Young Vasospastic Angina Patients Less Than 20 Years Old

Shozo Sueda

doi:10.1253/circj.CJ-19-0433

Abstract

Background: Japanese Circulation Society (JCS) guidelines do not include adolescents with coronary artery spasm.

Methods and Results: We recruited 18 adolescents less than 20 years old with vasospastic angina (VSA): 11 were Japanese and 3 had chest symptoms for >12 months before admission. ST-segment elevation was observed in 11 patients and none of the 18 patients had a fixed stenosis. Spasm provocation tests were performed in 9 patients and two-thirds had multiple spasms; 6 suffered from acute myocardial infarction and ventricular fibrillation occurred in 2 patients; 1 patient died and the remaining 17 patents survived.

Conclusions: Clinical status of adolescents with VSA was as severe as in adults with refractory VSA. Cardiologists should cooperate with pediatricians to diagnose and treat adolescents with VSA. There is a need to establish the additional issues for adolescents with coronary spasm in the JCS guidelines.

Coronary artery spasm may be involved in the pathogenesis of various cardiac diseases such as sudden cardiac death, acute myocardial infarction, fatal arrhythmias, heart failure, angina pectoris, atypical chest pain and other disorders.¹^–⁵ The majority of patients with vasospastic angina (VSA) are older than 50 or 60 years, but occasionally adolescents present with VSA in the clinic. However, the particular issues of adolescent VSA are not covered by the Japanese Circulation Society (JCS) guidelines.⁶

Therefore, we recruited patients less than 20 years old with VSA and investigated their real-world data.

Methods

We recruited the data for 18 patients less than 20 years old with VSA reported in the PubMed database;⁷^–²¹ As shown in Table 1, 11 were less than 15 years old; 10 were male and 8 were female; 11 patients were Japanese, and the other 7 patients were included 3 Americans, 1 Turk and 1 Chinese. None of the 18 patients had hypertension or diabetes mellitus/dyslipidemia. Coronary artery stenosis was not found in any of the 18 patients.

Table 1. Clinical Characteristics of Patients Less Than 20 Years Old With Vasospastic Angina

No.	Author (Year)	Age (years)	Sex	Race	Family history	Onset (months)	Chief complaint	Passive smoking	Effort/rest	Timing	Duration (min)	ECG
1	Wilkes (1985)¹⁶	11	M	American black	No	6	Chest P	UC	Rest	UC	0.5–3	ST ele in V1–3, aVR, aVL
2	Ivy (1994)¹⁴	16	M	American of Spanish	No	Sudden	Chest P	UC	Rest	Daytime	60	ST ele in II, III, aVF, V5–6
3	Hosoi (1997)¹¹	13	M	Japanese	HCM	4	Chest OP	UC	Effort	Daytime	5	ST ele in aVL, V1–5
4	Fukuda (2003)¹³	13	F	Japanese	No	Sudden	CPA	UC	Effort	Daytime	UC	Anteroseptal ischemia
5	Flohr	18	F	UC	IHD	Sudden	UC	UC	UC	UC	UC	UC
6	Karaaslan (2003)¹⁷	16	M	Turk	No	Sudden	Chest P	UC	Rest	Nighttime	60	ST ele in V5–6
7	Kobayashi (2003)¹⁵	16	F	Japanese	VSA, KD, sudden death	Sudden	Chest OP	UC	Rest/Effort	Daytime/nighttime	2–3	No abnormality
8	Li (2005)¹⁸	17	M	Chinese	No	Sudden	Chest P	UC	UC	UC	UC	ST ele in II, III, aVF
9	Jefferies (2005)¹⁹	13	F	American	No	Sudden	Chest P	UC	UC	UC	UC	ST ele in II, III, aVF
10	Hasegawa (2005)¹⁰	13	M	Japanese	VT	Sudden	CPA	UC	Effort	Daytime	UC	ST ele in aVR, V1–3
11	Okajima (2007)¹²	13	F	Japanese	No	36	Toothache	UC	UC	Daytime	UC	UC
12	Lim (2007)	6	M	UC	AMI DL	Sudden	UC	UC	UC	UC	UC	Ischemia positive
13	Mori (2008)²⁰	14	M	Japanese	No	Sudden	Chest OP	UC	Rest	Daytime (06:00 hours)	150	ST ele in I, aVL, V4–6
14	Mori (2008)²⁰	11	F	Japanese	No	Sudden	Chest P	UC	Rest	Nighttime (05:00 hours)	180	ST ele in V2–3
15	Odanaka (2011)²¹	14	F	Japanese	No	Sudden	Chest P	UC	Rest	Daytime (06:00/12:00/15:00 hours)/ nighttime	10–30	ST ele in II, III, aVF, V3–6
16	Sueda (2013)⁸	15	F	Japanese	No	24	Chest OP	UC	Rest	Nighttime	5	ST ele in II, III, aVF
17	Sueda (2013)⁷	13	M	Japanese	No	12	Chest OP	Yes	Rest/Effort	Daytime/Nighttime	5–10	No abnormality
18	Yamaguchi (2019)⁹	17	M	Japanese	No	Sudden	Dyspnea	No	Effort	Daytime	UC	ST dep in III, aVF

AMI, acute myocardial infarction; Chest P, chest pain; Chest OP, chest oppression; CPA, cardiopulmonary arrest; DL, dyslipidemia; HCM, hypertrophic cardiomyopathy; IHD, ischemic heart disease; KD, Kawasaki disease; ST ele, ST elevation; ST dep, ST depression; UC, uncertain; VSA, vasospastic angina.

Duration of VSA Before Admission

Sudden onset occurred in 13 patients, who had emergency admission by ambulance, and 5 patients had a history of chest symptoms before admission; 3 patients had chest symptoms for more than 12 months. The longest duration of chest symptoms before diagnosis was 36 months.

Chief Complaint

Chest pain or chest oppression was the chief complaint in 12 patients and cardiopulmonary arrest was the first event in 2 patients. In 1 case the patient only had toothache without chest symptoms and another patient had dyspnea on effort without chest pain or oppression.

Passive Smoking

In 1 case the patient had an obvious passive smoking history because both parents had a history of smoking for more than 18 years, even at home. Another patient did not have a history of passive smoking, but we could not obtain definitive history of passive smoking for the remaining 16 patients (Table 1).

Time and Duration of Chest Pain

Chest symptoms occurred at rest in 7 patients, 4 patients complained of chest symptoms on effort and 2 patients had chest symptoms both at rest and on effort. Chest pain occurred in the daytime in 7 patients, 3 patients complained of chest pain at nighttime, and 3 patients had chest pain attacks both day and night. The duration of chest pain was a few minutes to 3 h; 5 patients had <10 min of angina whereas 4 patents had >60 min of chest pain.

ECG Findings on Admission

Ischemic ECG changes were observed in 14 patients, ST-segment elevation was observed in 11 patients, and 1 patient had ST-segment depression on admission. Ischemic ECG changes in inferior leads were recognized in 6 patients, and anterolateral ischemia was found in 9 patients.

Elevation of Cardiac Enzymes and Wall Motion Abnormality

As shown in Table 2, elevated creatine phosphokinase (CPK) was detected in 8 patients, 1 patient had positive troponin T and 1 patient had elevated troponin I. Maximum elevated CPK <1,000 IU/L was found in 4 of 8 patients, and 1 patient had >10,000 IU/L CPK. Left ventricular wall motion abnormality was found in 6 patients, but 7 patients had no decreased left ventricular wall motion.

Table 2. Clinical Characteristics and Angiographic Findings in Patients Less Than 20 Years Old With Vasospastic Angina

No.	Cardiac enzymes	UCG	CAG	ACh/ER	Spasm	Alive/dead	Medication	Complications
1	Normal	Septal akinesia	Normal	Not done	UC	Alive	Nifedipine 10 mg (3 months)	Angina-free for 14 months
2	CPK 349 IU/L	Normal	Normal	Not done	UC	Alive	Nifedipine/ isosorbide dinitrate	None
3	CPK 11,690 IU/L	Anterolateral akinesis	Normal	ACh (L 100)	LAD (90)/ LCX (95)	Alive	UC	AMI, VF, DC, IABP, PCPS
4	UC	UC	Normal	ACh	LAD/LCX	Alive	UC	AMI, CPA, eNOS abnormality
5	UC	UC	UC	UC	Positive	Alive	UC	AMI, VSA
6	CPK 905 IU/L	Normal	Normal	Not done	UC	Alive	Verapamil 4 mg/kg	AMI, Ca-67
7	Normal	Anterolateral hypo LVG	Normal	ACh (L 100)	LAD (d)	Alive	Ca unknown (20 months)	Angina-free for 20 months
8	Normal	Normal	Normal	Not done	UC	Alive	Ca/nitrate	None
9	Troponin I elevated	UC	Normal	Not done	UC	Alive	UC	None
10	Normal	LVH (apex)	Normal	ACh (L 50/R 50)	RCA (d)/LAD (d)/LCX (d)	Alive	Ca/vasodilator/ statin	VF, DC
11	UC	Lateral OMI on autopsy	No stenosis	Not done	UC	Dead	None	Marked intimal hyperplasia
12	CPK/CK-MB elevated	UC	Normal	Not done	UC	Alive	UC	None
13	CPK 1,815 IU/L	Normal	Normal	Not done	Dilated after ISDN	Alive	UC	None
14	Troponin T positive	Normal	Normal	ACh (L 50/R 50)	LAD (d)	Alive	UC	None
15	CPK 1,050 IU/L	Normal	Normal	ACh (L 50)	LAD (d)/ LCX (d)	Alive	Ca	AMI
16	CPK 407 IU/L	Normal	Normal	ACh (R 50/L 100)	8 (d)	Alive	Ca	AMI
17	Normal	Diffuse hypo %FS 28	Normal	ACh/ER/ERACh	RCA (d)/LAD (d)/LCX (d)	Alive	Diltiazem R 100 mg/ nifedipine CR 20 mg	None
18	CPK 408 IU/L	Decreased EF 60%	Normal	ACh (R 25/L 50)	RCA (d)/LAD (d)/LCX (d)	Alive	Benidipine 2 mg/ isosorbide mononitrate 20 mg/ nicorandil 15 mg	Decreased LV

ACh, acetylcholine; AMI, acute myocardial infarction; Ca, calcium-channel antagonist CAG, coronary arteriography; CPA, cardiopulmonary arrest; CPK, creatinine phosphokinase; (d), diffuse spasm; DC, direct current; EF, ejection fraction; eNOS; endothelial nitric oxide synthase gene; ER, ergonovine; FS, fractional shortening; Ga, gadolinium; IABP, intra-aortic balloon pumping; L, left; LAD, left anterior descending artery; LCX, left circumflex artery; LVH, left ventricular hypertrophy; OMI, old myocardial infarction; PCPS, percutaneous cardiopulmonary support; VF, ventricular fibrillation; VSA, vasospastic angina; R, right; RCA, right coronary artery; UC, uncertain; UCG, ultracardiography.

Spasm Provocation Tests

Spasm provocation tests were performed in 9 Japanese patients, but not in the other 11 patients. Intracoronary administration of acetylcholine (ACh) provoked diffuse spasm in all 9 patients. Both right and left coronary artery spasm provocation tests were performed in 5 patients. Multiple spasms occurred in 6 of 9 patients, and 3 patients had triple vessel spasm.

Medications

Calcium-channel antagonists were administered to 10 patients (2 for 1 patient; 1 for 9 patients), 4 patients had another vasodilator and there was no precise description of medications for the remaining 7 patients. Nitrates were administered to 2 patients.

Complications and Prognosis

In 6 cases the patient suffered from acute myocardial infarction and ventricular fibrillation occurred in 2 patients. Direct current was necessary to recover sinus rhythm for 2 patients. As cardiopulmonary support, intra-aortic balloon pumping and percutaneous cardiopulmonary support were necessary for 1 rescue patient. Endothelial nitric oxide synthase gene abnormality was found in 1 patient (case no. 4, Table 2): T⁻⁷⁸⁶→C, A⁻⁹²²→G, and T⁻¹⁴⁶⁸→A mutations in the 5′-flanking region on 1 allele. Overall, 1 patient died but the remaining 17 patients survived.

Discussion

Here we summarize the clinical data for adolescents less than 20 years old with VSA. A total of 6 patients had AMI and 1 patient died. In all 18 cases, a severe clinical state similar to refractory adulthood VSA was observed in the past. Cardiologists should cooperate with pediatricians to establish the diagnosis and treatment of adolescents with VSA.

Pitfalls of Spasm in Adolescents

If adolescent patients complain of chest pain, pediatricians and cardiologists may suspect mitral valve prolapse, myocarditis, or atypical chest pain. Although coronary artery spasm is involved in the pathogenesis of chest pain even in adolescents, we may infrequently encounter these young VSA patients. In this study, the majority of adolescents complained of chest pain or chest oppression, but cardiopulmonary arrest was the first attack in 2 adolescents, another complained just of toothache without chest symptoms and another patient had dyspnea on effort. Pediatricians and cardiologists should consider coronary artery spasm when an adolescent less than 20 years old complains of chest pain. Furthermore, cardiologists and pediatricians should question the adolescent’s condition precisely.

Spasm Provocation Testing in Adolescents

Spasm provocation tests are necessary to diagnose the presence of coronary artery spasm in the clinic. We used the dose of pharmacological agents recommended in the JCS guidelines. When we perform ACh testing, we inject an incremental ACh dose of 20/50/100 μg into the left coronary artery and 20/50 μg into the right coronary artery. Furthermore, the JCS guidelines recommend continuous administration of ergonovine (ER), not bolus injection. Cardiologists perform ACh or ER testing when diagnosing adult patients with VSA, whereas pediatricians are not familiar with performing these spasm provocation tests in the clinic. Pediatricians should perform these spasm provocation tests with trained cardiologists. The optimal maximum dose of ACh or ER in adolescents needs to be determined in order to perform the spasm provocation tests without irreversible complications.

Medications

Spontaneous remission is rarely observed in patients with VSA and sudden cardiac death can occur after self-cessation of medications by some with adult VSA patients. Medications including vasodilators in adolescents with coronary spasm will be life-long. However, we did not find a clinical course longer than 30 or 40 years periods for adolescents with VSA. Cardiologists should corroborate with pediatricians to ensure good quality of life and excellent outcomes for adolescents with VSA.

Adolescents With Coronary Spasm in the Future

Cardiologists and pediatricians should investigate coronary artery spasm in adolescents in the clinic, because coronary abnormal response has increased in Japanese patients,²² possibly with the widespread occurrence of metabolic syndrome, which has increased all over the world, even in adolescents.

Nakayama et al reported that the T⁻⁷⁸⁶→C mutation in the 5′-flanking region of the endothelial nitric oxide synthase (eNOS) gene was associated with coronary spasm.²³ We found 1 patient with that mutation. Genetic analysis including eNOS may help diagnose adolescents with VSA in the future. Cardiologists should also campaign to protect adolescents from secondhand smoke. Furthermore, many adolescents with non-variant angina or low disease activity VSA could be present clinically, so collaboration between pediatricians and cardiologists is essential for successfully treating adolescents with VSA in Japan.

Funding

None.

Conflicts of Interest

The authors declare that they have no conflicts of interest.

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