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Introduction

Testicular torsion or torsion of the spermatic cord is one of the most serious urological emergencies encountered and is generally identified in newborn and adolescent males (1). It causes testicular injury, which potentially leads to the development of male subfertility when misdiagnosed and inappropriately treated (2). The turning of the spermatic cord and spermatic structures around themselves results in biochemical and histological changes and ultimately, the development of testicular dysfunction (3). Due to testicular torsion, blood flow to the testicular tissues is interrupted and this interruption leads to ischemia during which energy rich phosphates (ATP) are depleted and levels of their degradation products, such as hypoxanthine, rise (4,5).

Following testicular detorsion, tissues undergo reperfusion, causing more severe damage than that induced by ischemia (6). Ischemia-reperfusion (I/R) injury occurs when blood circulation is restored following an episode of acute ischemia (7,8). In this type of injury, the blood supply to the tissue is initially interrupted, damaging metabolically active tissues. However, the restoration of blood flow to the tissues initiates a paradoxic cascade of events, including free oxygen radical production, intracellular calcium overload and lipid peroxidation, leading to further cellular and tissue damage (8). Following the onset of ischemia, adenosine triphosphate is degraded to hypoxanthine and xanthine dehydrogenase is converted to xanthine oxidase (9). Testicular ischemia/reperfusion (tIR) activates a complex cascade of cellular and molecular reactions that are not yet fully understood. However, a number of studies suggest that restoration of blood supply to ischemic testes is associated with the excessive production of reactive oxygen species (ROS) and the generation of testicular oxidative stress (10) that activates mitogen activated protein kinases (11–13). tIR leads to lipid peroxidation, protein denaturation, DNA damage and activation of the apoptotic machinery (11). Furthermore, it has been determined that in tIR, activated neutrophils adhere to microvascular endothelium and subsequently emigrate and secrete the enzyme myeloperoxidase, which catalyses the formation of ROS. Testes are sensitive to free radical damage. Under normal conditions, enzymatic antioxidant defence systems, including glutathione peroxidase (GPx), superoxide dismutase (SOD) and catalase (CAT), protect those cells from free radical damage (14). During tIR, alterations in cellular and mitochondrial Ca2+ (mCa2+) depositions are critically important (15,16). Levels of mCa2+ increase via mCa2+ uniporter channels that increase intracellular Ca2+. Excessive mCa2+ loads initiate irreversible events that result in cell apoptosis through permeability transitions and pore formation (17).

It has been demonstrated in animal models that a number of substances have some benefit at reducing testicular reperfusion injury (18). The current study used papers from the National Center For Biotechnology Information database (https://www.ncbi.nlm.nih.gov/pubmed/) from 2005, using the search terms ‘testicular ischemia reperfusion injury’ and ‘ischemia reperfusion injury testis’. Papers that did not focus on the medical treatment of tIR were excluded.

Agonists of erythropoietin receptors (EPO-R)

EPO-R and darbepoetin alfa

EPO-R have been detected in different types of tissue including brain, spinal cord, heart and testes, and exhibit neuroprotective, anti-apoptotic, antioxidant, anti-inflammatory and angiogenic activity (19). EPO and the long acting EPO analogue darbepoetin alfa may have a protective effect on testicular I/R injury (20,21).

Anaesthetics

Dexmedetomidine (Dex)

Dex is a selective and potent α2-adrenoceptor agonist, approved for use by the US Food and Drug Administration in 1999 to sedate patients hospitalized in intensive care settings. In addition to sedative and analgesic effects, it has been demonstrated that Dex has organ-protective effects in a number of inflammatory models, including tIR injury (22). It has been suggested that sympatholysis may be a property of Dex, due to its mechanism of action via presynaptic α-adrenoceptors. Through this mechanism, Dex may reduce the noradrenaline release induced by ischemia, thus reducing overall oxidant status (23).

Morphine

Morphine administration decreases I/R injury in the rat heart and protects the rabbit kidney against oxidative stresses resulting from I/R (24,25). It has been determined that morphine increases levels of ipsilateral intratesticular antioxidant markers during the reperfusion phase that follows unilateral testicular torsion, and this is reflected in lower testicular malondialdehyde (MDA) levels (26). This effect seems to be mediated through opioid receptors. The observed effect of morphine may be due to its impact on neutrophils and its direct scavenging action against peroxynitrite (26).

Propofol

Propofol seems to have antioxidant effects that inhibit lipid peroxidation by forming relatively unreactive free radicals capable of breaking the production chain of radicals that are potentially damaging to cell membranes in tIR injury (27).

Antioxidants

α-Lipoic Acid

α-Lipoic Acid decreases the cellular damage and apoptosis occurring during testicular I/R injury in rats (28). Additionally, it has been reported that α-lipoic acid administration has significant protective effects against oxidative stress by decreasing GPx and SOD activity. Furthermore, α-lipoic acid reduces MDA levels, which is considered to be an important indicator of lipid peroxidation (28).

Dimethylsulfoxide (DMSO)

DMSO exerts a protective effect against testes lipid peroxidation injury caused by I/R in rats. The increase in GSH levels during reperfusion in DMSO-treated rats favours the hypothesis that the use of this substance in the pretorsion period may attenuate the damaging effects of tIR injury (29).

Ebselen

Ebselen is a type of synthetic antioxidant that has a wide spectrum of therapeutic actions. It exhibits anti-atherosclerotic and renoprotective effects; therefore, clinical trials are currently investigating its efficacy against stroke and reperfusion injury (30). It is considered an antioxidant and ROS scavenger and reduces the oxidative biochemical and histopathological damage that occur following tIR (31).

Edaravone

Edaravone, a free-radical scavenger, is used for the clinical treatment of cerebral ischemia in Japan. It has been reported that edaravone reduces levels of 8-hydroxydeoxyguanosine, a marker of oxidative DNA damage (3). Moreover, edaravone seems to protect germ cells (3).

Mannitol

Mannitol is an intravascular volume expander with free radical scavenging properties, as well as being an osmotic diuretic and it is has been reported that it reduces ischemic renal damage (32). Mannitol infusion also has a protective effect against experimental tIR injury (33).

Melatonin

Melatonin is a potent antioxidant and a free radical scavenger that promotes the formation of antioxidant enzymes and inhibits lipid membrane peroxidation (34–37). It has been demonstrated that melatonin, with or without ozone, decreases levels of MDA, thus limiting the tissue injury that occurs following tIR (36,37).

Selenium

Selenium is a well-known antioxidant that increases glutathione peroxidase activity (38,39). It acts by reducing the oxidative stress and apoptosis that result from testicular tIR injury and therefore protects against testicular damage (40).

Statins

Statins are recognized as atypical anti-inflammatory agents that possess various immunomodulatory effects in addition to their conventional lipid-lowering properties (41). The precise mechanism by which statins exert this anti-inflammatory effect is currently unclear. Some studies have demonstrated that statins serve a protective role in tIR injury by inducing heme-oxygen-1 in endothelial and macrophage cells, leading to a reduction in caspase-3 activity and germ cell apoptosis (41,42).

Polydeoxyribonucleotide (PDRN)

Administration of PDRN, an active fraction of a preparation extracted from sperm trout, is used in therapy to stimulate tissue repair (43). It acts as an agonist on adenosine A2A receptors, stimulating VEGF production during pathological conditions of low tissue perfusion, including limb ischemia, varicocele, diabetes mellitus and thermal injury (43–46). It has been demonstrated that PDRN has potent anti-apoptotic activity, decreasing histological damage and ameliorating spermatogenic activity (47).

Vitamin E and Raxofelast

Vitamin E and its analogue raxofelast have potent antioxidant activity (11). Their administration results in a significant decrease in extracellular signal-regulated kinases 1/2 and c-Jun N-terminal kinase activation, reducing lipid peroxidation and protecting the testes from tIR (11).

Calcium channel blockers

Verapamil, Lidocaine, Nifedipine, Amlodipine

During I/R, damage occurs due to accumulation of intercellular Ca2+ and free radicals (48). The Ca2+/Na+ channel blockers verapamil, lidocaine and nifedipine ameliorate the effect of I/R (49–52). Recently, it was demonstrated that amlodipine decreases free radical levels and increases the levels antioxidants including SOD and GSH (14).

Interaction with neutrophils

Antagonist of E-selectin

E-selectin acts by tethering neutrophils and facilitating their slow rolling along endothelial cells (53,54). Neutrophil recruitment to affected organs is one of the hallmarks of I/R injury and E-selectin serves a critical role in neutrophil recruitment to the testes following I/R and the resulting germ cell-specific apoptosis (55). Blocking E-selectin with function-blocking monoclonal E-selectin antibody, even after the onset of reperfusion inhibits neutrophil recruitment to the I/R-induced murine testes. Blockade of E-selectin may therefore be a potential strategy to protect post-ischaemic testes and prevent infertility (54).

Sivelestat sodium aminoacetate tetrahydrate and taurine

Sivelestat sodium aminoacetate tetrahydrate is a synthetic, specific, low-molecular weight neutrophil elastase inhibitor (56). It has been demonstrated that sivelestat and taurine inhibit neutrophil elastase, which seems to serve a substantial role in tIR injury by releasing toxic mediators such as oxygen-free radicals, that initiate a chain reaction leading to damage of the cell membrane (57). In this way, these molecules may offer efficient protection against testicular reperfusion injury (56–58).

Interaction with renin-angiotensin system (RAS)

Bosenta, Losartan, Enalapril, Zofenopril

In the testes, it has been reported that a local RAS is responsible for maintaining blood pressure and volume (59). During tIR injury, inhibition of the classical RAS pathway leads to reductions in testicular injury, inflammation and oxidative stress (10,60). Recently, the testicular angiotenis converting enzyme (tACE)/Ang-(1–7)/Mas receptor axis has been described and it has been suggested that Ang-(1–7)-mediated protection may increase nitric oxide (NO) bioavailability, inhibit ROS generation and suppress apoptosis in tIR (10). Furthermore, it has been documented that bosentan, a dual endothelin receptor antagonist, has more beneficial effects than losartan, an angiotensin II type I antagonist and the ACE inhibitors enalapril and zofenopril in tIR injury (60).

Modulators of inflammation

Interleukin (IL)-10

IL-10 is a type of T Helper 2 type cytokine that modulates inflammatory responses by inhibiting the production of pro-inflammatory cytokines, including tumour necrosis factor (TNF)-α, IL-1, IL-6, and IL-8 (61). Furthermore, IL-10 upregulates monocyte production of soluble TNF-α and IL-1 receptor antagonist (62). IL-10 appears to attenuate the damage in testes caused by tRI, due to its anti-inflammatory and antioxidant properties (62). It has been suggested that IL-10 may act by inhibiting the effects of ROS, thus reducing the levels of lipid peroxidation and myeloperoxidase and increasing GPx levels (62).

Melanocortins (MC)

MCs are bioactive peptides derived from the cleavage of proopiomelanocortin and activate the motor arm of the vagal reflex by stimulating brain MC3 and MC4 receptors. In this way, they blunt the inflammatory cascade and the apoptotic reaction and exert strong protection against ischemia in a number of experimental models (63). The selective MC4 receptor antagonist HS024 activates the cholinergic anti-inflammatory pathway that projects towards the testes, and thus is responsible for the beneficial effects of MCs against tIR injury (63).

Metformin

Metformin, typically used to manage type II diabetes, may serve a role in alleviating inflammatory responses, which is beneficial in protecting the testes from tIR injury (64).

Pyrrolidine dithiocarbamate (PDTC)

PDTC is a specific inhibitor of nuclear factor (NF) κB, a protein complex associated with immune responses, inflammatory processes, cellular proliferation and apoptosis (65). Activation of NFκB by IL-1, TNF-α and lipopolysaccharides is blocked by administration of PDTC. Results from an experimental study demonstrated that PDTC has beneficial effects against tIR injury by lowering MDA levels and increasing SOD activity, as well as reducing the number of apoptotic cells (66).

Montelukast

Montelukast is an antioxidant that is also a selective antagonist of cysteinyl leukotriene receptor 1 and is used as an anti-asthmatic drug in clinical settings (67). It protects testes against I/R by inhibiting neutrophil activity, decreasing inducible nitric oxide synthase (iNOS) levels and attenuating apoptosis (68).

Physical therapies

Hyperbaric oxygen (HBO)

HBO therapy, through plasma oxygen transport, is currently used as an alternative treatment for ischemic tissues including brain, heart, liver, kidney, lung, skeletal muscle, and intestinal tissue (69,70). HBO therapy attenuates tIR-induced injury by blocking oxidative stress, suppressing inflammation, and reducing NO formation (69). Furthermore, HBO therapy reduces dimethylarginine dimethylaminohydrolase activity and asymmetric dimethylarginine content, which may contribute to a reduction of NO formation in tIR (69).

Hypothermia

Hypothermia treatment, which involves placing the testicle in ice slush during ischemia and maintaining a surface temperature of 2–4°C, reduces histological damage in a rat model of tIR (71).

Ischemic post-conditioning

Ischemic post-conditioning is an innovative surgical technique against reperfusion injury, defined as rapid intermittent interruptions of blood flow at the early phase of reperfusion. Ischemic post-conditioning mechanically alters hydrodynamics of reperfusion and has been demonstrated to have an early beneficial effect in tIR (72). However, its role against late damage in tIR remains controversial (73).

Phytotherapeutics

Apocynin

Apocynin (4-hydroxy-3methoxy-acetophenone) is a naturally occurring methoxysubstituted catechol, extracted from the roots of Apocynumcannabinum (Canadian hemp) and Picrorhiza kurroa (Scrophulariaceae), and is a known inhibitor of NADPH-oxidase (74), which is considered to be an important source of ROS and reactive nitrogen species (RNS). In this way, apocynin depresses the generation of toxic reactive metabolites, restoring levels of antioxidant GSH and inhibiting oxidative stress-associated tissue neutrophil accumulation induced by tIR (75).

Caffeic acid phenethyl ester (CAPE)

The administration of CAPE inhibits increases in iNOS and myeloperoxidase, and it has been suggested that CAPE may inhibit neutrophil mediated cellular injury (76).

3′,4′-dihydroxyflavonol

3′,4′-dihydroxyflavonol may exert a protective effect against lipid peroxidation in experimental I/R injury by both inhibiting oxidants and strengthening the action of antioxidants (77).

Epigallocatechin-3-gallate (EGCG)

EGCG, one of the primary components of polyphenols in green tea, has been widely investigated as it suppresses the inflammatory processes that lead to transformation, inhibits cell proliferation and exerts strong antiradical activity (78–80). EGCG is used as a nutritional supplement due to its many health benefits and it has been demonstrated to protect against I/R-induced apoptosis in vitro and in vivo (80). An adjunct interventional use of EGCG prior to testicular detorsion surgery may prevent the destructive effects of tIR injury (78).

Genistein

Genistein is an isoflavone extracted from soy that has been demonstrated to protect the testes via attenuation of oxidative stress and inhibition of the caspase-8 apoptosis pathway (81).

Ginkgo biloba

Extract of Ginkgo biloba leaves has antioxidant properties as a free-radical scavenger (82). It contains flavone glycosides (primarily quercetin, kaempferol and isorhamnetin), terpene lactones (2.8–3.4% ginkgolides A, B and C, and 2.6–3.2% bilobalide), ginkgolide B, bilobalide, proanthocyanadins, glucose, rhamnose, organic acids, D-glucaric acid and ginkgolic acid (82). Ginkgo biloba leaves promote vasodilation and improve blood flow through arteries, veins and capillaries. They inhibit platelet aggregation and prolong bleeding time. Therefore, administration of the Ginkgo biloba leaves extract offers potential protection against tIR injury (82).

Goji berry

Goji berry is a herb from the Solanaceae family that also has reported antioxidant effects. Experimental studies have demonstrated that goji berry reduces blood sugar and lipid levels, and exhibits anti-ageing, immuno-modulating, antitumour, anti-fatigue and male fertility-enhancing effects (83). Goji berry extracts seem to reduce tIR injury via their antioxidant effects in testes torsion (83).

Lycopene

Lycopene is a red carotenoid found in large amounts in tomatoes. A number of studies support that lycopene, rather than β-carotene, is a precursor of vitamin A (84,85). It has been proposed as a useful molecule for different types of cancer, coronary artery disease, bone health, male fertility, hypertension and neurodegenerative diseases (39,85). Lycopene is an effective antioxidant and may protect against the negative effects of tIR when used in the early phase of testicular torsion (85).

Psoralea corylifolia

Psoralea corylifolia is a widely used traditional Chinese medicine, extracted from mature and dry fruits of Leguminous plant Psoralea corylifolia. It has been officially listed in the Pharmacopoeia of the People's Republic of China (86,87) and is used to treat male reproductive dysfunctions, such as premature ejaculation, impotence and spermatorrhea. The constituents of Psoralea corylifolia include coumarins, flavonoids and meroterpenes, such as psoralen, isopsoralen, bavachinin, bavachin, psoralidin, neobavaisoflavone and bavachalcone (86). Psoralea corylifolia may exert a protective effect against tIR injury, as it exhibits scavenging activity against ROS (87).

Quercetin

Quercetin is a major flavonol in the diet and its primary dietary sources are tea, onions, apples and red wine (88). Quercetin has been found to possess antilipoperoxidant, antiplatelet and anti-inflammatory activities and inhibits the enzymic activities of lipooxygenase, xanthine oxidase and cyclooxygenase (88). Quercetin is considered to be the most potent scavenger of ROS, such as superoxide and RNS, such as NO, and seems to alleviate ischemia and reperfusion injury in rat testes (88).

Resveratrol (RSV)

RSV (trans-3,5,4′-tri-hydroxystilbene) is a natural phytoalexin with antioxidant properties. RSV is found in many plants, including berries, grapes and peanuts, and it protects the cell by preventing lipid peroxidation in the cell membrane and preventing DNA damage caused by excessive ROS production (89). It has been reported that RSV treatment has a positive effect in balancing the oxidant/antioxidant equilibrium, thus reducing the apoptotic rate in an experimental tIR model (89).

Rutin

Rutin is a flavone glycoside that is abundant in a wide variety of plants. It possesses several physiological properties, including antioxidant, anti-inflammatory and anticancer activities (90,91). Rutin ameliorates tIR by scavenging ROS and increasing the activity of SOD and CAT (92).

Ternatin (TTN)

TTN, a tetramoxyflavone extracted from Egletes viscosa L., has protective effects against the testes tissue lipid peroxidation injury and oxidative stress that results in tIR (93).

Thymoquinone (TQ)

TQ is the primary bioactive constituent of Nigella sativa seed oil. TQ has diverse pharmacological properties, including antidiabetic, analgesic and anti-inflammatory properties, and is considered to be a very strong antioxidant (94–96). In Turkey, India, Arabia and many Middle Eastern countries, there is a belief that ‘regular use of Black Seed can cure anything, except death’. It is thus suggested that TQ may have protective effects in tIR injury (97,98).

Platelet inhibitors

Dipyridamole and acetylsalicylic acid (ASA)

Dipyridamole and ASA possess antioxidant properties. Dipyridamole is an adenosine transporter inhibitor that inhibits cellular adenosine reuptake and increases interstitial adenosine concentration by inhibiting the activity of caspase, thus inhibiting apoptosis. (99,100). Dipyridamole blocks the activity of caspases, which serve a major role during apoptotic cell death. ASA suppresses platelet aggregation by inhibiting thromboxane A2 production and subsequently blocking the arachidonate cascade. It has also been demonstrated that ASA exhibits free radical-scavenging properties, thus protecting endothelial cells against the negative effects of hydrogen peroxide (101).

In a study comparing the potential protective effects of dipyridamole and ASA in a rat model of tIR, it was observed that a significant decrease in apoptotic index in tIR injury in the dipyridamole group (99).

Sex steroid precursors

Dehydroepiandrosterone

It remains unclear whether dehydroepiandrosterone exerts its effects directly or does so following its conversion to androgens or estrogens. Inserting DHEA into the lipid membranes may make them more resistant to oxidative stress, thus protecting the testes against tIR injury (9).

Vasodilator agents

Carvedilol (CVD)

CVD [1-[carbazolyl-(4)-oxy]-3-[(2- methoxyphenoxyethl) amino]-2-propanol] is a third-generation vasodilator agent used in the treatment of hypertension, ischemic heart disease and congestive heart failure (102–104). It selectively blocks α1-receptors and non-selectively blocks β1 and β2-adrenoceptors (102). CVD and some of its metabolites also exhibit antioxidant activity. Following CVD administration in an experimental model of tIR injury, levels of malondialdehyde decrease to a level similar to a sham group (105).

Sildenafil and udenafil

Sildenafil increases the activity of antioxidant enzymes and decreases MDA levels following tIR injury in rats (106). Sildenafil may inhibit the production of lipid peroxidation by inhibiting the activity and expression of nicotinamide adenine dinucleotide phosphate (NADPH) oxidase (106). Udenafil citrate also acts in a similar fashion to protect the testes from tIR injury (107).

Trapidil

Trapidil (5-methyl-7-diethylamino-s-triazolopyrimidine), originally used as an anti-anginal drug, is a phosphodiesterase and platelet derived growth factor inhibitor (108). It decreases free oxygen radical formation in tIR and attenuates histopathological damage in ipsilateral twisted testes (109).

Other mechanisms

Rosiglitazone

Rosiglitazone is the most potent and selective peroxisome proliferator-activated receptor-gamma (PPAR-g) ligand. PPAR-g is a member of the nuclear hormone receptor superfamily involved in a number of physiological processes, including atherosclerosis, inflammation, cancer, infertility and demyelination (110). It has been demonstrated that rosiglitazone prevents cell injury by increasing endothelial NOS expression in the contralateral testicular tissue in a model of tIR (110).

Conclusions

By reviewing the current literature, it seems that a number of medications, experimentally and sometimes clinically, serve an adjuvant role in cellular damage following ischemia-reperfusion. Testicular torsion in animals represents a practical model of ischemia-reperfusion in humans.

A number of experimental studies have been published regarding the use of different types medication and their role in decreasing cellular damage following reperfusion. Since the primary causes of testicular damage are represented by ROS production, an increase in the levels of intra-mitochondrial calcium and an increased rate of cellular apoptosis, different types of medication have been proposed as potentially useful.

Antioxidants, calcium channel blockers, phytotherapeutics, anaesthetics, hormones and platelet inhibitors may potentially create a solid bases for an adjuvant restoring therapy and ameliorate testicular function following torsion. However, currently, the immediate restoration of blood flow is the primary therapeutic approach to treat torsion of the spermatic cord. In order to avoid or reduce the rate of reperfusion injury, future multicentric randomized controlled trials are warranted. These may provide further insight into the actions of the aforementioned molecules and their precise roles.

Reference