodrigues AC, Gallacci M, Vicente PC, Santos SMR, da Costa DMN. Recuperação funcional do nervo ciático reparado pela cola de fibrina. HU Revista, Juiz de Fora. 2008;34(1):53–6. https://hurevista.ufjf.emnuvens.com.br/hurevista/article/viewFile/86/65.
Buchaim RL, Andreo JC, Barraviera B, Ferreira Junior RS, Buchaim DV, Rosa Junior GM, et al. Effect of low-level laser therapy (LLLT) on peripheral nerve regeneration using fibrin glue derived from snake venom. Injury. 2015;46(4):655–60. doi:10.1016/j.injury.2015.01.031.
de Vries J, Menovsky T, van Gulik S, Wesseling P. Histological effects of fibrin glue on nervous tissue: a safety study in rats. Surg Neurol. 2002;57(6):415–22. discussion 422.
Tse R, Ko JH. Nerve glue for upper extremity reconstruction. Hand Clin. 2012;28(4):529–40. doi:10.1016/j.hcl.2012.08.006.
Becker CM, Gueuning CO, Graff GL. Sutures or fibrin glue for divided rat nerves: Schwann cell and muscle metabolism. Microsurgery. 1985;6(1):1–10.
Povlsen B. A new fibrin seal in primary repair of peripheral nerves. J Hand Surg Br. 1994;19(1):43–7.
Faldini A, Puntoni P, Magherini PC, Lisanti M, Carlucci F, Risaliti R. Comparative neurophysiological assessments of nerve sutures performed by microsurgical methods and with fibrin glue: experimental study. Ital J Orthop Traumatol. 1984;10(4):527–32.
Inalöz SS, Ak HE, Vayla V, Akin M, Aslan A, Sari I, et al. Comparison of microsuturing to the use of tissue adhesives in anastomosing sciatic nerve cuts in rats. Neurosurg Rev. 1997;20(4):250–8.
Acknowledgments
The authors would like to thank Giullio Piettro Gomes da Silva for drawing Fig. 1. Thanks are also due to the Center for the Study of Venoms and Venomous Animals (CEVAP) of UNESP for enabling the publication of this paper (Edital Toxinologia CAPES no. 063/2010, Process no. 230.38.006285/2011-21, AUXPE Toxinologia 1219/2011).
Funding
The authors are thankful to São Paulo Research Foundation (FAPESP) for providing financial support (2009/53846-9, 2010/00729-2, 2011/23377-7, 2011/02889-0, 2012/22750-9, 2012/02689-3, 2012/08101-8, 2012/13514-0, 2012/20456-6, 2013/23030-2, 2013/04409-0, 2014/06892-3, 2014/11405-4) and to the National Council for Scientific and Technological Development (CNPq) (Proc. No. 300553/2013-9, 563582/2010-3). This work was also supported by the Coordination for the Improvement of Higher Education Personnel (CAPES) through Edital Toxinologia CAPES no. 063/2010, Process no. 230.38.006285/2011-21, AUXPE Toxinologia 1219/2011. RSF Jr. is a CNPq DTI fellow researcher (310395/2014-3).
Authors’ contributions
NPB, LPC, SUB, RBP, MVC and ABS, search the databases (PubMed, Scopus, Scielo and Web of Science) and wrote the review. SUB and ALRO prepared Fig. 1. RSFJr, BB and ALRO corrected the manuscript. All authors read and approved the final manuscript.
Competing interests
One of the authors of this article, Dr. Benedito Barraviera, is the Editor-in-Chief of Journal of Venomous Animals and Toxins including Tropical Diseases. He did not get involved in the peer review process of this manuscript.
Consent for publication
Not applicable.
Ethics approval and consent to participate
Not applicable.
Author information
Authors and Affiliations
Corresponding author
Additional files
Video showing loss of weight-bearing capacity following ventral root avulsion (VRA), 12 weeks post-surgery, in the the CatWalk System. (AVI 10692 kb)
Video showing restoration of weight-bearing capacity following ventral root avulsion (VRA) and reimplantation with the heterologous fibrin sealant (HFS), 12 weeks post-surgery, CatWalk System. (AVI 12966 kb)
Video showing restoration of weight-bearing capacity following ventral root avulsion (VRA) and reimplantation with commercial fibrin sealant (FS), 12 weeks post-surgery, CatWalk System. (AVI 15923 kb)
Video showing normal gait pattern evaluation in a control animal. (AVI 17628 kb)
Video showing gait pattern evaluation after neonatal (P2) sciatic nerve axotomy followed by coaptation: sciatic nerve repair with the heterologous (HFS) sealant. (AVI 14347 kb)
Video showing gait pattern evaluation after neonatal (P2) sciatic nerve axotomy followed by coaptation: recovery following nerve repair using commercial fibrin sealant (FS), 12 weeks post-surgery. (AVI 10675 kb)
Rights and permissions
Open Access This article is distributed under the terms of the Creative Commons Attribution 4.0 International License (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted use, distribution, and reproduction in any medium, provided you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made. The Creative Commons Public Domain Dedication waiver (http://creativecommons.org/publicdomain/zero/1.0/) applies to the data made available in this article, unless otherwise stated.
About this article
Cite this article
Biscola, N.P., Cartarozzi, L.P., Ulian-Benitez, S. et al. Multiple uses of fibrin sealant for nervous system treatment following injury and disease. J Venom Anim Toxins Incl Trop Dis 23, 13 (2017). https://doi.org/10.1186/s40409-017-0103-1
Received:
Accepted:
Published:
DOI: https://doi.org/10.1186/s40409-017-0103-1