- Email: [email protected]
Critical Determinants of Limb Ischemia⁎
Journal of the American College of Cardiology © 2008 by the American College of Cardiology Foundation Published by Elsevier Inc.
EDITORIAL COMMENT
Critical Determinants of Limb Ischemia* John P. Cooke, MD, PHD, FACC Stanford, California
Peripheral arterial disease (PAD) involving the lower extremities affects 8 to 12 million Americans (1). Typically, PAD is secondary to atherosclerotic occlusive disease of the aortoiliac, femoral, popliteal, and/or the infrapopliteal arteries. The clinical manifestations depend in part on the level of disease and its severity. The classic symptom of intermittent claudication (pain with walking, relieved by rest) typically involves the calf, but the thigh and/or buttocks can be affected with more proximal arterial disease. Classic symptoms are only manifested by 10% to 30% of patients (2,3). More often, the patients are asymptomatic, or their symptoms are disguised by (or attributed to) associated diabetic neuropathy or musculoskeletal disorders, each of which are common in the demographic affected by PAD.
Vol. 52, No. 5, 2008 ISSN 0735-1097/08/$34.00 doi:10.1016/j.jacc.2008.05.004
the pressure at the arm), with functional capacity as assessed by treadmill testing (5). This heterogeneity may be in part due to individual differences in the response of the skeletal muscle to ischemia. For example, the expression and activity of key mitochondrial enzymes are altered in skeletal muscle from PAD patients, and mitochondrial electron transport is impaired (6). Metabolic byproducts of fatty acid oxidation, the acylcarnitines, accumulate in both the plasma and the skeletal muscle of patients with PAD, and are strongly correlated with impairment in exercise capacity (6). The vascular response to conduit vessel occlusion also seems to be subject to individual variation. Measures of skin microcirculation have been used prospectively to predict amputation in CLI patients with unreconstructable vascular disease (7). In patients with reduced skin capillary density (⬍20/mm2), low transcutaneous oxygen (TcPO2 ⬍10 mm Hg), and absent reactive hyperemia, limb survival at 1 year was only 15%, compared with 88% in CLI patients with greater values for the skin microcirculation. Furthermore, it is widely recognized that collateral vessel formation is heterogeneous in patients with the same degree of conduit vessel obstruction. In 1 patient with a superficial femoral artery occlusion, robust collateral formation (arteriogenesis) via the deep femoral artery and geniculate collaterals will revascularize the infrapopliteal vessels. The patient may have minimal or no symptoms. Another patient will be significantly limited by the same occlusive disease, in a setting of sparse collateral formation.
See page 387
Regulation of Angiogenesis
A more severe form of PAD is characterized by pain at rest (typically in the foot, occurring often at night, and relieved by dependency). These individuals have a limb in jeopardy, and the most minor trauma (from a poorly fitting shoe, or a carelessly clipped toenail) can result in a nonhealing wound, infection, and amputation. This form of PAD is known as critical limb ischemia, and affects about 10% of PAD patients. Critical limb ischemia (CLI) is a mortal illness: at 1 year after presentation, 30% have suffered an amputation and 25% of patients are dead (4). Why Are There Differences in the Clinical Presentation of PAD?
Although hemodynamically significant obstructions of the conduit arteries play an acknowledged role in the manifestations of PAD, there is considerable heterogeneity in the degree of symptoms. Furthermore, there is only a modest correlation of hemodynamic assessments, such as the anklebrachial index (ABI) (the pressure at the ankle divided by *Editorials published in the Journal of the American College of Cardiology reflect the views of the authors and do not necessarily represent the views of JACC or the American College of Cardiology. From the Falk Cardiovascular Research Center, Stanford University School of Medicine, Stanford, California.
What is responsible for the heterogeneity of vascular regeneration in PAD patients? An important clue has been provided by the work of Findley et al. (8) in this issue of the Journal. These investigators studied healthy control subjects and patients with peripheral arterial disease (PAD) manifested as intermittent claudication (IC) or as CLI. In these patients they measured plasma levels of proteins from 2 families of angiogenic growth factors, the vascular endothelial growth factors (VEGFs) and the angiopoietins (Ang). The vascular endothelial growth factors (VEGF-A, -B, -C, and -D, and placental growth factor) and the angiopoietins (Ang1 and -2) are major mediators of angiogenesis and lymphangiogenesis (9). The receptors for the VEGFs include VEGFR-1, -2, and -3, whereas the angiopoietin receptors include Tie1 and -2. The diversity of angiogenic factors and their receptors permits fine-tuning of the angiogenic response as new capillaries form and differentiate, and allows for specificity. The prototype member of the VEGF family is VEGF-A. The loss of a single allele of VEGF-A is embryonically lethal because of failure of hematopoiesis and vasculogenesis. VEGF-A has 4 isoforms, including the one analyzed in the Findley study, VEGF165. The various isoforms of VEGF induce endothelial cell proliferation, migration, and capillary tube formation. The angiopoietins are also neces-
Cooke Editorial Comment
JACC Vol. 52, No. 5, 2008 July 29, 2008:394–6
sary for angiogenesis, modulating endothelial cell migration, adhesion, and survival, acting through their endothelial receptor Tie2. Genetic disruption of Tie2 also results in embryonic lethality because of vascular defects (10). Findley et al. (8) noted higher plasma levels of the angiogenic cytokines Ang2 and VEGF in the PAD patients. Furthermore, plasma levels of VEGF were significantly greater in those with more severe disease, that is, in patients with CLI. The levels of Ang2 also tended to be higher in the CLI patients (the lack of statistical significance was likely a type II error because of insufficient numbers of patients in this small study). These findings are consistent with the notion that greater ischemia is associated with greater activation of the angiogenic response to hypoxia. Parenthetically, much of the hypoxic response is under the control of the transcriptional factor, hypoxia-inducible factor (HIF)-1␣. At low oxygen tension, HIF-1␣ is stabilized and can translocate to the nucleus to orchestrate the genetic response to ischemia, activating genes encoding angiogenic cytokines, metabolism, vasodilation, and cell survival (11). Endogenous Inhibitors of Angiogenesis
Of relevance to this study, it is known that the angiogenic receptors VEGFR-1 and Tie2 can be released by endothelial cells into the circulation. These solubilized receptors can still bind their respective growth factors. By scavenging VEGF or Ang, these soluble receptors may act as a brake on angiogenesis. The soluble receptors may represent a form of negative feedback, because VEGF is known to promote the endothelial shedding of Tie2 (12). Notably, overexpression of either of these soluble receptors in animal models inhibits tumor angiogenesis and tumor growth (13,14). The logical extension of these fundamental insights, a soluble VEGF receptor for inhibition of tumor angiogenesis and growth, is showing promise in early clinical trials (15). Could endogenous soluble receptors, scavenging angiogenic cytokines, play an adverse role in the angiogenic response to PAD? Intriguingly, Findley et al. (8) also observed an increase in the plasma levels of the soluble Ang receptor (sTie2) in the PAD patients. Furthermore, the plasma levels of sTie2 were highest in the most symptomatic patients. The greater elevation of sTie2 in the CLI patients remained after controlling for differences in CV risk factors or ABI. These findings suggest that increased levels of sTie2 correlate with the severity of disease, independently of the hemodynamic impairment. One might speculate that the elevation of the soluble receptor impairs the angiogenic response in these patients. To confirm this hypothesis, it would be useful to study a larger group of PAD patients, including asymptomatic to most symptomatic subjects. One would correlate plasma levels of the angiogenic cytokines and their soluble receptors to an angiographic assessment of collaterals, as well as capillary density in needle biopsies of calf muscle. Individuals with greater levels of the angiogenic cytokines and
395
lower levels of the soluble receptors would be expected to have a greater angiogenic response. New Insights Into Angiogenic Modulation
The notion that individual patients may have different responses to the same ischemic stimulus finds support in the coronary circulation. Recently, a genetic variant of HIF-1␣ has been described. Patients with coronary artery disease who also had this genetic variant were observed to have fewer coronary collateral vessels (16). Undoubtedly, other genetic factors will be found to play a role in the heterogeneity of vascular regeneration in response to ischemia. Indeed, the Duke group is continuing their hunt in C57Bl/6 mice, where a segment of chromosome 7 containing 37 genes confers resistance to limb loss after femoral artery ligation (17). One or more of these genes may be involved in the enhanced angiogenic response and superior perfusion observed in this strain of mice. Taken together, the translational studies of Findley et al. (8) will provide new clues to the mechanisms underlying impaired vascular regeneration in PAD, and may lead us to new therapeutic approaches to promote arteriogenesis and to enhance angiogenesis. Reprint requests and correspondence: Dr. John P. Cooke, Falk Cardiovascular Research Center, Stanford University School of Medicine, 300 Pasteur Drive, Stanford, California 94305-5406. E-mail: [email protected]. REFERENCES
1. Hirsch AT, Haskal ZJ, Hertzer NR, et al. ACC/AHA 2005 practice guidelines for the management of patients with peripheral arterial disease (lower extremity, renal, mesenteric, and abdominal aortic): a collaborative report from the American Association for Vascular Surgery/Society for Vascular Surgery, Society for Cardiovascular Angiography and Interventions, Society for Vascular Medicine and Biology, Society of Interventional Radiology, and the ACC/AHA Task Force on Practice Guidelines (Writing Committee to Develop Guidelines for the Management of Patients With Peripheral Arterial Disease). J Am Coll Cardiol 2006;47:e1–192. 2. Hirsch AT, Criqui MH, Treat-Jacobson D, et al. Peripheral arterial disease detection, awareness, and treatment in primary care. JAMA 2001;286:1317–24. 3. McDermott MM, Greenland P, Liu K, et al. Leg symptoms in peripheral arterial disease: associated clinical characteristics and functional impairment. JAMA 2001;286:1599 – 606. 4. Norgren L, Hiatt WR, Dormandy JA, et al. Inter-Society Consensus for the Management of Peripheral Arterial Disease (TASC II). J Vasc Surg 2007;45 Suppl S:S5– 67. 5. Szuba A, Oka RK, Harada R, Cooke JP. Limb hemodynamics are not predictive of functional capacity in patients with PAD. Vasc Med 2006;11:155– 63. 6. Brass EP, Hiatt WR, Green S. Skeletal muscle metabolic changes in peripheral arterial disease contribute to exercise intolerance: a pointcounterpoint discussion. Vasc Med 2004;9:293–301. 7. Ubbink DT, Spincemaille GH, Reneman RS, Jacobs MJ. Prediction of imminent amputation in patients with non-reconstructible leg ischemia by means of microcirculatory investigations. J Vasc Surg 1999;30:114 –21. 8. Findley CM, Mitchell RG, Duscha BD, Annex BH, Kontos CD. Plasma levels of soluble Tie2 and vascular endothelial growth factor distinguish critical limb ischemia from intermittent claudication in patients with peripheral arterial disease. J Am Coll Cardiol 2008;52: 387–93.
396
Cooke Editorial Comment
9. Kowanetz M, Ferrara N. Vascular endothelial growth factor signaling pathways: therapeutic perspective. Clin Cancer Res 2006;12:5018 –22. 10. Sato TN, Tozawa Y, Deutsch U, et al. Distinct roles of the receptor tyrosine kinase Tie-1 and Tie2 in blood vessel formation. Nature (Lond) 1995:376:70 – 4. 11. Semenza GL. Hypoxia-inducible factor (HIF-1) pathway. Sci STKE 2007;2007:cm8. 12. Findley CM, Cudmore MJ, Ahmed A, Kontos CD. VEGF induces Tie2 shedding via a phosphoinositide 3-kinase/Akt dependent pathway to modulate Tie2 signaling. Arterioscler Thromb Vasc Biol 2007; 27:2619 –26. 13. Siemeister G, Schirner M, Weindel K, et al. Two independent mechanisms essential for tumor angiogenesis: inhibition of human melanoma xenograft growth by interfering with either the vascular
JACC Vol. 52, No. 5, 2008 July 29, 2008:394–6
14. 15. 16. 17.
endothelial growth factor receptor pathway or the Tie-2 pathway. Cancer Res 1999;59:3185–91. Becker CM, Farnebo FA, Iordanescu I, et al. Gene therapy of prostate cancer with the soluble vascular endothelial growth factor receptor Flk1. Cancer Biol Ther 2002;1:548 –53. Riely GJ, Miller VA. Vascular endothelial growth factor trap in non small cell lung cancer. Clin Cancer Res 2007;13:s4623–7. Resar JR, Roguin A, Voner J, et al. Hypoxia-inducible factor 1alpha polymorphism and coronary collaterals in patients with ischemic heart disease. Chest;128:787–91. Dokun AO, Keum S, Hazarika S, et al. A quantitative trait locus (LSq-1) on mouse chromosome 7 is linked to the absence of tissue loss after surgical hindlimb ischemia. Circulation 2008;117: 1207–15.
EDITORIAL COMMENT
Critical Determinants of Limb Ischemia* John P. Cooke, MD, PHD, FACC Stanford, California
Peripheral arterial disease (PAD) involving the lower extremities affects 8 to 12 million Americans (1). Typically, PAD is secondary to atherosclerotic occlusive disease of the aortoiliac, femoral, popliteal, and/or the infrapopliteal arteries. The clinical manifestations depend in part on the level of disease and its severity. The classic symptom of intermittent claudication (pain with walking, relieved by rest) typically involves the calf, but the thigh and/or buttocks can be affected with more proximal arterial disease. Classic symptoms are only manifested by 10% to 30% of patients (2,3). More often, the patients are asymptomatic, or their symptoms are disguised by (or attributed to) associated diabetic neuropathy or musculoskeletal disorders, each of which are common in the demographic affected by PAD.
Vol. 52, No. 5, 2008 ISSN 0735-1097/08/$34.00 doi:10.1016/j.jacc.2008.05.004
the pressure at the arm), with functional capacity as assessed by treadmill testing (5). This heterogeneity may be in part due to individual differences in the response of the skeletal muscle to ischemia. For example, the expression and activity of key mitochondrial enzymes are altered in skeletal muscle from PAD patients, and mitochondrial electron transport is impaired (6). Metabolic byproducts of fatty acid oxidation, the acylcarnitines, accumulate in both the plasma and the skeletal muscle of patients with PAD, and are strongly correlated with impairment in exercise capacity (6). The vascular response to conduit vessel occlusion also seems to be subject to individual variation. Measures of skin microcirculation have been used prospectively to predict amputation in CLI patients with unreconstructable vascular disease (7). In patients with reduced skin capillary density (⬍20/mm2), low transcutaneous oxygen (TcPO2 ⬍10 mm Hg), and absent reactive hyperemia, limb survival at 1 year was only 15%, compared with 88% in CLI patients with greater values for the skin microcirculation. Furthermore, it is widely recognized that collateral vessel formation is heterogeneous in patients with the same degree of conduit vessel obstruction. In 1 patient with a superficial femoral artery occlusion, robust collateral formation (arteriogenesis) via the deep femoral artery and geniculate collaterals will revascularize the infrapopliteal vessels. The patient may have minimal or no symptoms. Another patient will be significantly limited by the same occlusive disease, in a setting of sparse collateral formation.
See page 387
Regulation of Angiogenesis
A more severe form of PAD is characterized by pain at rest (typically in the foot, occurring often at night, and relieved by dependency). These individuals have a limb in jeopardy, and the most minor trauma (from a poorly fitting shoe, or a carelessly clipped toenail) can result in a nonhealing wound, infection, and amputation. This form of PAD is known as critical limb ischemia, and affects about 10% of PAD patients. Critical limb ischemia (CLI) is a mortal illness: at 1 year after presentation, 30% have suffered an amputation and 25% of patients are dead (4). Why Are There Differences in the Clinical Presentation of PAD?
Although hemodynamically significant obstructions of the conduit arteries play an acknowledged role in the manifestations of PAD, there is considerable heterogeneity in the degree of symptoms. Furthermore, there is only a modest correlation of hemodynamic assessments, such as the anklebrachial index (ABI) (the pressure at the ankle divided by *Editorials published in the Journal of the American College of Cardiology reflect the views of the authors and do not necessarily represent the views of JACC or the American College of Cardiology. From the Falk Cardiovascular Research Center, Stanford University School of Medicine, Stanford, California.
What is responsible for the heterogeneity of vascular regeneration in PAD patients? An important clue has been provided by the work of Findley et al. (8) in this issue of the Journal. These investigators studied healthy control subjects and patients with peripheral arterial disease (PAD) manifested as intermittent claudication (IC) or as CLI. In these patients they measured plasma levels of proteins from 2 families of angiogenic growth factors, the vascular endothelial growth factors (VEGFs) and the angiopoietins (Ang). The vascular endothelial growth factors (VEGF-A, -B, -C, and -D, and placental growth factor) and the angiopoietins (Ang1 and -2) are major mediators of angiogenesis and lymphangiogenesis (9). The receptors for the VEGFs include VEGFR-1, -2, and -3, whereas the angiopoietin receptors include Tie1 and -2. The diversity of angiogenic factors and their receptors permits fine-tuning of the angiogenic response as new capillaries form and differentiate, and allows for specificity. The prototype member of the VEGF family is VEGF-A. The loss of a single allele of VEGF-A is embryonically lethal because of failure of hematopoiesis and vasculogenesis. VEGF-A has 4 isoforms, including the one analyzed in the Findley study, VEGF165. The various isoforms of VEGF induce endothelial cell proliferation, migration, and capillary tube formation. The angiopoietins are also neces-
Cooke Editorial Comment
JACC Vol. 52, No. 5, 2008 July 29, 2008:394–6
sary for angiogenesis, modulating endothelial cell migration, adhesion, and survival, acting through their endothelial receptor Tie2. Genetic disruption of Tie2 also results in embryonic lethality because of vascular defects (10). Findley et al. (8) noted higher plasma levels of the angiogenic cytokines Ang2 and VEGF in the PAD patients. Furthermore, plasma levels of VEGF were significantly greater in those with more severe disease, that is, in patients with CLI. The levels of Ang2 also tended to be higher in the CLI patients (the lack of statistical significance was likely a type II error because of insufficient numbers of patients in this small study). These findings are consistent with the notion that greater ischemia is associated with greater activation of the angiogenic response to hypoxia. Parenthetically, much of the hypoxic response is under the control of the transcriptional factor, hypoxia-inducible factor (HIF)-1␣. At low oxygen tension, HIF-1␣ is stabilized and can translocate to the nucleus to orchestrate the genetic response to ischemia, activating genes encoding angiogenic cytokines, metabolism, vasodilation, and cell survival (11). Endogenous Inhibitors of Angiogenesis
Of relevance to this study, it is known that the angiogenic receptors VEGFR-1 and Tie2 can be released by endothelial cells into the circulation. These solubilized receptors can still bind their respective growth factors. By scavenging VEGF or Ang, these soluble receptors may act as a brake on angiogenesis. The soluble receptors may represent a form of negative feedback, because VEGF is known to promote the endothelial shedding of Tie2 (12). Notably, overexpression of either of these soluble receptors in animal models inhibits tumor angiogenesis and tumor growth (13,14). The logical extension of these fundamental insights, a soluble VEGF receptor for inhibition of tumor angiogenesis and growth, is showing promise in early clinical trials (15). Could endogenous soluble receptors, scavenging angiogenic cytokines, play an adverse role in the angiogenic response to PAD? Intriguingly, Findley et al. (8) also observed an increase in the plasma levels of the soluble Ang receptor (sTie2) in the PAD patients. Furthermore, the plasma levels of sTie2 were highest in the most symptomatic patients. The greater elevation of sTie2 in the CLI patients remained after controlling for differences in CV risk factors or ABI. These findings suggest that increased levels of sTie2 correlate with the severity of disease, independently of the hemodynamic impairment. One might speculate that the elevation of the soluble receptor impairs the angiogenic response in these patients. To confirm this hypothesis, it would be useful to study a larger group of PAD patients, including asymptomatic to most symptomatic subjects. One would correlate plasma levels of the angiogenic cytokines and their soluble receptors to an angiographic assessment of collaterals, as well as capillary density in needle biopsies of calf muscle. Individuals with greater levels of the angiogenic cytokines and
395
lower levels of the soluble receptors would be expected to have a greater angiogenic response. New Insights Into Angiogenic Modulation
The notion that individual patients may have different responses to the same ischemic stimulus finds support in the coronary circulation. Recently, a genetic variant of HIF-1␣ has been described. Patients with coronary artery disease who also had this genetic variant were observed to have fewer coronary collateral vessels (16). Undoubtedly, other genetic factors will be found to play a role in the heterogeneity of vascular regeneration in response to ischemia. Indeed, the Duke group is continuing their hunt in C57Bl/6 mice, where a segment of chromosome 7 containing 37 genes confers resistance to limb loss after femoral artery ligation (17). One or more of these genes may be involved in the enhanced angiogenic response and superior perfusion observed in this strain of mice. Taken together, the translational studies of Findley et al. (8) will provide new clues to the mechanisms underlying impaired vascular regeneration in PAD, and may lead us to new therapeutic approaches to promote arteriogenesis and to enhance angiogenesis. Reprint requests and correspondence: Dr. John P. Cooke, Falk Cardiovascular Research Center, Stanford University School of Medicine, 300 Pasteur Drive, Stanford, California 94305-5406. E-mail: [email protected]. REFERENCES
1. Hirsch AT, Haskal ZJ, Hertzer NR, et al. ACC/AHA 2005 practice guidelines for the management of patients with peripheral arterial disease (lower extremity, renal, mesenteric, and abdominal aortic): a collaborative report from the American Association for Vascular Surgery/Society for Vascular Surgery, Society for Cardiovascular Angiography and Interventions, Society for Vascular Medicine and Biology, Society of Interventional Radiology, and the ACC/AHA Task Force on Practice Guidelines (Writing Committee to Develop Guidelines for the Management of Patients With Peripheral Arterial Disease). J Am Coll Cardiol 2006;47:e1–192. 2. Hirsch AT, Criqui MH, Treat-Jacobson D, et al. Peripheral arterial disease detection, awareness, and treatment in primary care. JAMA 2001;286:1317–24. 3. McDermott MM, Greenland P, Liu K, et al. Leg symptoms in peripheral arterial disease: associated clinical characteristics and functional impairment. JAMA 2001;286:1599 – 606. 4. Norgren L, Hiatt WR, Dormandy JA, et al. Inter-Society Consensus for the Management of Peripheral Arterial Disease (TASC II). J Vasc Surg 2007;45 Suppl S:S5– 67. 5. Szuba A, Oka RK, Harada R, Cooke JP. Limb hemodynamics are not predictive of functional capacity in patients with PAD. Vasc Med 2006;11:155– 63. 6. Brass EP, Hiatt WR, Green S. Skeletal muscle metabolic changes in peripheral arterial disease contribute to exercise intolerance: a pointcounterpoint discussion. Vasc Med 2004;9:293–301. 7. Ubbink DT, Spincemaille GH, Reneman RS, Jacobs MJ. Prediction of imminent amputation in patients with non-reconstructible leg ischemia by means of microcirculatory investigations. J Vasc Surg 1999;30:114 –21. 8. Findley CM, Mitchell RG, Duscha BD, Annex BH, Kontos CD. Plasma levels of soluble Tie2 and vascular endothelial growth factor distinguish critical limb ischemia from intermittent claudication in patients with peripheral arterial disease. J Am Coll Cardiol 2008;52: 387–93.
396
Cooke Editorial Comment
9. Kowanetz M, Ferrara N. Vascular endothelial growth factor signaling pathways: therapeutic perspective. Clin Cancer Res 2006;12:5018 –22. 10. Sato TN, Tozawa Y, Deutsch U, et al. Distinct roles of the receptor tyrosine kinase Tie-1 and Tie2 in blood vessel formation. Nature (Lond) 1995:376:70 – 4. 11. Semenza GL. Hypoxia-inducible factor (HIF-1) pathway. Sci STKE 2007;2007:cm8. 12. Findley CM, Cudmore MJ, Ahmed A, Kontos CD. VEGF induces Tie2 shedding via a phosphoinositide 3-kinase/Akt dependent pathway to modulate Tie2 signaling. Arterioscler Thromb Vasc Biol 2007; 27:2619 –26. 13. Siemeister G, Schirner M, Weindel K, et al. Two independent mechanisms essential for tumor angiogenesis: inhibition of human melanoma xenograft growth by interfering with either the vascular
JACC Vol. 52, No. 5, 2008 July 29, 2008:394–6
14. 15. 16. 17.
endothelial growth factor receptor pathway or the Tie-2 pathway. Cancer Res 1999;59:3185–91. Becker CM, Farnebo FA, Iordanescu I, et al. Gene therapy of prostate cancer with the soluble vascular endothelial growth factor receptor Flk1. Cancer Biol Ther 2002;1:548 –53. Riely GJ, Miller VA. Vascular endothelial growth factor trap in non small cell lung cancer. Clin Cancer Res 2007;13:s4623–7. Resar JR, Roguin A, Voner J, et al. Hypoxia-inducible factor 1alpha polymorphism and coronary collaterals in patients with ischemic heart disease. Chest;128:787–91. Dokun AO, Keum S, Hazarika S, et al. A quantitative trait locus (LSq-1) on mouse chromosome 7 is linked to the absence of tissue loss after surgical hindlimb ischemia. Circulation 2008;117: 1207–15.