Stable Gastric Pentadecapeptide BPC 157 as Useful Cytoprotective Peptide Therapy in the Heart Disturbances, Myocardial Infarction, Heart Failure, Pulmonary Hypertension, Arrhythmias, and Thrombosis Presentation

In heart disturbances, stable gastric pentadecapeptide BPC 157 especial therapy effects combine the therapy of myocardial infarction, heart failure, pulmonary hypertension arrhythmias, and thrombosis prevention and reversal. The shared therapy effect occurred as part of its even larger cytoprotection (cardioprotection) therapy effect (direct epithelial cell protection; direct endothelium cell protection) that BPC 157 exerts as a novel cytoprotection mediator, which is native and stable in human gastric juice, as well as easily applicable. Accordingly, there is interaction with many molecular pathways, combining maintained endothelium function and maintained thrombocytes function, which counteracted thrombocytopenia in rats that underwent major vessel occlusion and deep vein thrombosis and counteracted thrombosis in all vascular studies; the coagulation pathways were not affected. These appeared as having modulatory effects on NO-system (NO-release, NOS-inhibition, NO-over-stimulation all affected), controlling vasomotor tone and the activation of the Src-Caveolin-1-eNOS pathway and modulatory effects on the prostaglandins system (BPC 157 counteracted NSAIDs toxicity, counteracted bleeding, thrombocytopenia, and in particular, leaky gut syndrome). As an essential novelty noted in the vascular studies, there was the activation of the collateral pathways. This might be the upgrading of the minor vessel to take over the function of the disabled major vessel, competing with and counteracting the Virchow triad circumstances devastatingly present, making possible the recruitment of collateral blood vessels, compensating vessel occlusion and reestablishing the blood flow or bypassing the occluded or ruptured vessel. As a part of the counteraction of the severe vessel and multiorgan failure syndrome, counteracted were the brain, lung, liver, kidney, gastrointestinal lesions, and in particular, the counteraction of the heart arrhythmias and infarction.

We suggested these particular effects and this background as a network of the evidence for the physiologic significance of the revealed BPC 157/vascular-system interplay  (i.e., in situ hybridization and immunostaining studies in humans evidenced BPC 157 large distribution in tissues [102] and suggested its additional physiologic regulatory roles [8,102]).
In this agenda, we will further review heart disturbances and specifically indicate the particular effects of BPC 157 therapy.

Noxious Procedure BPC 157 Therapy Effects
Initial heart infarct induction and re-infarction, isoprenaline one or two application Escalated general peripheral and central syndrome [38] Reduced levels of all necrosis markers, CK, CK-MB, LDH, and cTnT, and attenuated gross (no visible infarcted area) and histological damage, ECG (no ST-T ischemic changes), and echocardiography (preservation of systolic left ventricular function) damage induced by isoprenaline. Decrease in oxidative stress parameters and likely maintained NO-system function evidenced that BPC 157 interacted with eNOS and COX2 gene expression in a particular way and counteracted the noxious effect of the NOS-blocker, L-NAME. Early vessel and multiorgan failure (brain, heart, lung, liver, kidney, and gastrointestinal lesions), thrombosis, intracranial (superior sagittal sinus) hypertension, portal and caval hypertension, and aortal hypotension, ECG disturbances), in its full presentation was attenuated/eliminated by BPC 157 therapy (given at 5 min after isoprenaline) via activation of the azygos vein).
Intragastric administration of 96% alcohol Escalated general peripheral and central syndrome acute subendocardial infarct [40] Intragastric administration of absolute alcohol-induced gastric lesions, intracranial (superior sagittal sinus) hypertension, severe brain swelling and lesions (i.e., intracerebral hemorrhage with degenerative changes of cerebral and cerebellar neurons), portal and vena caval hypertension, aortal hypotension, severe thrombosis, inferior vena cava and superior mesenteric vein congestion, azygos vein failure (as a failed collateral pathway), electrocardiogram disturbances, and heart (acute subendocardial infarct), lung (parenchymal hemorrhage), liver (congestion), and kidney (congestion) lesions. BPC 157 therapy (10 µg/kg or 10 ng/kg given intraperitoneally 1 min after alcohol) counteracted these deficits rapidly. Specifically, BPC 157 reversed brain swelling and superior mesenteric vein and inferior vena caval congestion and helped the azygos vein to recover, which improved the collateral blood flow pathway.
Lithium sulfate regimen in rats (500 mg/kg/day, ip, for three days, with assessment at 210 min after each administration of lithium) Escalated general peripheral and central syndrome Severe myocardial congestion, along with subendocardial infarcts [39] BPC 157 counteracted the lithium-induced occlusive-like syndrome; rapidly counteracted brain swelling and intracranial (superior sagittal sinus) hypertension, portal hypertension, and aortal hypotension, which otherwise would persist; counteracted vessel failure; abrogated congestion of the inferior caval and superior mesenteric veins; reversed azygos vein failure; and mitigated thrombosis (superior mesenteric vein and artery), congestion of the stomach, and major hemorrhagic lesions. Both regimens of BPC 157 administration also counteracted the muscular weakness and prostration (as shown in microscopic and ECG recordings), myocardial congestion and infarction, in addition to edema and lesions in various brain areas; counteracted marked dilatation and central venous congestion in the liver; large areas of congestion and hemorrhage in the lung; and degeneration of proximal and distal tubules with cytoplasmic vacuolization in the kidney, attenuating oxidative stress.
Abdominal compartment syndrome (intra-abdominal pressure in thiopental-anesthetized rats at 25 mmHg (60 min), 30 mmHg (30 min), 40 mmHg (30 min), and 50 mmHg (15 min), and, in esketamine-anesthetized rats (25 mmHg for 120 min)) as a model of multiple occlusion syndrome Escalated general peripheral and central syndrome Severe myocardial congestion, along with subendocardial infarcts [31] BPC 157 administration recovered the azygos vein via the inferiorsuperior caval vein rescue pathway. Additionally, intracranial (superior sagittal sinus), portal, and caval hypertension and aortal hypotension were reduced, as were the grossly congested stomach and major hemorrhagic lesions, brain swelling, venous and arterial thrombosis, congested inferior caval and superior mesenteric veins, and collapsed azygos vein; thus, the failed collateral pathway was fully recovered. Severe ECG disturbances (i.e., severe bradycardia and ST-elevation until asystole) were also reversed. Microscopically, transmural hyperemia of the gastrointestinal tract, intestinal mucosa villi reduction, crypt reduction with focal denudation of superficial epithelia, and large bowel dilatation were all inhibited. In the liver, BPC 157 reduced congestion and severe sinusoid enlargement. In the lung, a normal presentation was observed, with no alveolar membrane focal thickening and no lung congestion or edema, and severe intra-alveolar hemorrhage was absent. Moreover, severe heart congestion, subendocardial infarction, renal hemorrhage, brain edema, hemorrhage, and neural damage were prevented.

Noxious Procedure BPC 157 Therapy Effects
Bile duct ligation acute pancreatitis as local disturbances (i.e., improved gross and microscopy presentation, decreased amylase level) Escalated general peripheral and central syndrome Severe myocardial congestion, along with subendocardial infarcts [37] Bile duct-ligated rats commonly presented intracranial (superior sagittal sinus), portal and caval hypertension and aortal hypotension, gross brain swelling, hemorrhage and lesions, heart dysfunction, lung lesions, liver and kidney failure, gastrointestinal lesions, and severe arterial and venous thrombosis, peripherally and centrally. Unless antagonized with the key effect of BPC 157 regimens, reversal of the inferior caval and superior mesenteric vein congestion and reversal of the failed azygos vein activated azygos vein-recruited direct delivery to rescue the inferior-superior caval vein pathway; these were all antecedent to acute pancreatitis major lesions (i.e., acinar, fat necrosis, hemorrhage). These lesions appeared in the later period but were markedly attenuated/eliminated (i.e., hemorrhage) in BPC 157-treated rats. To summarize, while the innate vicious cycle may be peripheral (bile duct ligation), or central (rapidly developed brain disturbances), or peripheral and central, BPC 157 resolved acute pancreatitis and its adjacent syndrome.
Superior mesenteric artery permanent occlusion Escalated general peripheral and central syndrome Severe myocardial congestion [19] BPC 157 rapidly recruits collateral vessels (inferior anterior pancreaticoduodenal artery and inferior mesenteric artery) that circumvent occlusion and ascertains blood flow distant from the occlusion in the superior mesenteric artery. Portal and caval hypertension, aortal hypotension, and, centrally, superior sagittal sinus hypertension were attenuated or eliminated, and ECG disturbances were markedly mitigated. BPC 157 therapy almost annihilated venous and arterial thrombosis. Multiple organ lesions and disturbances (i.e., heart, lung, liver, and gastrointestinal tract, in particular, as well as brain) were largely attenuated.

Noxious Procedure BPC 157 Therapy Effects
Complex syndrome of the occluded superior sagittal sinus, brain swelling and lesions, and multiple peripheral organs lesions in rat Escalated general peripheral and central syndrome Severe myocardial congestion [27] The increased pressure in the superior sagittal sinus, portal and caval hypertension, aortal hypotension, arterial and venous thrombosis, severe brain swelling and lesions (cortex (cerebral, cerebellar), hypothalamus/thalamus, hippocampus), particular veins (azygos, superior mesenteric, inferior caval) dysfunction, heart dysfunction, lung congestion as acute respiratory distress syndrome, kidney disturbances, liver failure, and hemorrhagic lesions in gastrointestinal tract were all assessed. Rats received BPC 157 medication (10 µg/kg, 10 ng/kg) intraperitoneally, intragastrically, or topically to the swollen brain at 1 min ligation time or at 15 min, 24 h, and 48 h ligation time. BPC 157 therapy rapidly attenuates the brain swelling, rapidly eliminates the increased pressure in the ligated superior sagittal sinus and the severe portal and caval hypertension and aortal hypotension, and rapidly recruits collateral vessels, centrally ((para)sagittal venous collateral circulation) and peripherally (left superior caval vein azygos vein-inferior caval vein). BPC 157 therapy rapidly overwhelms the permanent occlusion of the superior sagittal sinus in rats and counteracts the brain, heart, lung, liver, kidney, and gastrointestinal lesions, and annihilates thrombosis, given at 1 min, 15 min, 24 h, or 48 h ligation-time.
Monocrotaline-induced pulmonary arterial hypertension in rats (wall thickness, total vessel area, heart frequency, QRS axis deviation, QT interval prolongation, increase in right ventricle systolic pressure, and body weight loss) [41] After monocrotaline (80 mg/kg subcutaneously), BPC 157 (10 µg/kg or 10 ng/kg, days 1-14 or days 1-30 (early regimens), or days 14-30 (delayed regimen)) was given once daily intraperitoneally (last application 24 h before sacrifice) or continuously in drinking water until sacrifice (day 14 or 30). Without therapy, the outcome was the full monocrotaline syndrome, marked by right-side heart hypertrophy and massive thickening of the precapillary artery's smooth muscle layer, clinical deterioration, and sometimes death due to pulmonary hypertension and right-heart failure during the fourth week after monocrotaline injection. With all BPC 157 regimens, monocrotaline-induced pulmonary arterial hypertension (including all disturbed parameters) was counteracted, and consistent beneficial effects were documented during the whole course of the disease. Pulmonary hypertension was not even developed (early regimens) as quickly as advanced pulmonary hypertension was rapidly attenuated and then completely eliminated (delayed regimen).
Congestive heart failure after doxorubicin regimen (total dose of 15 mg/kg intraperitoneally, divided at six time points, every third day for 14 days to induce congestive heart failure). After four weeks of rest, assessed in mice and rats with advanced disease course, the increased big endothelin-1 (BET-1) and plasma enzyme levels (CK, MBCK, LDH, AST, ALT), before and after next subsequent fourteen days of therapy, and clinical status (hypotension, increased heart rate and respiratory rate, and ascites) every two days [84].
Without therapy, throughout 14 days, both rats and mice further raised BET-1 serum values and aggravated clinical status, while enzyme values maintained their initial increase. BPC 157 (10 µg/kg) and amlodipine treatment reversed the increased BET-1 (rats, mice), AST, ALT, CK (rats, mice), and LDH (mice) values. BPC 157 (10 ng/kg) and losartan opposed further increase of BET-1 (rats, mice). Losartan reduces AST, ALT, CK, and LDH serum values. BPC 157 (10 ng/kg) reduces AST and ALT serum values. Clinical status of chronic heart failure in rats and in mice is accordingly improved by the BPC 157 regimens and amlodipine. However, indicatively, translation to the counteracted hypotension, no dyspnea with increased heart and respiratory occurred in BPC 157 treated animals, whereas hypotension and dyspnea with increased heart rate and respiratory rate persisted in the losartan and amlodipine treated animals.
Thus, given the initial infarct induction and re-infarction (the myocardial lesions after two isoprenaline applications) and that BPC 157 markedly counteracts myocardial isoprenaline lesions, the findings provide multidirectional evidence [38]. Specifically, there is a large range of the BPC 157 regimens (ng-µg) [38] and huge range of the therapy possibilities (i.e., a sustained effect given before isoprenaline, and a rapid effect given after isoprenaline, mortality absent in BPC 157 rats) [38]. Thus, there is consistent and quite complete evidence (i.e., reduction in all of the routine necrosis markers, grossly no visible infarcted area, attenuated histological damage, ECG (no ST-T ischemic changes), and echocardiography (preservation of systolic left ventricular function) damage and oxidative stress parameters decreased) [38]. The interaction with eNOS and COX2 gene expression, and counteraction of the aggravation effect of the NOS-blocker, L-NAME [38], might suggest that NO system function might be accordingly recovered.
In this, the BPC 157 therapy prompt activation of the azygos vein, as before upon BPC 157 therapy [19,[22][23][24][27][28][29]31,[37][38][39][40]) goes along with the combining notation about the atrial myocardium and azygos vein resemblance in the rat [49]. Consequently, the counteraction of the myocardial infarction course might go via azygos vein activation that BPC 157 therapy might promptly initiate (note, without BPC 157 therapy, the azygos vein remained completely collapsed, in the isoprenaline-treated rats, in particular) [38]. There might be prompt direct delivery of blood flow, compensation, and no more failed vessel (i.e., initially congested inferior caval vein and superior mesenteric vein recovered to the normal vein presentation), and blood flow reorganized, seeable with the absent caval and portal hypertension and the decreased brain swelling, and the decreased intracranial (superior sagittal sinus) hypertension [30]. The restored function immediately upon administration might regain reversal of the venous and intracranial hypertension [38] since recovered heart function [38] might ascertain the ability to drain venous blood adequately for a given cerebral blood inflow without raising venous pressures. Grossly, the counteracted progressing venous and arterial thrombosis, peripherally and centrally, counteracted ECG disturbances, and no heart dilatation and absent gastrointestinal (stomach) lesion [38] were present with all microscopic findings. The myocardial presentation was without congestion, and confluent areas of subendocardial ischemic myocytes and the lung, liver, kidney, and gastrointestinal tract were with only mild congestion. Intracerebral hemorrhage and intraventricular hemorrhage in the third ventricle were absent, and karyopyknosis was almost annihilated in all of the brain areas. As mentioned for isoprenaline-myocardial infarction [38], the same chain of events might be seen as a shared principle [19,[22][23][24][27][28][29]31,[37][38][39][40]. Illustratively, the rats underwent the endothelium damaging agent overdose, alcohol [40] and lithium [39], bile duct ligation, acute pancreatitis [37] and maintained intra-abdominal hypertension, grade III and grade IV [31], as well as the described occlusion syndrome with major vessels occlusion, peripheral [19,24,29] or central [27].
Thus, this might be recognized as a special heart-brain-blood vessels interacting axis (providing in the counteracted multiorgan failure, the attenuated myocardial lesions, and arrhythmias as an achieved important tool, either as a cause or as a consequence), peripheral and central interplay, as an essential defensive response [19,[22][23][24][27][28][29]31,[37][38][39][40]. This would be further analyzed specifically with respect to the particular myocardial lesion and heart failure in the large syndrome commonly seen also with the endothelium damaging agent overdose, alcohol [40] and lithium [39], acute pancreatitis [37], and maintained intra-abdominal hypertension, grade III and IV [31], as well as in the described occlusion syndrome with major vessels occlusion, peripheral [19,24,29] or central [27].

Heart Failure
As a follow-up of the described therapy course in the rats with acute myocardial infarction [38], we evidenced that BPC 157 therapy might counteract acute heart failure as it might compensate for the effect of the severe blood flow restriction to the heart ( Table 1). This might occur in a very short time with the major vessel occlusion [19,24,27,29], artery [19] or vein [24], or artery and vein [29], peripherally and centrally, and trapped large blood volume [19,24,29]. The evidenced marked congestion within the myocardium and large coronary branches included the occlusion of the superior mesenteric vein [24], the occlusion of the superior mesenteric artery [19], the simultaneous occlusion of both the superior mesenteric artery and the superior mesenteric vein [29], and centrally, the occlusion of the superior sagittal sinus [27]. The subendocardial infarct, as well as congestion within the myocardium, regularly appeared in the rats with the occluded superior mesenteric vein and artery [29].
Furthermore, as mentioned before (see Section 2.1, Isoprenaline-myocardial infarction [38]), we demonstrated that, in addition to the isoprenaline-myocardial infarction [38], the other major noxious events [31,[37][38][39][40] also acutely caused the prominent heart failure and widespread dysfunction similar to that observed in rats after the occlusion of the peripheral [19,24,29] and central [27] vessels. These were the endothelium damaging agents, i.e., alcohol [32] or lithium [31], bile duct occlusion (acute pancreatitis) [29], organs and vessels compression (intra-abdominal hypertension) [31]. As emphasized before, these occlusion-like syndromes [19,24,27,29] shared the previously described peripheral and central deficits noted in the occlusion syndromes and were largely counteracted by the given BPC 157 therapy. Characteristically, with intragastric absolute alcohol, a prototype noxious agent in the cytoprotection studies, there was timely advancing heart failure [40]. There were rapidly produced heart dilatation and lesions worsening (i.e., 1 min < 5 min < 15 min < 30 min; moderate congestion < tissue congestion and persistent hemorrhage < passive congestion in the myocardium, with acute subendocardial infarct (note contribution of low aortic pressure) < prominent congestion and acute subendocardial infarct) [40]. Rats treated with lithium sulfate overdose for three days since the beginning of treatment presented with severe myocardial congestion, along with subendocardial infarcts and neutrophilic infiltration of the infarcted areas, in particular after the second and third doses of lithium [39]. In the rats with a ligated bile duct, heart dilatation and marked myocardial congestion was consistently noted at 30 min, 5 h, and 24 h ligation time [37]. Already within a very short time with severe intra-abdominal hypertension 25 mmHg, grade III, there was myocardial congestion and sub-endocardial infarction, which appeared as the ultimate outcome [31]. The myocardial congestion and sub-endocardial infarction occurred in an even shorter time with the more severe intra-abdominal hypertension, grade IV (i.e., 30 mmHg/30 min, 40 mmHg/30 min, 50 mmHg/25 min) [31]. Rats with the occluded major vessel(s) superior mesenteric vessels or superior sagittal sinus commonly presented prominent congestion and acute subendocardial infarct (rats with the occluded superior mesenteric artery and vein) [19,24,27,29].
It might be claimed that this therapeutic effect might also ascertain the resolution of the concomitant arrhythmias in heart failure (in heart failure, arrhythmias are commonly acknowledged as the final cause of death [126]). Commonly, there was marked tachycardia, prolonged PQ and QTc intervals, and ST elevation (major vessel(s) occlusion, bile duct occlusion, alcohol intoxication) as identifiers of acute thrombotic coronary occlusion and right heart failure [18,19,23,24,[27][28][29]31,[37][38][39][40]. These all rapidly disappeared under all the BPC 157 regimens (as also noticed in the Pringle maneuver ischemia, reperfusion, portal triad temporary occlusion, and in the Budd-Chiari syndrome with BPC 157 therapy in rats) [18,19,23,24,[27][28][29]31,[37][38][39][40]. Note, it might be a biventricular failure that was accordingly counteracted (as a follow-up of the right heart failure, there was marked congestion of the inferior caval vein, superior mesenteric vein, liver, kidney, and gastrointestinal tract while congested lung with hemorrhage also evidenced left heart failure, all counteracted by BPC 157 therapy) [18,19,23,24,[27][28][29]31,[37][38][39][40]. Lithium overload induced rapidly significant ST elevation, prolonged QTc intervals, and atrioventricular conduction disturbances (i.e., total AV block), in addition to marked bradycardia [39]. Contrarily, BPC 157-treated rats exhibited no repolarization changes, and they showed the conduction system of the heart functioned normally and the normal heart frequency at all time checkpoints and none of the atrioventricular conduction disturbances [39]. There might be additional particular relevance. Namely, the used regimen (500 mg/kg, ip, once daily for three consecutive days) (i.e., higher than usual lithium regimens [127][128][129] but markedly below usual LD50 for lithium application in rats [130]) might be closer to those used in patients considering the conversion of animal doses to human-equivalent doses based on body surface area [131]. Maintaining the severe intra-abdominal hypertension 30 mmHg/30 min, 40 mmHg/30 min, and 50 mmHg/25 min revealed the downhill course timely along with the nodal rhythm, with dominant ST-elevation and bradycardia [31]. Extreme bradycardia and asystole appeared as the ultimate outcome [31]. Contrarily, all BPC 157-treated rats exhibited consistently preserved heart function, with fewer ECG disturbances [31] (preserved sinus rhythm, with occasional first-degree AV block, without ST-elevation, extreme bradycardia and asystole) [31] and normal heart microscopic presentation. To emphasize the achieved therapy effect significance, we should stress the persisting worst circumstances of intraabdominal hypertension, grade III and grade IV [31], pushing up the diaphragm, the most constrained thoracic cavity [31], the rapid transmission of the increased pressure between the three body cavities [31].
Considering the more extended experiments, there was by BPC 157 therapy the counteraction of the monocrotaline-induced pulmonary hypertension in rats [41]. It might be that BPC 157 therapy might affect the monocrotaline course as a whole since pulmonary damage (hours), edema (after one week), pulmonary artery hypertension (after two weeks), right ventricle hypertrophy (after three weeks), and considerable fatal rate (after four weeks), given the same beneficial effect of both the prophylactic regimen and the delayed therapeutic regimen [41]. Analyzing how pentadecapeptide BPC 157 prevents and counteracts monocrotaline-induced pulmonary arterial hypertension and cor pulmonale in rats, the evidence seems to be quite compelling. The experimental protocol [41] comparable to the clinical situation [132] (pulmonary hypertension in the untreated monocrotaline group on day 14) meant the delayed therapy initiation (i.e., day 14) was well-chosen [133] (avoiding the misleading considering the therapeutic effect [132] with shorter premature intervals (day 11 or day 12) after monocrotaline [132,134]). Additionally, the range of the assessed disturbed parameters (which were all counteracted) fully corresponded to other studies [132]. They included disturbed wall thickness, total vessel area, and heart frequency; QRS axis deviation; QT interval prolongation (known to correlate with pulmonary pressure and right ventricle dilation and inversely correlate with right ventricle function [135]; right ventricle hypertrophy; increased right ventricle weight [136,137]; an increase in right ventricle systolic pressure; mortality; and bodyweights loss). In particular, the reduced body weight as a marker of clinical deterioration in the animal, as in the patient, again accords with previous studies [136]. Likewise, with respect to the timing of the initiation of therapy being crucial [132], there was the prophylactic effect (just after monocrotaline), pulmonary hypertension not even developed, as well as the therapeutic effect (on day 14 after monocrotaline) the advanced pulmonary hypertension was rapidly attenuated and then completely eliminated (delayed regimen) [41]. Thus, there is compelling evidence [41] that the right ventricle can be therapeutically targeted in pulmonary arterial hypertension [135].
Further extension toward the chronic heart failure effect [84] was based on the estimated role of the endothelin, and thereby NO-system [137], doxorubicin model [138], and delayed BPC 157 therapy application [84]. After the doxorubicin regimen (total dose of 15 mg/kg intraperitoneally, divided at six time points, every third day for 14 days to induce congestive heart failure), and after four weeks of rest, assessed in mice and rats with advanced disease, the increased big endothelin-1 (BET-1) and plasma enzyme levels (CK, MBCK, LDH, AST, ALT), before and after the subsequent 14 days of therapy, and clinical status (hypotension, increased heart rate, and respiratory rate, and ascites) every two days [84]. Without therapy, throughout 14 days, both rats and mice further raised BET-1 serum values and aggravated clinical status, while enzyme values maintained their initial increase [84]. BPC 157 (10 µg/kg) and amlodipine treatment reversed the increased BET-1 (rats, mice), AST, ALT, CK (rats, mice), and LDH (mice) values. BPC 157 (10 ng/kg) and losartan opposed further increase of BET-1 (rats, mice). Losartan reduces AST, ALT, CK, and LDH serum values. BPC 157 (10 ng/kg) reduces AST and ALT serum values. The clinical status of chronic heart failure in rats and in mice is accordingly improved by the BPC 157 regimens and amlodipine [84]. However, indicatively, in translation to the counteracted hypotension, no dyspnea with increased heart and respiratory occurred in BPC 157 treated animals, whereas hypotension and dyspnea with increased heart rate and respiratory rate persisted in the losartan and amlodipine treated animals [84].

Heart Failure Concomitant Pathology
As mentioned before in the acute myocardial infarction studies [19,24,27,29,31,[37][38][39][40][41] and BPC 157 therapy application, the evidence that the heart failure cause-consequence occurred with the wide range of the concomitant multiorgan failure and initiated multicausal noxious circuit that might also be counteracted by BPC 157 therapy, was specifically elaborated. This was conducted in a series of the different major noxious events and BPC 157 therapy effects, peripherally or centrally, and/or peripherally and centrally [19,24,27,29,31,[37][38][39][40][41]. As challenges confronted with BPC 157 therapy beneficial effects, we used distinctive noxious procedures. This was a confrontation with the occlusion of the superior mesenteric vein, the occlusion of the superior mesenteric artery, the occlusion of the superior mesenteric vein and artery, the occlusion of the superior sagittal sinus, the intragastric application of the absolute alcohol, subsequent intraperitoneal administrations of the lithium overdose, and maintained severe intra-abdominal hypertension grade III and grade IV [19,24,27,29,31,[37][38][39][40][41]. Thereby, there was a large range of the therapy effect, given the similar heart failure described before, and all concomitant similar to multiorgan failure, relayed to the various noxious conditions (i.e., constant major vessel(s) occlusion, constant mechanical compression of the organs and vessels, abrupt challenge of the intragastric bolus (absolute alcohol) or repeated subsequent applications of the lithiumoverdose) [19,24,27,29,31,[37][38][39][40][41]. These multiple organ failure lesions might be perceived as the lesions following diverse noxious agents' direct effect, highlighted in the cytoprotection studies, and vice versa; the counteraction, pleiotropic beneficial effect by BPC 157 therapy might also be understood in the general cytoprotection terms [2][3][4][5][6][7][8].
Centrally, without therapy, there was intracranial (superior sagittal sinus) hypertension as a shared disturbance (note, the regular negative values (i.e., −27 mmHg) changed to the high positive values), quickly counteracted by BPC 157 therapy (reestablished negative pressure values) [27]. Thus, given the recovered heart failure, there was a recovered ability to drain venous blood adequately for a given cerebral blood inflow without raising venous pressure (in contrast, the harmful inability suddenly causes venous and intracranial hypertension) [27]. Moreover, the instant severe brain swelling was shared (i.e., in lithiumrats [39] as well as in the alcohol-rats [40]; the brain volume proportional with the change in the brain surface area revealed an immediate increase to 120% of the healthy presenta-tion). Likewise, there was also shared therapy effect of BPC 157 therapy, and promptly attenuated brain swelling. Regularly, without therapy, all investigated noxious procedures (i.e., alcohol intoxication, lithium intoxication, maintained severe intra-abdominal hypertension, vessels occlusion, superior mesenteric artery and/or vein, and superior sagittal sinus) [19,24,27,29,31,[37][38][39][40] presented the severely damaged brain areas, i.e., cerebral and cerebellar cortex, hypothalamus/thalamus, and hippocampus. Prominent edema and large areas with increased numbers of karyopyknotic cells occurred as shared harmful and inevitable outcomes. These were all attenuated or even eliminated by BPC 157 therapy. As a distinctive point, there was a large intracerebral hemorrhage fully counteracted by BPC 157 therapy. Illustratively, the lithium rats exhibited hemorrhage in the deeper brain, both gray and white matter. Rats with bile duct occlusion presented pronounced intracerebral hemorrhage affecting large areas of the corpus callosum, amygdala, thalamus, neocortex, and striatum, and intraventricular hemorrhage in the third and lateral ventricles [39]. After intragastric alcohol, brain edema after 1 and 5 min, with vascular congestion progressed after 15 and 30 min to generalized congestion, edema, and intracerebral hemorrhage, with degenerative changes in the cerebral and cerebellar neurons indicating toxic changes created by the ethanol [40]. In the rats with occluded superior mesenteric artery and superior mesenteric vein [29], there was a subarachnoid hemorrhage at the base of the brain in the cerebellar area, and more karyopyknotic cells in the cerebral and cerebellar cortex, hippocampus, and hypothalamus/thalamus. In the rats with the occluded bile duct, there were timely progressing pronounced intracerebral hemorrhages in areas of the corpus callosum, amygdala, thalamus, neocortex, and striatum, intraventricular hemorrhage involving the third and lateral ventricles and more karyopyknotic cells in the cerebral and cerebellar cortex, hippocampus, and hypothalamus/thalamus [37]. In the rats with the occluded superior sagittal sinus, complete infarction appeared at 24 h and marked karyopyknosis at 48 h [27]. Rats with maintained severe intra-abdominal hypertension exhibited subarachnoid hemorrhage at the base of the brain in the cerebellar area and more karyopyknotic cells in the cerebral and cerebellar cortex, hippocampus, and hypothalamus/thalamus [31]. These brain lesions appeared to be distinctively affected by high intra-abdominal pressure; i.e., the most progressive hippocampal neuronal damage was found with the highest intra-abdominal pressure [31].
Thus, the indication of the brain lesions and hemorrhage and their counteraction evidence might be seen as particular maxim (i.e., occluded superior mesenteric vessels vs. occluded superior sagittal sinus vs. alcohol/lithium application vs. bile duct occlusion vs. maintained intra-abdominal pressure, prime peripheral lesions vs. prime central lesions vs. peripheral and central lesions) [19,24,27,29,31,[37][38][39][40]. This might suggest that the heart failure cause-consequence might occur in a bidirectional way that might be both beneficially affected by the BPC 157 therapy.
At the periphery, there were portal and caval hypertension and aortal hypotension, markedly attenuated or even eliminated by BPC 157 therapy [19,24,27,29,31,[37][38][39][40]. In particular, depending on the prime injurious challenge (i.e., vascular occlusion vs. bile duct occlusion vs. intragastric absolute alcohol vs. intraperitoneal lithium challenge vs. maintained intra-abdominal hypertension), the lesion shared considerable severity along with the described heart failure and prominent brain lesions [19,24,27,29,31,[37][38][39][40]. These were all attenuated or even eliminated by BPC 157 therapy [19,24,27,29,31,[37][38][39][40]. Illustratively, rats with maintained severe intra-abdominal hypertension exhibited lung parenchyma with marked congestion and large areas of intra-alveolar hemorrhage, vascular dilation of the liver parenchyma, and severe congestion of renal tissue [31]. With a severity increase from the upper toward the lower part of the gastrointestinal tract, there was transmural hyperemia of the entire gastrointestinal tract, stomach, duodenum, and small and large bowel wall, along with a reduction in the villi in the intestinal mucosa, crypt reduction with focal denudation of superficial epithelia, and dilatation of the large bowel [31]. Likewise, without therapy, all of the rats with the occluded superior mesenteric vessel(s) (i.e., occluded superior mesenteric artery, or occluded superior mesenteric vein, or occluded both superior mesenteric artery and vein) exhibited marked transmural congestion in an ascending sequence from the stomach to the large bowel [19,24,29]. This might be the particular maxim: the stomach (dilated capillaries in the lamina propria) < duodenum (mild mucosal injury, blunt villi, and mild hyperplasia of the crypts) < small bowel wall (focal hemorrhage in the lamina propria) < large bowel wall (severe mucosal injury with lumen dilatation and reduction of crypts). There were the focal thickening of the alveolar membranes, lung congestion, pulmonary edema, intra-alveolar hemorrhage, focal interstitial neutrophil infiltration, mild activation of Kupffer cells, and severe enlargement of sinusoids with liver congestion, mild degeneration of proximal tubules, severe renal vascular congestion and interstitial edema [19,24,29]. A similar presentation appeared with the central occlusion [27]. In rats with the occluded superior sagittal sinus, the marked congestion in the heart tissue within the myocardium and large coronary branches exhibited huge additional pathology [27]. There were the gross stomach lesions, and microscopically, erosive gastritis, the liver congestion, and lung congestion with intra-alveolar hemorrhage and pyknotic hepatocyte nuclei, hyaline tubular cylinders, cell degeneration of proximal and distal tubule with cytoplasmic vacuolization in the kidney after both a short-term (15 min ligation time, and period thereafter) and a long-term (24 h, 48 h) period. In the rats challenged with the intragastric absolute alcohol instillation [40], the large gross hemorrhagic lesions and severe pathology in the stomach (i.e., mucosal surface erosion, even in the macroscopically intact areas) were along since very early time (i.e., 1 min post-alcohol) with the progression of the other lesions. They exhibited lung tissue congestion with persistent hemorrhage, liver lesions, congestion, and a ballooning of hepatocytes in zone three of the liver lobules and kidney lesions, congestion, and its progression in the renal tissues presented with dilated and congested small, medium, and large blood vessels, as well as glomeruli. In the rats challenged with the subsequent lithium overdose, along with the described heart failure, there was the progressing lesions presentation [39]. They exhibited in the lungs marked congestion, intra-alveolar hemorrhage, and interstitial neutrophil infiltration, liver with congestion and dilatation of central veins, sinusoids, and portal tracts vessels, marked congestion and vacuolization of the renal tubular epithelia with degenerative changes and marked congestion in the gastrointestinal tract (and gross stomach lesions). As an interesting point, severe muscular weakness might appear immediately, while a decrease in muscular fibers microscopically appears later. In the rats with the occluded bile duct, there was timely progress of a large range of lesions [37]. They exhibited marked lung parenchyma congestion along with intra-alveolar hemorrhage. Moreover, they had marked dilatation and congestion of blood vessels in the portal tracts, central veins, and sinusoids, along with the zones of confluent necrosis affecting the liver lobuli and the portal tract. There was marked dilatation and congestion of blood vessels in the kidney tissue as well as glomeruli and marked congestion in the gastrointestinal tract (and gross stomach and duodenal lesions). These were along with the timely progressing acute pancreatitis lesions. They exhibited grossly separate to confluent hemorrhagic zones and/or foci of necrosis, and microscopically to diffuse edema of interlobar septe, interlobular septe, interacinal spaces, diffuse expansion of intercellular spaces, increased number of necrotic acinar cells/HPF (extensive confluent necrosis) and foci of hemorrhage and fat necrosis, perivascular increased infiltration leukocytes/HPF, and confluent microabscesses [37].
Thus, the indication of the larger range of peripheral lesions and hemorrhage and their counteraction evidence might be seen as a particular and complex maxim. This complex maxim might be the particularity of the prime lesion (i.e., occluded superior mesenteric vessels vs. occluded superior sagittal sinus). This complex maxim equally supposed one prime lesion (alcohol-hemorrhagic lesions, bile duct occlusion pancreatitis) or many prime lesions (lithium application, maintained intra-abdominal pressure), and thereby, prime peripheral lesions vs. prime central lesions vs. peripheral and central lesions. This might suggest that the heart failure cause-consequence might occur in the periphery between the heart and affected organ (i.e., lung, liver, kidney, gastrointestinal tract) in a multidirectional way that might be all beneficially affected by the BPC 157 therapy.
Thereby, it might be that the alcohol intoxication [40], lithium intoxication [39], maintained severe intra-abdominal hypertension [31], and vessels occlusion, superior mesenteric artery and/or vein, and superior sagittal sinus [19,24,27,29] appeared as a multiple occlusion syndrome that could not be avoided unless therapy was given. Regularly, reciprocal changes in the abdominal, thoracic, and brain cavities rapidly transmitted through the venous system rapidly appeared as determinants of vascular failure. Therefore, with BPC 157, there might be a rapid improvement of venous system function as an essential common point to prevent and reverse the noxious chain of events and attenuate all harmful consequences. For illustration, an activated azygos vein as a rescuing pathway, avoiding both the lung and liver, combines the inferior caval vein and superior caval vein via direct blood delivery [19,24,27,29,31,[37][38][39][40]. Thus, an activated azygos vein shunt could reorganize blood flow and instantly attenuate the consequences of maintained occlusion-induced vascular failure, both peripherally and centrally [19,23,24,27,29,31,[37][38][39][40]. Consequently, as a chain of events that might be fully counteracted with BPC 157 therapy, there were counteracted in these rats with the occlusion and occlusion-like syndrome, the multiorgan failure (i.e., gastrointestinal, brain, heart failure, liver, and kidney lesions), portal and caval hypertension, aortal hypotension, intracranial (superior sagittal sinus) hypertension, and generalized thrombosis counteracted. This led to the useful BPC 157 therapy of the harmful circle, the counteraction of the generalized stasis, generalized Virchow triad presentation, and heart failure and severe ECG disturbances. As a prime and practical confirmation, rats with major vessel ligation and occlusion, in either artery and/or vein, and either peripherally or centrally, and other alike noxious occlusion-like procedures exhibited a similar syndrome (occlusion syndrome or occlusion-like syndrome) and shared full therapy benefit with the given BPC 157 therapy [18,19,23,24,27,29,31,[37][38][39][40].

Specifically maintained function of thrombocytes (aggregometry and thromboelastometry studies)
Intragastric application of aspirin, clopidogrel, cilostazol, and BPC 157 in rats: Platelet aggregation and blood clot. Oxid. Med. Cell. Longev. 2019, 2019, 9084643. [60] Commonly, illustrating thrombotic complications' major role in patients with heart failure is a major issue in therapy; in 2021, several major trials attempted to resolve whether shortened dual antiplatelet therapy reduced bleeding risk without increasing the risk of further ischemic events [1].
On the other hand, it might be that BPC 157 (cytoprotection as endothelium function maintenance) [2][3][4][5][6][7][8] might collaborate with the evidence of heart failure innate etiopathology [163]. There are significant pro-thrombotic shifts and endothelial damage/dysfunction as a hallmark of heart failure, irrespective of any cause, related to the severity of heart failure [163]. Thereby, there are thrombi formations both within cardiac chambers (particularly in atrial fibrillation) and blood vessels, and both arterial endothelial dysfunction and venous dysfunction present in heart failure contribute to the pro-thrombotic state seen in this condition [163].
Providing strong interrelations between the arrhythmias, heart failure, and thrombosis [164], assuming the venous and arterial thrombosis as two aspects of the same disease [165,166], the BPC 157 counteracting effect might be reciprocally related. Thus, in heart failure therapy, the therapeutic effect of BPC 157 administration might counteract the escalating thrombosis as a shared common point [19,24,27,29,31,[37][38][39][40]. This might be the consequent reversal of the general stasis (i.e., otherwise large volumes trapped in the damaged stomach, CNS, and portal and caval vein tributaries, which may also perpetuate the brain and heart ischemia). Along with this, it might be the reversal of the failed activation of the collateral bypassing pathways. This rapidly appeared within minutes while the major veins which had been disabled (inferior caval and superior mesenteric veins failed as congested and the azygos vein failed as collapsed [19,24,27,29,31,[37][38][39][40]) might be quickly recovered, rapidly made fully functional. At the same time (i.e., direct blood delivery by the activated azygos vein), in the heart failure recovery, the otherwise progressing thrombosis in veins and arteries might be markedly attenuated (or even eliminated) as well as the progressing intracerebral and interventricular bleeding markedly attenuated or even annihilated [19,24,27,29,31,[37][38][39][40]. Thus, this might be the innate resolution of the Virchow triad consequences [19,24,27,29,31,[37][38][39][40]. Likely, this might be the effect related to the modulatory interaction with NO-system [61][62][63]. As proof, BPC 157 therapy effects might counteract in the same dosage range NOS-blockade (L-NAME)-induced pro-thrombotic and hypertensive effect as well as NOS-over-activity (L-arginine)-induced anti-thrombotic and hypotensive effect [59,62].

Blood Pressure
Interestingly, in patients who were hospitalized for heart failure, the risks of mortality and readmission increased at low and high blood pressures, with similar trends for patients with heart failure with reduced ejection fraction and with heart failure with preserved ejection fraction [167,168].
On the other hand, in the severe hyperkalemic condition regularly fatal within 30 min time, BPC 157 therapy, along with ascertained survival and counteraction of arrhythmias, might counteract hyperkalemia-induced hypertension [67]. Likewise, BPC 157 therapy might counteract hypertension induced by unilateral renal artery stenosis or by unilateral renal artery stenosis and contralateral nephrectomy [169]. Moreover, as mentioned before, BPC 157 therapy might counteract NOS-blocker L-NAME-induced hypertension, an effect along with counteraction of the L-NAME-induced pro-thrombotic effect [58,61,62]. Finally, in glaucomatous rats, BPC 157 might normalize the increased intraocular pressure [26].
Furthermore, BPC 157 therapy might oppose hypovolemic shock, hypotension, and mortality after controlled blood volume withdrawal [169]. Likewise, as mentioned before, BPC 157 therapy might counteract the NOS-substrate L-arginine-induced hypotension, an effect along with counteraction of the L-arginine-induced anti-thrombotic effect [58,61,62]. As in the mentioned acute studies, in the heart failure chronic studies with doxorubicin, along with counteraction of the heart failure, BPC 157 therapy strongly opposed hypotension [84]. This effect was along with the counteraction of the increased big endothelin-1 (BET-1) and plasma enzyme levels (CK, MBCK, LDH, AST, ALT) and improved clinical status in general [84].
As a particular notation, BPC 157 had no effect on normal blood pressure [61,62]. Thus, the effect on blood pressure of BPC 157 therapy might be effectively related to the resolution of particular sick conditions, likely depending on the normalization of the heart function, as cytoprotection application is able to normalize either disturbed blood pressure or hypotension.

Smooth Muscle
BPC 157 therapy might exert the described particular effect on blood pressure given the relaxation noted in the aorta without endothelium ex vivo but not relaxation directly on the 3D model composed of vascular smooth muscle cells (unlike the effect of NOdonor sodium nitroprusside) [53]. Possibly, this might be the release of the NO by its own [61][62][63], activated phosphorilazation of eNOS [53] as a special modulatory effect, given the mentioned counteraction of the adverse effect of NOS-blockade (i.e., L-NAMEhypertension and pro-thrombotic effect), as well as the counteraction of the adverse effect of NOS-over-stimulation (i.e., L-arginine-hypertension and anti-thrombotic effect) [58,62]. Moreover, the VEGFR2-Akt-eNOS signaling pathway might be activated without the need for other known ligands or shear stress, controlling vasomotor tone and the activation of the Src-Caveolin-1-eNOS pathway [53,54]. These might also be perceived as BPC 157/NOsystem interaction in controlling blood pressure by a particular mechanism.
Life-saving effect in severe hyperkalemia without affecting the extremely high level of potassium in blood. Given 30 min before KCl, all BPC 157 regimens regained sinus rhythm, had less prolongation of QRS, and had no asystolic pause. BPC 157 therapy, given 10 min after KCl-application, starts the rescue within 5-10 min, completely restoring normal sinus rhythm at 1 h. Likewise, other hyperkalemia disturbances (muscular weakness, hypertension, low sphincteric pressure) were also counteracted. Intragastric BPC 157 (10 ng, 10 µg) application, given 30 min before or 10 min after intragastric KCl, fully counteracted the severe stomach mucosal lesions, sphincter failure, and peaked T waves. In HEK293 cells, in hyperkalemic conditions (18.6 mM potassium concentrations), BPC 157 directly affects potassium conductance, counteracting the effect on membrane potential and depolarizations caused by hyperkalemic conditions.
Succinylcholine administration (1.0 mg/kg into the right anterior tibial muscle). Assessments were made at 3 and 30 min and one, three, five, and seven days after. The local paralytic effect Systemic muscle disability (and consequent muscle damage), Hyperkalemia, arrhythmias, and a rise in serum enzyme values [68] BPC 157 successfully antagonized the depolarizing neuromuscular blocker effects of succinylcholine. BPC 157 (10 µg/kg, 10 ng/kg) (given intraperitoneally 30 min before or immediately after succinylcholine or per-orally in drinking water through 24 h until succinylcholine administration) mitigated both local and systemic disturbances. BPC 157 completely eliminated hyperkalemia and arrhythmias, markedly attenuated or eradicated behavioral agitation, muscle twitches, motionless resting, and completely eliminated post-succinylcholine hyperalgesia. BPC 157 immediately eliminated leg contractures and counteracted both edema and the decrease in muscle fibers in the diaphragm and injected/non-injected anterior tibial muscles.
Life-saving effect in severe hypokalemia without affecting the extremely low level of potassium in blood.
All of the fatalities with T-wave elevation, high-degree AV-block, respiratory arrest, and asystole.
BPC 157 as potential antidote for bupivacaine cardiotoxicity. Bradycardia, AV-block, ventricular ectopies, ventricular tachycardia, T-wave elevation, and asystole. All of the fatalities had developed T-wave elevation, high-degree AV-block, respiratory arrest, and asystole. These were largely counteracted by BPC 157 administration (50 µg/kg, 10 µg/kg, 10 ng/kg, or 10 pg/kg IP) given 30 min before or 1 min after the bupivacaine injection. When Since very early, a prolonged QTc interval has been continually noted with haloperidol, fluphenazine, clozapine, olanzapine, quetiapine, sulpiride, and metoclopramide in rats as a common central effect not seen with domperidone [72].
To counteract neuroleptic-or prokinetic-induced prolongation of the QTc interval, rats were given a BPC 157 regimen once daily over seven days (10 µg, 10 ng/kg ip) immediately after each administration of haloperidol, fluphenazine, clozapine, quetiapine, sulpiride, metoclopramide or domperidone. Consistent counteraction appears with the stable gastric pentadecapeptide BPC 157. Thus, BPC 157 rapidly and permanently counteracts the QTc prolongation induced by neuroleptics and prokinetics.

Digitalis
Without therapy, the used digitalis regimen was regularly fatal, and thereby, it might be a particular challenge for the BPC 157 therapy, which might be dose-dependent, to both prevent or attenuate the development of the digitalis intoxication and reverse already established digitalis intoxication [66]. Without therapy, the established digitalis intoxication (the grade 3 AV-block quickly developed) outcome was inevitably complicated by fatal ventricular tachycardia and fatality in all animals.
In digitalis rats, AV-block might be a particular target for the BPC 157 therapy [66]. Given prophylactically, ng regimens reduced just the AV-block duration, while higher dose regimens, BPC 157 µg regimens, aside from AV-block, also reduced the number of ventricular premature beats, prolonged the time until the onset of ventricular tachycardia, and reduced the duration of ventricular tachycardia [66].
Moreover, BPC 157 therapy also had the potential to compensate for the additional aggravation that might occur in the digitalis rats. Illustratively, the BPC 157 effect as NO-system related activity might evidence the BPC 157 administration to annihilate the strong aggravation that occurred with NOS-blocker L-NAME application, given either prophylactically or in the established digitalis intoxication [66].

Hyperkalemia
The hyperkalemia challenge for the BPC 157 therapy was intraperitoneal KCl-solution application (9 mEq/kg). In regularly deadly hyperkalemia (>12 mmol/L), arrhythmias with an ultimate and a regularly inevitable lethal outcome within 30 min [67] were both prevented with BPC 157 given before KCl application, as well as cured with BPC 157 therapy given later, in the conditions of the advanced and established huge hyperkalemia-induced disturbances. Intraperitoneal prophylactic regimen goes with the recovered sinus rhythm, less prolongation of QRS, and without asystolic pause [67]. Given at the 10 min point of the severely advanced downhill course after KCl application, the therapeutic regimen required 5-10 min period to start recovery, with normal sinus rhythm at 1 h. Of note, the particular BPC 157 counteracting potential toward hyperkalemia might first encourage the similar results obtained with the intragastric KCl application (27 mEq/kg)-(hyperkalemia 7 mmol/L) and BPC 157 therapy protocol (i.e., peaked T waves, fully counteracted by BPC 157 application, applied 30 min before or 10 min after KCl [67]). Then, the supporting point is the evidence that BPC 157 administration might have the potential to compete with further worsening instances. Illustratively, the direct effect seeable on potassium conductance in HEK293 cells, hyperkalemic conditions (18.6 mM potassium concentrations), counteracting the effect on membrane potential and depolarizations caused by hyperkalemic conditions, might annihilate L-NAME, NOS-blocker-induced aggravation, and thereby, BPC 157-hyperkalemia's direct relationship might occur as a NO-system related interconnection. Likewise, other hyperkalemia disturbances (muscular weakness, hypertension, low sphincteric pressure with intraperitoneal KCl-application, severe stomach mucosal lesions, and sphincter failure with intragastric KCl-application) were also counteracted [67].

Succinylcholine
The counteraction/attenuation of the adverse effect of succinylcholine by BPC 157 therapy [68] might illustrate that, depending on the cause (potassium-overload [67]; succinylcholine application [68]), BPC 157 therapy (microgram and nanogram dose, intraperitoneal and peroral regimen) might distinctively affect hyperkalemia. While in the rats after potassium overload, the hyperkalemia persisted and the adverse effects were counteracted [67]. The illustrative might be the findings in the rats intramuscularly treated with succinylcholine (counteracted hyperkalemia, counteracted adverse effects). As succinylcholine acts as depolarizing neuromuscular blocker and disabling neuromuscular junction [68], this might indicate a particular recovering effect of BPC 157 therapy. Normokalemia and no arrhythmias, completely absent intermittent AV block and asystolic pauses, continuously maintained sinus rhythm, supplementing the evidence that BPC 157 therapy might attenuate the succinylcholine course as a whole. The therapeutic effect included the succinylcholine-induced behavioral agitation, muscle twitches, and motionless resting, and completely eliminated post-succinylcholine hyperalgesia, immediately eliminated leg contractures (intramuscular succinylcholine), counteracted both edema and the decrease in muscle fibers in the diaphragm and injected/non-injected anterior tibial muscles) [68]. Otherwise, succinylcholine-rats exhibited hyperkalemia with brisk arrhythmias (peaked T waves, widening of PR and QRS complexes, aggravation in intermittent AV block, and asystolic pauses (at 4-5 min period, but spontaneously recovered by the 15th min) [68].

Hypokalemia
The hypokalemia challenge for the BPC 157 therapy was a huge furosemide dose application and consequent efficacy in the otherwise deadly hypokalemia (<2.7 mmol/L) against the severe arrhythmias (i.e., polymorphic ventricular tachycardia ("torsades de pointes")) (note, unlike full survival with BPC 157 therapy, without therapy, the lethal outcome occurred within 90-150 min) [69]. These were both prevented with BPC 157 given before furosemide application (AV block and abnormal ventricular rhythm were absent). Likewise, these were both annihilated with BPC 157 therapy given later after furosemide in the conditions of the advanced severe disturbances, i.e., the third-degree AV block and ventricular tachycardia, as complete restoration of the sinus rhythm occurred within a few minutes upon application of BPC 157 therapy [69]. In addition, the supporting point for BPC 157-hypokalemia particular relation is the evidence that BPC 157 administration might also counteract the further worsening. Illustratively, BPC 157 completely annihilated the aggravation induced by NOS-blocker L-NAME in the furosemide rats [69]. Moreover, BPC 157 therapy might have a direct effect on potassium conductance, seeable in HEK293 cells, BPC 157 (1 µM) abolished hyperpolarizations of HEK293 cells during hypokalemic (0.4 mM K) conditions [69]. Finally, as support of the effect on hypokalemia as a whole, all of the BPC 157 treated furosemide rats were without sudden, brief, shock-like, involuntary movements (i.e., hypokalemia-induced myoclonus), either completely prevented or rapidly reversed when they had been advanced along with arrhythmias [69].

Local Anesthetics, Bupivacaine
After an overdose of bupivacaine or any of the related amide local anesthetic agents, cardiovascular collapse, or even death, may occur [178]. Thereby, providing the used dose of bupivacaine (100 mg/kg IP), there is important evidence that BPC 157 successfully prevents and counteracts bupivacaine cardiotoxicity [70]. As a highlight of the practical applicability, BPC 157 is effective even against the worst outcomes, such as a severely prolonged QRS complex [70].
Amide local anesthetic agents overdose, in particular an overdose of bupivacaine (note, we used 100 mg/kg IP), might be associated with cardiovascular collapse or even death [188]. Likewise, BPC 157 therapy might be associated with counteraction of bupivacaine cardiotoxicity (i.e., bradycardia, high-degree AV-block, ventricular ectopies and tachycardia, T-wave elevation, respiratory arrest, and asystole), even with the upmost counteraction that might be needed against the worst outcomes (counteraction of the severely prolonged QRS complex). BPC 157 has no apparent limitation considering the therapy initiation. It might be effective early (at 30 min before or at 1 min after the bupivacaine injection, counteraction encompassed 50 µg/kg, 10 µg/kg, 10 ng/kg, or 10 pg/kg IP BPC 157 regimens). Likewise, it might be effective after delaying treatment (at 6 min after bupivacaine administration, and after the development of prolonged QRS intervals (20 ms), the fatal outcome was markedly postponed). Together, this might indicate a par-ticular direct competition with the escalating bupivacaine course since, in HEK293 cells, BPC 157 inhibited the bupivacaine-induced depolarization [70]. Likewise, it remains to be seen how BPC 157 might specifically interfere with the specific bupivacaine inhibitory targets, such as the transient outward K+ current in ventricular myocytes or the fast block of sodium channels during the action potential with slow recovery from block during diastole [189,190].

Local Anesthetics, Lidocaine
The antagonism of the entire spectrum of local anesthetic-induced neurotoxic and cardiotoxic effects [71] was the issue with lidocaine, as prototype application (intraperitoneal, intraplantar and axillary, and spinal (L4-L5) intrathecal block) toward the particular beneficial recovering effect of BPC 157 therapy, intraplantar, intraperitoneal, and intragastric application. First, BPC 157 counteracted lidocaine-bradycardia, which might be a severe one, prevented bradycardia development as well as reversed established bradycardia, given either before or after lidocaine [71]. Likewise, BPC 157, given before or after, counteracted the lidocaine-induced local anesthesia via the intraplantar application and axillary and spinal (L4-L5) intrathecal block. Moreover, BPC 157 counteracted lidocaine-induced convulsions. In vitro, BPC 157 counteracted lidocaine-induced HEK293 cell depolarization [71]. There might be BPC 157-lidocaine-NO-system interconnections [71], providing that BPC 157 administration might completely annihilate the strong aggravation that might occur with the NOS-blocker L-NAME application [71].

Neuroleptics and Prokinetics Induced Prolonged QTc Interval
The evidence of the beneficial BPC 157 effect with the neuroleptics and prokinetics application versus the prolonged QTc intervals is a known shared adverse effect of the neuroleptics and prokinetics application [72]. Here, with the prolonged QTc intervals effect after application of the dopamine neuroleptics and prokinetic metoclopramide, but not after domperidone (known to act peripherally), the neuroleptics and prokinetic prolonged QTc intervals occurred as the particular central effect [72]. Finally, the consistent antagonization and the use of the various neuroleptics, both typical (haloperidol, fluphenazine) and atypical (sulpiride, clozapine, quetiapine), might provide the BPC 157 therapy potential (i.e., the counteraction of the prolonged QTc intervals) as capable of antagonizing an essential class adverse effect [72]. Note that the potential involvement of pathological ion channel modulation might be shared disorder in the etiology of neurological disorders, cardiovascular disease, and, ultimately, arrhythmias [191]. Likewise, in the same dose regimens, BPC 157 therapy counteracted the neuroleptic-induced catalepsy and akinesia and gastrointestinal disturbances [173,192] and hippocampal ischemia/reperfusion injuries in rats in the stroke studies (therapy after reperfusion initiation, after carotid arteries clamping) [20]. Additionally, with BPC 157 therapy, there might be the brain-gut and gutbrain axis function recovery [2,193], while BPC 157, when given peripherally, might exert particular central beneficial effects [2,193]. Illustratively, these were the release of serotonin in the specific brain areas (i.e., nigrostriatum) [194], as opposed to the schizophrenia-like positive symptoms models [187] and schizophrenia-like negative symptoms models [195]. Finally, BPC 157 counteracted various encephalopathies [91][92][93][94][95][96].

Conclusions
As the essential new result of the stable gastric pentadecapeptide BPC 157 therapy, as a part of the implemented cytoprotective effect (see Sections 1, 1.1 and 1.2), specifically proved in the vascular studies, there was the particular activation of the collateral pathways . Illustratively, in the rats with myocardial infarction and heart failure, the azygos vein might be completely collapsed (failed collateral pathways), while with BPC 157 therapy activated the azygos vein which might provide direct blood flow delivery to the superior caval vein and reestablish reorganized blood flow [19,24,27,29,31,[37][38][39][40]. With BPC 157 therapy, this might be the upgrading of the minor vessel to take over the function of the disabled major vessel, competing with and resolving the Virchow triad circumstances, which might be devastatingly present (i.e., almost annihilated thrombosis as a positive outcome of the regained endothelium function and resolved stasis). This might make possible the recruitment of collateral blood vessels, compensating vessel occlusion, and reestablishing blood flow or bypassing the occluded or ruptured vessel . Thereby, the described BPC 157 therapy beneficial effects (see Sections 2, 2.1, 2.2 and 3-5) might be seen as a network of the interrelated evidence that together might support each other effect for the physiologic significance of the revealed BPC 157/vascular-system interplay. As a part of the effectively realized BPC 157/vascular-system interplay (lack of the adverse effect), there was the heart failure innate recovery as a whole (including counteracted various arrhythmias and counteracted thrombosis, blood pressures disturbances (intracranial (superior sagittal sinus), portal and caval hypertension, and aortal hypotension [19,24,27,29,31,[37][38][39][40]84], or hypertension (hyperkalemia, NOS-blockade) [62,67] attenuated/eliminated peripherally and centrally). Moreover, as part of the general beneficial pleiotropic effect (as part of the cytoprotection background) [2][3][4][5][6][7][8], there was the counteraction of the concomitant severe vessel and multiorgan failure syndrome [19,24,27,29,31,[37][38][39][40], the counteraction of the brain, lung, liver, kidney and gastrointestinal severe lesions, almost annihilated thrombosis, counteraction of the escalated general peripheral and central syndrome. Thus, given the obtained beneficial effects in the heart failure of the BPC 157 therapy and the counteraction of the concomitant pathology, it might be that the heart failure cause-consequence circuit might occur in a multidirectional way that BPC 157 therapy might beneficially affect as a whole. Centrally, illustrative heart failure cause-consequence circuit [27] goes as the comparable BPC 157 therapy effect on the stroke in rats, therapy in the reperfusion after bilateral clamping of the common carotid arteries for a 20-min period [20]. At the periphery, the heart failure cause-consequence circuit might occur between the heart and affected organ (i.e., lung, liver, kidney, gastrointestinal tract) in a multidirectional way that might be all beneficially affected by the BPC 157 therapy [19,24,27,29,31,[37][38][39][40]. Finally, the physiologic significance of the revealed BPC 157/vascular-system interplay goes with the BPC 157 found in situ hybridization and immunostaining studies in humans to be largely distributed in tissues [3,102], and similar effects and roles in other species (i.e., birds [86], and insects, honeybees [204,205]). There might also be additional physiologic regulatory roles [3,102] (i.e., plethora interactions with distinctive molecular pathways [50][51][52][53][54][55][56][57] (in particular NO-system [53,54,[61][62][63]] and prostaglandin-system [2][3][4][5][6][7][8]74]), throughout the healing and vascular recovery). These might be along with the very safe BPC 157 profile (i.e., absent adverse effects in clinical trials (ulcerative colitis, phase II), LD1 could be not achieved in toxicological studies) (for review, see, i.e., [2][3][4][5][6][7][8]61,74,102]). This might be taken as a definitive advantage, as recently confirmed in a large study conducted by Xu and collaborators [206]. Together, these findings (for review, see, i.e., [2][3][4][5][6][7][8]61,74,102]) are suggestive of the BPC 157 cytoprotection application in further vascular injuries therapy, and suitable for use on myocardial infarction, heart failure, pulmonary hypertension, arrhythmias, and thrombosis therapy as well (for a suited summary see concluding Figure 1).