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Revista mexicana de neurociencia

versión On-line ISSN 2604-6180versión impresa ISSN 1665-5044

Rev. mex. neurocienc. vol.22 no.1 Ciudad de México ene./feb. 2021  Epub 23-Abr-2021

https://doi.org/10.24875/rmn.20000021 

Original article

Wallenberg syndrome and isolated lateral bulbar infarction: Clinical characteristics and prognosis in a cohort of Mexican patients

Síndrome de Wallenberg e infarto bulbar lateral aislado: características clínicas y pronóstico en una cohorte de pacientes mexicanos

José L. Ruiz-Sandoval1  2  * 

Fernando Barinagarrementeria-Aldatz3 

Carlos Cantú-Brito4 

Antonio Arauz-Góngora5 

Germán López-Valencia1 

Amado Jiménez-Ruiz4 

Patricia Laguna-Cruz5 

Jesús A. Aldana López1 

Sergio Cerpa-Cruz1 

Christian Menchaca-Gutiérrez1 

1Department of Neurology, Hospital Civil de Guadalajara “Fray Antonio Alcalde”, Guadalajara, Jalisco, Mexico

2Department of Neurology, Instituto de Neurociencias Traslacionales, Centro Universitario de Ciencias de la Salud, Universidad de Guadalajara, Guadalajara, Jalisco, Mexico

3Department of Neurology, Hospital Ángeles, Querétaro, Querétaro; Jalisco, Mexico

4Department of Neurology, Instituto Nacional de Ciencias Médicas y Nutrición “Salvador Zubirán”, Mexico City; Ciudad de México; Mexico

5Clinic for Cerebral Vascular Disease, Instituto Nacional de Neurología y Neurocirugía “Manuel Velasco Suárez”, Mexico City; Mexico


Abstract

Background:

Wallenberg syndrome (WS) is a classic neurologic disorder secondary to vascular pathology of the vertebrobasilar circulation.

Methods:

Consecutive patients > 18 years with WS and isolated lateral medullary infarction syndrome were included from two Mexican hospitals. Risk factors, initial signs, symptoms, radiological findings, and acute treatment were evaluated; the prognosis was assessed using the Glasgow Outcome Scale.

Results:

Twenty-six patients were studied in a 26-year period (1988-2014); 17 patients were men (67%); and the average age was 45 years (range 19-77). Fourteen patients were under 45 years old (54%). The most common risk factors were dyslipidemia (41%) and hypertension (37%). The main initial symptoms were vertigo-dizziness (89%) gait ataxia (70%), and crossed-sensory deficit; and the main signs were crossed-sensitive deficit (93%), Horner syndrome (85%), and nystagmus (82%). In the bivariate analysis, age under 45 years was associated with a vertebral arterial dissection (p = 0.001), and age > 45 with atherothrombotic etiology (p = 0.01). About 96% of patients presented good recovery at an average of 17 months follow-up.

Conclusion:

Non-atherosclerotic vasculopathy was the main cause of WS-ILBI in young people. The clinical characteristics were similar to those reported in other series with a usually benign prognosis.

Key words Postero-lateral bulbar infarct; Stroke; Vertebral artery dissection; Wallenberg’s syndrome

Resumen

Antecedentes:

El síndrome de Wallenberg (SW) es un diagnóstico clásico en neurología, generalmente secundario a patología vascular de la circulación vertebro-basilar.

Métodos:

Se incluyeron a pacientes mexicanos consecutivos mayores de 18 años de edad con síndrome de SW e infarto bulbar lateral aislado (SW-IBLA) en dos hospitales mexicanos. Se evaluaron los factores de riesgo, signos y síntomas iniciales, hallazgos radiológicos, tratamiento agudo y pronóstico mediante el Glasgow Outcome Scale (GOS).

Resultados:

Se estudiaron 26 pacientes en un periodo de 26 años (1988-2014); Diecisiete pacientes fueron hombres (67%); el promedio de edad fue de 45 años (rango 19-77). Catorce pacientes fueron menores de 45 años (54%). Los factores de riesgo más frecuentes fueron dislipidemia (41%) e hipertensión arterial (37%). Los principales síntomas al inicio fueron vértigo-mareo (89%) y ataxia para la marcha (70%), así como déficit sensorial cruzado (93%), síndrome de Horner (85%) y nistagmo (82%) a la exploración neurológica. En el análisis bivariado, la edad menor a 45 años se asoció a disección arterial vertebral (p = 0.001), y la edad > 45 a etiología aterotrombótica (p = 0.01). El 96% de los pacientes presentaron buena recuperación en un seguimiento promedio de 17 meses.

Conclusión:

La vasculopatía no ateroesclerosa fue la principal causa de SW-IBLA en jóvenes. Las características clínicas para esta localización fueron similares a lo reportado en otras series con un pronóstico habitualmente benigno.

Palabras clave Circulación vertebro-basilar; Disección arterial vertebral; Enfermedad vascular cerebral; Ictus; Infarto bulbar; Síndrome de Wallenberg

Introduction

Twenty percent of brain infarctions occur in the vertebrobasilar territory, usually affecting the medulla1-3. In bulbar infarctions, the lateral or posterolateral topography is mainly compromised, causing a constellation of signs and symptoms encompassed in the Wallenberg syndrome (WS)4-7. The WS has been described throughout history from various perspectives. It began with clinical and clinical-pathological descriptions, followed by neurophysiological studies, as well as vascular findings (due to the use of cerebral angiography), culminating in precise clinical-radiological correlates after the advent of sophisticated magnetic resonance imaging (MRI)8,9. The prognosis for WS is usually favorable, and the sequelae, although frequent, are usually mildly disabling with complete remission in most cases9-11. We describe the clinical, radiological, and prognostic findings in a cohort of Mexican patients with WS and isolated lateral bulbar infarction (WS-ILMI) in two consecutive hospital records.

Patients and methods

Consecutive patients older than 18 years with WS confirmed with MRI admitted to the Neurology Department of the Instituto Nacional de Neurología y Neurocirugía “Manuel Velasco Suárez” (Mexico City, Mexico) from 1988 to 1998 were considered, as well as those admitted to the Neurology and Neurosurgery Department of the Hospital Civil de Guadalajara “Fray Antonio Alcalde” (Guadalajara, Jalisco, Mexico) from 1999 to 2014. Acute, ambulatory cases with these same diagnostic criteria attended in the outpatient clinic were also included in both cohorts. Socio-demographic variables, risk factors for stroke, symptoms at the onset of the infarct, and clinical signs on neurological examination, as well as antithrombotic management in the acute phase and secondary prevention strategies, were also analyzed.

Medullary infarctions were classified according to their location as rostral, caudal o rostrocaudal using MRI (FLAIR/DWI in the most recent cohort). Cerebral angiography, extracranial or transcranial Doppler of vertebrobasilar territory as well as magnetic resonance angiography (MRA) of the brain – individually or in combination – were considered to define the site of vascular stenosis or occlusion: vertebral, basilar, or the posteroinferior cerebellar artery (PICA).

The clinical condition at discharge was evaluated according to the Glasgow Prognostic Scale (GOS), where 1 = death; 2 = persistent vegetative state, without evident cortical activity; 3 = severe disability, with dependency; 4 = moderate disability in which he is independent but unable to return to his trade; and 5 = good recovery, returning to previous activities12. During outpatient follow-up, the clinical condition and sequelae in the last evaluation were recorded. Likewise, two age groups were considered: a young group (< 45 years) and an older group (> 45 years). For the registry of the information regarding clinical, radiological, therapeutic, and prognostic data, the same format was used for all patients.

Demographic data are presented as simple relative frequencies. Age is presented and analyzed as median with minimum and maximum. Pearson’s × 2 or Fisher’s test was used for nominal variables in the univariate analysis, when values with n > 5, or n < 5 were distributed in the boxes of the contingency tables, respectively. The T-student test was used to compare normally distributed continuous variables, and the Mann–Whitney U-test was performed when an ordinal or non-parametric numerical variable was distributed between two groups (e.g., comparison of medians). The analyses with p < 0.05 were considered significant. The analyses and “p” value were calculated at two tails. All cases were captured for analysis in the SPSS Statistics Bass 20.0 program (IBM SPSS Inc. Chicago, IL). Ethics Committees were aware of the study and agreed to its development.

Results

A total of 73 patients with “medullary infarction,” “medullary-cerebellar infarction,” or “WS” were initially considered. Of these, 36 patients were excluded: ten due to cerebellar involvement, six because they had simultaneously affected multiple structures of the vertebrobasilar territory, and another 13 because they corresponded to medullary infarcts of anteromedial (2 cases) or postero, and posterolateral (11 cases) location. Sixteen cases were excluded due to incomplete clinical or radiological information. Twenty-six patients with WS-IBLI were included for the present analysis.

Of the total of 26 patients, 17 (65%) were men and 9 (35%) women with an average age of 44 years (range of 19-77 years). There were 14 (54%) young patients (younger than 45 years). The main risk factors were: dyslipidemia (42%), high blood pressure (38%), alcoholism (35%), and smoking (27%). Two patients (8%) had a history of ischemic stroke in another territory (Table 1). According to the location of the WS-IBLI, 18 (69%) were caudal, five (19%) rostral, and three (12%) rostrocaudal.

The most frequent symptoms at WS-IBLI presentation were: vertigo or dizziness (92%), gait ataxia (77%), headache (73%), dysphagia (65%), and body (62%) or facial (58%) hypoesthesia (Table 2), with no significant differences regarding sex or age groups. According to location, dysphagia and dysarthria were less frequent in WS-IBLI with caudal location (all with p < 0.05). Facial hypoesthesia was more common in infarcts with a caudal location, while facial paralysis was more frequently documented in those with a rostrocaudal location.

Table 1 General characteristics of patients with Wallenberg syndrome and isolated medullary infarction (WS-IBLI) n = 26 

N S/A Risk factors Etiology Topography (MRI) Arterial findings Treatment Follow-up (M) Sequelae (GOS)
1 M/36 Alcohol Spontaneous dissection C-L- Right A: V4 Right occlusion. Aspirin 72 Facial pain (GOS) = 4
2 M/29 ---- Spontaneous dissection C-L- Right A-MRI: V3 Right Anticoagulation 12 Facial hypoesthesia (GOS) = 5
3 F/40 AH, Dyslip. Spontaneous dissection C-L- Right D: V3 Right stenosis A (2 month) normal. Aspirin 2 Horner/Nystagmus (GOS) = 4
4 M/33 Alcohol, Dyslip, Migraine Spontaneous dissection C-L- Right A: V3-4 Right stenosis and ACPI occlusion Aspirin 22 No (GOS) = 5
5 M/46 Sm, Alcohol, PCD Traumatic dissection C-L- Right RM: V3 Right dissection. Aspirin 9 Facial hypoesthesia (GOS) = 4
6 M/40 Dyslip. Sm Traumatic dissection C-L- Right A: V3 Right occlusion. Anticoagulation 14 None (GOS) = 5
7 M/33 AH Traumatic dissection C-L- Left A: V4 Left stenosis. Aspirin 5 None (GOS) = 5
8 F/28 ---- Spontaneous dissection RC-L- Left A: V3-4 Left occlusion. Aspirin 24 None (GOS) = 5
9 M/46 Alcohol, Dyslip. Traumatic dissection C-L-I Left A: V4 bilateral stenosis Aspirin 24 None (GOS) = 5
10 M/30 ---- Traumatic dissection R-L- Right A: V3 Right occlusion. Anticoagulation 65 None (GOS) = 5
11 M/34 Sm, Alcohol Traumatic dissection R-L- Right A: V3 Right stenosis. Anticoagulation 6 None (GOS) = 5
12 M/29 Sm, Dyslip. Spontaneous dissection RC-L- Right A: V4 bilateral stenosis. Aspirin 7 None (GOS) = 5
13 F/48 Estenosis mitral, Dyslip. Cardioembolic C-L- Right A: V3-4 Right occlusion. Clopidogrel 12 Severe dysphagia (GOS) = 3
14 M/52 AH, PFO Cardioembolic C-L- Right A: PICA stenosis Aspirin 3 No (GOS) = 5
15 F/37 PFO Cardioembolic C-L- Left A: PICA distal occlussion Clopidogrel 8 Vrtigo (GOS) = 4
16 M/33 PFO, Dyslip, ISA, FVL, AFL, SLE. Cardioembolic R-L- Left A: normal Anticoagulation 17 Dysarthria, dysmetria, nystagmus (GOS) = 4
17 M/60 Alcohol, Dyslip, DM. Cardioembolic C-L- Right A: PICA occlusion Ticlopidine 13 No (GOS) = 5
18 M/60 AH, Alcohol, Sm., Dyslip. Cardioembolic C-L- Left A-RMI: V4 Left stenosis. Aspirin 2 No (GOS) = 5
19 M/63 AH, Alcohol, DM, Dyslip. Cardioembolic C-L- Left A: V4 Left stenosis. Ticlopidine 36 No (GOS) = 5
20 F/47 AH Atherothrombotic C-L- Right A: V4 Right stenosis. Clopidogrel 12 No (GOS) = 5
21 F/49 Ah, Sm., Dyslip. Atherothrombotic C-L- Right A: V4 Right stenosis. PICA stenosis Aspirin 2 Dysarthria, facial hypoesthesia (GOS) = 4
22 M/68 Previous Stroke, AH Atherothromboembolic A-A C-L- Left D, MRI: V1 Left stenosis. Aspirin 6 Vertigo (GOS) = 4
23 F/77 Previous Stroke, AH, DM Cryptogenic R-C-L ---- Aspirin 0 Death (GOS) = 1
24 F/77 AH Cryptogenic R-L- Right ---- Aspirin 36 Dysphonia (GOS) = 4
25 F/37 Sm, Alcohol Cryptogenic C-L- Right A: normal Aspirin 2 No (GOS) = 5
26 M/19 ---- Cryptogenic C-L- Right A: normal Aspirin 15 No (GOS) = 5

PFO: patent foramen ovale; ISA: interatrial septum aneurysm; PCD: protein C deficiency; APL: antiphospholipid; SAPL: secondary antiphospholipid; C-L: caudal-lateral;

R-L: rostral-lateral; RC-PL: rostral-caudal-postero-lateral; CP-L: caudal-postero-lateral; A: angiography; A-MRI: angio-magnetic resonance; D: Doppler neck/transcranial; Sm: smoking; AH: arterial hypertension; DM: diabetes mellitus; Dyslip: dyslipidemia; SLE: systemic lupus erythematosus lupus; PICA: posteroinferior cerebellar artery;

S: sex; A: age (years); M: months; MRI: magnetic resonance imaging; CT: computerized tomography; A-A: arterio-arterial; FVL: Leiden V factor.

Table 2 Clinical manifestations, etiology, and prognosis of Wallenberg syndrome with isolated medullary infarction (WS-IBLI), n = 26 

Symptoms Signs Etiology n = 26
Vertigo/dizziness, n (%) 24 (92) Body hypoesthesia n (%) 25 (96) Arterial dissection, n (%) 12 (46)
Gait ataxia, n (%) 20 (77) Nystagmus, n (%) 21 (81) Atherothrombotic, n (%) 8 (31)
Headache, n (%) 19 (73) Palate weakness, n (%) 21 (81) Cardioembolism, n (%) 4 (15)
Dysphagia, n (%) 17 (65) Horner, n (%) 19 (73) Cryptogenic, n (%) 2 (8)
Body hypoesthesia, n (%) 16 (62) Gait Ataxia, n (%) 19 (73) 30-days prognosis (GOS) n=26
Vomiting, n (%) 15 (58) Facial hypoesthesia, n (%) 19 (73) (GOS 5) Good outcome, n (%) 16 (61)
Facial hypoesthesia, n (%) 15 (58) Nauseous abolished, n (%) 17 (65) (GOS 4), n (%) 8 (30)
Nausea, n (%) 15 (58) Dismetry, n (%) 14 (54) (GOS 3), n (%) 1 (4)*
Horner, n (%) 14 (54) Facial paralysis, n (%) 11 (42) (GOS 2), n (%) ------
Diplopia, n (%) 12 (46) Corneal reflex loss, n (%) 7 (27) (GOS 1) Death, n (%) 1 (4)
Dysmetry, (%) 11 (42) ------ Functional prognosis (17 months average) n = 25
Dysphonia or hoarseness, n (%) 11 (42) ------ (GOS 5) Good outcome, n (%) 24 (96)
Dysarthria, n (%) 11 (42) ------ (GOS 4), n (%) ------
Weakness, n (%) 9 (35) ------ (GOS 3), n (%) 1 (4) *
Hiccups or singultus, n (%) 8 (31) ------ (GOS 2), n (%) -----
Facial paralysis, n (%) 6 (23) ------ (GOS 1) Death, n (%) -----

*Dysphagia, GOS: Glasgow Outcome Scale.

At neurological examination, the main signs were ipsilateral or contralateral abnormalities of sensation (96%), nystagmus (81%), palatal weakness (81%), Horner syndrome (73%), and gait ataxia (73 %) (Table 2). Gait ataxia was more frequent in young subjects and facial paralysis in rostrocaudal infarcts (p < 0.05).

To identify the mechanism of the stroke, several studies were used, including MRA in 18 patients (69%), transcranial Doppler ultrasound in 9 (35%), transesophageal echocardiogram in nine (35%), and digital subtraction angiography in eight cases (31%). The vascular abnormalities included: vertebral stenosis in ten cases (37%), vertebral artery occlusion in six (22%), PICA occlusion in two (7%), and PICA stenosis in one (4%) (Tables 1 and 2). These findings did not show a significant association with the age, sex, or location of the IBLI.

The primary etiology of the WS-IBLI corresponded to non-atherosclerotic vascular disease, including arterial dissection in 12 patients (46%). In eight patients, the cause was classified as atherothrombotic (31%), and in four, it was classified ad cardioembolic (15%). Two of the patients (8%) were classified as cryptogenic. Two cases with thrombophilia were included: one patient with systemic erythematosus lupus (with positive antiphospholipid antibodies and factor V Leiden) deficiency and another with Protein C deficiency.

Of the potentially cardioembolic sources reported, patent foramen ovale was identified in three cases (in one patient associated with an intra-atrial septum aneurysm) (Tables 1 and 2).

The clinical condition at the time of hospital discharge according to the GOS reported: one death (4%)-associated with sudden respiratory arrest; 16 patients were discharged with minor non-disabling sequelae (61%), eight with moderate sequelae (38%), and one patient with severe sequelae (dysphagia) (4%). Regarding antithrombotic treatment in the acute phase and as a subsequent secondary prevention measure: 21 (80%) patients were treated with antiplatelet agents (17 with aspirin, three with clopidogrel, and two with ticlopidine). Five patients (20%) were anticoagulated (four extracranial dissections and one cardioembolic).

Follow-up was available with an average of 17 months (range 1-72) with a median 16 months in 25 patients, with a GOS of 5 at the time of the last evaluation in 24 patients (96%). The one remaining patient continued with severe dysphagia requiring the use of a permanent nasojejunal tube. In our series, no recurrence of stroke was observed at long-term follow-up.

Regarding the etiology, arterial dissection was significantly associated with age younger than 45 years, since it occurred in ten of 12 cases (p = 0.001), while atherothrombotic etiology predominated among those older than 45 years in 8 of eight patients (p = 0.001). No other significant differences were observed between arterial findings or prognosis concerning age, sex, and location of the infarction (findings not shown in the table).

Discussion

From the original clinical description made by Alex Marcet more than two centuries ago, and the first clinicopathological characterization made by Adolph Wallenberg at the beginning of the last century, WS syndrome is one of the most studied disorders throughout the history of neurology4,6,13.

In our setting, WS has been analyzed on more than one occasion, with isolated clinical-radiological reports14-17. Despite this, there is no precedent for a relatively large cohort of patients with SW and IBLA that provides the clinical, radiological, etiological, and prognostic information as in the present study.

In our cohort, the patients with WS-IBLI were mostly men (2:1 ratio), similar to other reported series18-23. The average age of our patients was 45 years, a much lower average compared with the previous by other authors (55 years)18-23. This may be due to the selection bias inherent in our reference hospital centers.

Traditional risk factors, including high blood pressure, diabetes, and dyslipidemia, were observed less frequently, due to the lower average age in our cohort. This observation is also supported by a higher frequency of alcoholism and smoking, more frequent in young patients24.

The caudal location of the ILMI predominated over the rostral topography in a 4:1 relationship. This finding is repeatedly reported by other series and is probably associated with the higher frequency of proximal vertebral artery involvement (due to stenosis or occlusion) observed in our study9,11.

Regarding the symptoms and signs of WS-ILMI, our patients did not show substantial differences with other reports19,20,23. The most common symptom was vertigo in comparison with others studies reporting dysphonia and dyshagia as the main clinical findings25. Headache was observed in 73% of cases with no difference regarding age, sex, or infarct location. This frequency is higher than other WS series, where it is reported in 30-52% of patients19,23,26. A plausible explanation is the association of arterial dissection with a presenting headache.

However, in the signs and symptoms analysis of symptoms according to the location (not shown in tables), the group of patients younger than 45 years presented more significant gait ataxia (p = 0.01); while dysarthria, dysphagia, and peripheral facial paralysis were observed more frequently in the WS-IBLI of rostral location (all with p < 0.05). This difference can be explained by the presence or absence of involvement of the ambiguous nucleus5,7. In rostral infarcts, this nucleus is affected, since these are narrower lesions that tend to affect the most ventral portion of the medulla7. Although the existence of facial paralysis is rare and its origin is unclear, in our series, this deficit occurred in a third of patients. It has been postulated that, in patients with facial paralysis, the injury could also affect the pons27. However, none of our patients had apparent involvement at this level. Kim, observed a greater involvement of the facial nerve fascicles and the corticobulbar fibers in relation to facial paralysis in rostral bulbar infarcts9.

In our cohort, the most frequent cause of WS-IBLI was arterial dissection (in < 45 years-old patients), unlike other series where it is reported as the second or third cause in frequency28,29. Vertebral dissection has also been reported as one the most common etiologies in young patients in some series30,31. Large vessel disease (atherothrombotic or atherothromboembolic) was the second cause associated with an age > 45 years. A probable explanation for the higher incidence of arterial dissections in young patients is the higher frequency of high-risk physical and occupational activity (violent or abrupt) compared to older age groups. Of the infrequent causes, two cases with prothrombotic status were found as associated conditions: one patient with systemic erythematosus lupus (with positive antiphospholipid antibodies and factor V Leiden deficiency) and one with Protein C deficiency, which is an uncommon association in the literature32,33.

The vascular abnormalities in our series coincide with those reported in the literature: vertebral artery stenosis was the most frequent, followed by vertebral artery occlusion, in 44% and 21%, respectively. Only two patients had PICA involvement34,35.

Regarding complications, prognosis, and sequelae, our data are similar to that provided by the literature. WS usually has a benign prognosis with a low percentage of moderate and severe long-term complications and a 5-year survival > 50%36. Since our long-term follow-up was heterogeneous (range from 1 to 72 months), we were unable to perform a 5-year survival statistical analysis.

Most of the symptoms and signs of WS tend to improve rapidly, as occurred in our work. In contrast to other series, the most frequent sequela was sensory (cross-body paresthesia) followed by residual Horner syndrome; the only severe sequel was dysphagia37-39. In our series, only one patient died suddenly due to probable bronchoaspiration. Respiratory failure is usually the most common cause of death reported in WS39.

During follow-up, 61% of the patients had good recovery (GOS of 5) at 30 days and 96% in the long-term, confirming the benign prognosis of this syndrome.

Conclusion

Our study contributes to the clinical characterization of WS with a strictly lateral and isolated location (WS-IBLI), in addition to offering a new perspective on the functional prognosis in the medium term. A non-atherothrombotic etiology of SW should be considered in young patients with no other associated risk factors. Close monitoring and antithrombotic or anticoagulant therapy are essential in patients with SW to prevent stroke recurrence and to detect complications associated with this syndrome, which usually presents a benign course. The main limitation of this study was the selective sample of cases obtained from high concentrations centers which can lead to information biases. Further multi-center studies are needed in the future to complement the information presented in this manuscript.

Funding

This research has not received any specific grant from agencies in the public, commercial, or non-profit sectors.

Ethical disclosures

Protection of human and animal subjects. The authors declare that no experiments were performed on humans or animals for this study.

Confidentiality of data. The authors declare that they have followed the protocols of their work center on the publication of patient data.

Right to privacy and informed consent. The authors declare that no patient data appear in this article.

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Received: April 19, 2020; Accepted: June 15, 2020

* Correspondence: José L. Ruiz-Sandoval. E-mail: jorulej-1nj@prodigy.net.mx

Conflicts of interest

None to report.

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