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Abstract

Acute pulmonary thromboembolism is associated with high mortality, similar to that of myocardial infarction and stroke. We studied the clinical presentation and management of pulmonary thromboembolism in the Indian population. An analysis of 140 patients who presented with acute pulmonary thromboembolism at a large volume center in India from June 2015 through December 2018 was performed. The mean age of our study population was 50 years with 59% being male. Comorbidities including deep vein thrombosis, diabetes mellitus, hypertension, and chronic obstructive pulmonary disease were present in 52.9%, 40%, 35.7% and 7.14% of patients, respectively. Out of 140 patients, 40 (28.6%) patients had massive pulmonary thromboembolism, 36 (25.7%) sub-massive pulmonary thromboembolism, and 64 (45.7%) had low-risk pulmonary thromboembolism. Overall, in-hospital mortality was 25.7%. Multivariate regression analysis found chronic kidney disease and pulmonary thromboembolism severity to be the only independent risk factors. Thrombolysis was performed in 62.5% of patients with a massive pulmonary thromboembolism and 63.9% of patients with a sub-massive pulmonary thromboembolism. In the massive pulmonary thromboembolism group, patients receiving thrombolytic therapy had lower mortality compared with patients who did not receive therapy (p=0.022), whereas this difference was not observed in patients in the sub-massive pulmonary thromboembolism group. We conclude that patients with acute pulmonary thromboembolism in India presented more than a decade earlier than our western counterparts, and it was associated with poor clinical outcomes. Thrombolysis was associated with significantly reduced in-hospital mortality in patients with massive pulmonary thromboembolism.

Keywords

acute pulmonary embolism thrombolysis shock acute cor-pulmonale

Introduction

Venous thromboembolism (VTE) constitutes a disease spectrum ranging from deep venous thromboembolism (DVT) of the extremities to massive pulmonary thromboembolism (PE), which is associated with high morbidity and mortality if left untreated. Incidence of VTE varies from 0.5 to 2 per 1000 inhabitants.^1,2 The exact incidence of PE remains unknown, as it may go undetected in 40–50% of patients with DVT.⁶ An autopsy-based study showed that approximately one-third of patients with a fatal PE could be identified before death.⁴ The International Cooperative Pulmonary Embolism Registry (ICOPER) demonstrated that the mortality rates for massive and sub-massive PE were 58.3% and 15.1%, respectively.⁵

There are limited data with regard to PE, its management and associated complications in India, with the majority of the clinical evidence being derived largely from case reports and a select few small-sized studies.⁶ An autopsy-based study from Northern India showed PE to be the cause of death in 15.9% of all hospitalized patients.⁷ A recent epidemiological study including 2420 Asian patients reported that the rate of symptomatic VTE or sudden death due to VTE to be 2.3% higher than their western counterparts.⁸ According to the guidelines set out by the American College of Cardiology (ACC) ⁹ and the European Society of Cardiology (ESC),¹⁰ therapeutic management of patients with PE included anti-coagulation, intravenous and catheter-directed thrombolysis (CBT), and surgical embolectomy. We sought to study the clinical characteristics, treatment strategy, in-hospital outcomes, and prognostic factors of patients with pulmonary embolism in India.

Methods

Study design

Our study was a non-randomized, retrospective, single-center, observational study, and was an investigator-initiated non-funded research project. Patients >18 years of age who were diagnosed and treated at our Institute from June 2015 through December 2018 were enrolled in the study. The study was approved by the Institute’s Ethics Committee. Informed consent was not obtained from the patients, as this study was a retrospective study which was based on a database. Patients with acute PE that was diagnosed by computer tomography-pulmonary angiography (CT-PA), patients with acute PE superimposed on a background of chronic PE, and patients in shock with screening echocardiogram showing evidence of PE were included in the study. Patients with chronic PE or diagnosed with PE in the remote past who were admitted for other medical reasons, patients with no demonstrable PE by CT-PA, and no echocardiographic evidence of PE were excluded from the study.

Data collection

Two physicians (MK and AVR) collected the patients’ data from the electronic database information system of our institution. If there was any discrepancy in the data collected, a third physician (NBS) served as an arbitrator to resolve any issues. Information about presenting symptoms, co-morbidities, laboratory results, and findings of imaging studies which included venous Doppler, trans-thoracic echocardiogram (TTE), and CT-PA was collected. Data pertaining to treatment administered to individual patients including anticoagulation therapy, thrombolytic therapy, and surgical thrombectomy were also collected. Patients were categorized into massive, sub-massive, and low-risk PE groups based on the 2011 American Heart Association (AHA) guidelines⁹ (Supplementary document) with the demographics, treatment, and outcomes being analyzed separately for each group. The primary outcome of the study was in-hospital mortality. Bleeding outcomes were evaluated and graded based on the Bleeding Academic Research Consortium (BARC), with patients who had a BARC grade of ≥3 being considered significant.^11,12

Statistical analysis

We expressed categorical data as ratio or proportion or percentage, and continuous data as mean ± standard deviation or median (Interquartile range), as appropriate. Continuous variables were analyzed by t-test or ANOVA when appropriate. We used the Chi-square test to assess the significance of categorical variables. Multiple logistic regression analysis was performed to identify the risk factors for in-hospital mortality. A two-tailed p-value <0.05 was considered significant. All analyses were performed using SPSS 26 (IBM, New York).

Results

Baseline characteristics

One hundred and forty patients were included in the study, with a mean age of 50 ± 15 years (41% female) (Table 1). The most common presenting symptom was NYHA class III and NYHA class IV dyspnea (61.5%), followed by chest pain (35%) and cough (32%). The mean duration from symptom onset to hospital presentation was 3.2 days with 75% of patients presenting within five days. DVT, diabetes mellitus, hypertension, recent surgery, recent trauma, malignancy, coronary artery disease, and COPD were present in 52.9%, 40%, 35.7%, 25.7%, 17.1%, 16.4%, 10.3%, and 7.14% of patients, respectively. The mean pulse rate was 109 beats per minute, and the mean respiratory rate was 25 breaths per minute. The in-hospital mortality was 25.7%. Right ventricular dysfunction and severe pulmonary hypertension (PH)were noticed in 50% and 5.7% of patients, respectively.

Table 1.

Baseline characteristics of study population

Baseline characteristics of the study population (n = 140)	Count (No.)	Percentage of patients/±1 standard deviation
Age (year)	50.3	±14.87
Sex
Female	57	40.7%
Male	83	59.3%
Symptoms
Dyspnea
NYHA I	23	16.4%
NYHA II	31	22.1%
NYHA III	53	37.9%
NYHA IV	33	23.6%
Syncope	14	10.0%
Chest Pain	49	35.0%
Cough	45	32.1%
Hemoptysis	14	10.0%
Palpitations	19	13.6%
Risk factors
Deep venous thrombosis	74	52.9%
Diabetes	56	40.0%
Malignancy	23	16.4%
Hypertension	50	35.7%
Chronic kidney disease	13	9.2%
Recent surgery	36	25.7%
Pregnancy	3	2.1%
Chronic obstructive pulmonary disease	10	7.1%
Trauma	24	17.1%
Travel	1	0.7%
Pulse (per minute)	108.89	±19.19
Respiratory rate (per minute)	25.62	±6.984
Pulmonary embolism severity index
<65	38	27.1%
66–85	36	25.7%
86–105	20	14.2%
106–125	16	11.4%
>125	30	21.4%
Right ventricular dysfunction	70	50%
Pulmonary hypertension (PH)/right ventricular systolic pressure (RVSP)
No PH (PH<30mmHG)	59	42.1%
Mild PH ( PH-30-49mmHg)	41	29.2%
Moderate PH (PH- 50-69mmHg)	32	22.8%
Severe PH (PH->70mmHg)	8	5.7%
Thrombolysis done	50	35.7%
Bleeding Academic Research Consortium (BARC) Bleeding ≥3	13	9.2%
Mortality	36	25.7%

Univariate and multivariate analysis

It was found that chronic kidney diseases (CKDs), chronic obstructive pulmonary disease (COPD), PESI score, pulmonary embolism severity index (PESI class), PE severity, and PH were significantly different between patients who survived and patients who died (Table 2). Patients with massive PE had PESI scores ranging between 124 and 144. Patients with sub-massive PE had PESI scores ranging between 81 and 99, while those with low-risk PE had PESI scores ranging between 59 and 69. Correlation between PESI and death was highly significant (p<0.001). Patients who survived had PESI scores between 72.5 and 83.95, whereas patients who died had PESI scores between 113.73 and 141.33, thereby emphasizing the importance of the PESI score as a prognostic tool. The receiver operating curve (ROC) comparing PESI score with in-hospital mortality showed a significant positive relationship between the two variables. The area under the curve for the ROC curve was 0.852 (CI: 0.772–0.932) with a p-value <0.001. Using a PESI score of 129 as a cutoff for predicting mortality, a strong positive correlation was seen between the two variables (p<0.001). Patients with a PESI score of ≥129 were found to have a mortality rate of 78.3%. However, multivariate regression analysis found massive PE to be an independent risk factor for in-hospital mortality (Table 3). A negative association of mortality with CKD status was also noted.

Table 2.

Univariate analysis for in-hospital mortality in patients with pulmonary embolism

Characteristics	Live	Death	p value
Age (year)	49.65 ± 15.35	52.25 ± 13.424	0.369
Sex
Female	41 (39.4%)	16 (44.40%)	0.597
Male	63 (60.6%)	20 (55.60%)	0.597
Acute worsening of symptoms (days)	3.34 ± 3.818	2.89 ± 2.435	0.512
Dyspnea NYHA I	20 (19.2%)	3 (8.3%)	0.077
NYHA II	26 (25.1%)	5 (13.90%)
NYHA III	38 (36.5%)	13 (41.70)%
NYHA IV	20 (19.2%)	9 (36.1%)
Syncope	9 (8.7%)	5 (13.90%)	0.367
Chest pain	39 (37.5%)	10 (27.80%)	0.292
Cough	32 (30.80%)	13 (36.10%)	0.554
Hemoptysis	12 (11.50%)	2 (5.60%)	0.302
Palpitations	14 (13.5%)	5 (13.90%)	0.949
DVT	55 (52.9%)	19 (52.80%)	0.991
DM	38 (36.50%)	18 (50.00%	0.155
Malignancy	17 (16.3%)	6 (16.70%)	0.964
Systemic hypertension	34 (32.7%)	16 (44.40%)	0.205
Recent surgery	29 (27.90%)	7 (19.40%)	0.318
Pregnancy	2 (1.90%)	1 (2.80%)	0.760
CKD	5 (4.8%)	8 (22.2%)	0.002
COPD	4 (3.80%)	6 (16.70%)	0.010
Trauma	19 (18.30%)	5 (13.90%)	0.548
Travel	1 (1.00%)	0 (0%)	0.555
PESI
≤65	36 (34.6%)	2 (5.6%)	0.001
66–85	33 (31.7%)	3 (8.3%)
86–105	16 (15.4%)	4 (11.1%)
106–125	13 (12.3%)	3 (8.3%)
>125	6 (5.8%)	24 (66.7%)
Pulmonary embolism severity index	78.26 ± 29.273	127.53 ± 40.790	<0.001
PTE severity
Massive	11 (10.6%)	29 (80.6%)	<0.001
Sub massive	33 (31.7%)	3 (8.3%)
Low risk	60 (57.7%)	4 (11.1%)
RV Dysfunction	43 (41.3%)	27 (75.0%)	0.001
Pulmonary hypertension(PH)/ Right ventricular systolic pressure (RVSP)
No PH (PAH<30mmHG)	47 (45.20%	12 (33.30%)	0.001
Mild PH ( PAH-30–49mmHg)	36 (34.60%)	5 (13.90%)
Moderate PH (PAH- 50–69mmHg)	15 (14.4%)	17 (47.2%)
Severe PH (PAH->70mmHg)	06 (5.8%)	02 (5.6%)
Thrombolysis-done	34 (32.7%)	16 (44.4%)	0.205

Table 3.

Multivariate analysis for in-hospital mortality in patients with pulmonary embolism.

Parameters	Significance (p)	Odds ratio	95% Confidence interval
Parameters	Significance (p)	Odds ratio	Lower limit	Upper limit
Chronic kidney disease	0.012	0.105	0.018	0.612
Chronic obstructive pulmonary disease	0.36	0.41	0.061	2.78
Massive PE	<0.0001	67.27	8.89	508.74
Sub massive PE	0.548	1.95	0.21	18.64
Right ventricular dysfunction	0.29	2.80	0.41	19.17
Mild pulmonary hypertension	0.71	1.55	0.16	15.4
Moderate pulmonary hypertension	0.80	0.74	0.70	7.72
Severe pulmonary hypertension	0.25	3.72	0.39	35.41

Subgroup analysis

Out of 140 patients, 40 (28.6%) had a massive PE, 36 (25.7%) had a sub-massive PE, and 64 (45.7%) had a low-risk PE (Fig. 1a). Age (p=0.003), COPD (p=0.008), and PESI score (p=0.001) were found to be significantly different in the sub-group analysis. Patients within the massive PE group were found to be significantly younger as compared to the rest (Table 4). Sub-group analysis showed that patients with a massive PE had an in-hospital mortality rate of 72.5% as opposed to 8.3% and 6.3% in patients with a sub-massive PE and a low-risk PE, respectively (Table 4). Further, subgroup analysis of patients with massive PE based on their thrombolytic status showed no difference between those who received thrombolytic therapy and those who had not received thrombolytic therapy except in hypertension and PESI class. Patients who had not received thrombolytic therapy had a history of hypertension in 57.1% as compared with 16.7% in the other group (p=0.01). In the non-thrombolytic therapy group, 92.9% belonged to PESI class 5 status as compared with 50% in the thrombolytic group (p=0.02).

Fig. 1.

(a) The classification of patients with pulmonary embolism based on clinical severity. (b) The percentage of patients who received thrombolysis in each category.

Table 4.

Pulmonary embolism and clinical outcomes based on clinical severity.

Characteristics	Pulmonary thromboembolism Severity
Characteristics	Massive(n=40)	Sub massive(n=36)	Low risk(n=64)	p value
Age (year)	47 ± 14	50 ± 16	52 ± 15	0.003
Sex
Female	16 (40%)	11 (30.60%)	30 (46.90%)	0.279
Male	24 (60%)	25 (69.40%)	34 (53.10%)	0.279
Dyspnea
NYHA I	4 (10%)	0 (0%)	19 (29.70%)	Stat test could not be performed
NYHA II	3 (7.50%)	11 (30.60%)	17 (26.60%)
NYHA III	16 (40%)	16 (44.40)%	21 (32.80%)
NYHA IV	17 (42.50%)	9 (25%)	7 (10.90%)
Syncope	6 (15%)	4 (11.10%)	4 (6.30%)	0.340
Chest pain	12 (30%)	16 (44.40%)	21 (32.80%)	0.371
Cough	11 (27.50%)	12 (33.30%)	22 (34.40%)	0.754
Hemoptysis	3 (7.50%)	4 (11.10%)	7 (10.90%)	0.823
Palpitations	6 (15%)	7 (19.40%)	6 (9.40%	0.352
Deep venous thrombosis	20 (50%)	19 (52.80%)	35 (54.70%)	0.897
Diabetes	15 (37.50%)	15 (41.70%	26 (40.60%)	0.925
Malignancy	6 (15%)	7 (19.40%)	10 (15.60%)	0.849
Hypertension	14 (35%)	15 (41.70%)	21 (32.80%)	0.671
Recent surgery	9 (22.50%)	8 (22.20%)	19 (29.70%)	0.614
Pregnancy	1 (2.50%)	1 (2.80%)	1 (1.60%)	0.906
Chronic kidney disease	6 (15%)	3 (3.80%)	4 (6.30%)	0.318
Chronic obstructive pulmonary disease	7 (17.50%)	2 (5.60%)	1 (1.60%)	0.008
Trauma	7 (17.50%)	6 (16.70%)	11 (17.20%)	0.995
Travel	1 (2.50%)	0 (0%)	0 (0%)	0.284
Duration (days)	4 ± 5	6 ± 4	6 ± 7	0.287
Acute worsening (days)	3 ± 2	4 ± 2	3 ± 5	0.154
Pulmonary embolism severity index	134 ± 32	90 ± 27	64 ± 20	<0.001
Outcome
Live	11 (27.50%)	33 (91.70%)	60 (93.80%)	<0.001
Death	29 (72.50%)	3 (8.30%)	4 (6.30%)	<0.001
Pulmonary embolism severity index
Live	119.91 ± 21.585	89.64 ± 27.26	64.37 ± 20.54	Not significant
Death	139.83 ± 33.37	97.33 ± 25.15	61 ± 17.91	Not significant
Lysed
Thrombolyzed	25 (62.50%)	23 (63.90%)	2 (3.10%)	<0.001
Not thrombolyzed	15 (37.50%)	13 (36.10%)	62 (96.90%)	<0.001
Bleeding
Yes	5 (12.50%	5 (13.90%)	3 (4.70%)	0.223
No	35 (87.50%)	31 (86.10%)	61 (95.30%)	0.223
Thrombolyzed
Live	10 (40%)^a	22 (95.7%)^b	2 (100 %)^c
Death	15 (60%)^a	1 (4.3%)^b	0 (0.1%)^c
Not thrombolyzed
Live	1 (6.7%)^a	11 (84.6%)^b	58 (58.1 %)^c
Death	14 (93.3%)^a	2 (15.4%)^b	4 (3.9%)^c

^ap=0.022.

^b,cp=not significant.

Use of thrombolytic therapy and its clinical effects

Thrombolytic therapy was given to 62.5% of patients who had massive PE and 63.9% of patients who had sub-massive PE (Fig. 1b). In-hospital mortality was significantly lower in patients who had a massive PE and received thrombolytic therapy compared with those who did not receive thrombolytic therapy (p=0.02) (Fig. 2 and Table 4). In contrast, in-hospital mortality was not significantly different between those patients who had sub-massive PE and received thrombolytic therapy compared with those who did not. In the low-risk PE group, two patients received intravenous thrombolytic therapy. One patient received thrombolytic therapy to prevent complications of post-thrombotic syndrome due to a large thrombus burden of DVT involving the left common iliac vein and inferior vena cava. The second patient had protein S deficiency and a history of recurrent PE with a large thrombus burden of DVT. The second patient underwent thrombolysis with tenecteplase, and during the post-thrombolysis phase, an IVC filter was placed. In total, 9.2% had significant bleeding, while 14% of patients with PE treated with thrombolytic therapy developed BARC grade ≥3 bleeding requiring a blood transfusion. In patients who were not administered thrombolytic therapy, 5.6% of them required a blood transfusion due to anemia or malignancy-related coagulopathy.

Fig. 2.

The survival of patients with different clinical presentation based on their status of thrombolysis.

Use of catheter-directed therapy and other medications

Three patients with acute massive PE received catheter-directed therapy (CDT). One patient had a history of a hemorrhagic cerebro-vascular accident (CVA) and survived, whereas the two other patients died from their disease. One patient with low-risk PE and significant DVT involving proximal deep veins was thrombolyzed peripherally using CDT. All survived patients were initially anticoagulated using unfractionated heparin or low molecular weight heparin and subsequently transitioned to one of the following oral anticoagulants warfarin, nicoumalone, apixaban, rivaroxaban, or dabigatran.

Discussion

To the best of our knowledge, this is the largest study from India evaluating the presenting symptoms and clinical outcomes in patients with PE. In our study, 25.7% of patients with PE died, while 72.5% of patients with massive PE died. Nearly two-thirds of patients with massive PE received thrombolytic therapy. The in-hospital mortality for the patients with massive PE who received thrombolytic therapy was 60%, while for those who did not receive thrombolytic therapy was 93.3%, with an absolute risk reduction of 33.3% (NNT=3).

Indians appear to have a greater propensity towards developing PE at an earlier age, especially massive PE, and are associated with higher mortality. In this study, we found that the mean age of the Indian population having PE was 50 years as opposed to above 65 years as seen in the Western population.^13,14 Our finding is in accordance with the findings observed in the Arrive registry which is one of the largest studies on VTE from India.¹⁵ A recent trial in South India also found that the mean age of presentation was 52 years.¹⁶ PE should therefore be suspected in any patient with unexplained or new-onset dyspnea, chest pain, palpitations, syncope, or unexplained hypotension.¹⁷ Early detection and prompt treatment are vital to the management of patients with PE .¹⁸

Previously published studies have found that a PESI score >125 was associated with a higher risk of mortality.¹⁹ We also found that a PESI score >129 was highly predictive of mortality in our univariate analysis alone. Of patients with a PESI score >129, 78.4% died. Multiple factors were found to be associated with in-hospital mortality in patients with PE in the univariate analysis. However, massive PE was an independent predictors of in-hospital mortality in the multivariate analysis. Nearly two-thirds of patients with massive PE received thrombolytic therapy. Patients who had a massive PE and received thrombolytic therapy had a lower mortality rate (NNT=3), thereby emphasizing the importance of initiating therapy promptly, specifically in critically ill patients with acute cor-pulmonale due to PE.

Thrombolytic therapy is associated with a higher rate of bleeding complications. It was observed that 12.5% of patients with massive PE who received thrombolytics developed bleeding BARC grade ≥3, requiring a blood transfusion. For patients who were deemed to be of high bleeding risk for systemic thrombolytics, catheter-directed therapy (CDT) is a potential alternative. ^20,21 CDT can be in the form of catheter-assisted embolectomy or catheter-directed intra-pulmonary thrombolysis and are proposed to have increased efficacy with better safety outcomes. Since we can directly instill the thrombolytic agent at a lower dosage into the thrombus via a side hole catheter, the rate of major systemic bleeding is reported to be lower as compared to systemic thrombolytic therapy^20,21 though occasional pulmonary hemorrhage can occur.²² These interventions need more research and standardization before they are widely used. At present, CDT can be used in patients with massive PE who have a high bleeding risk or failed systemic thrombolysis, provided appropriate expertise is available.²³ In our study, three patients with acute massive PE received catheter-directed therapy. One patient survived, while the other two succumbed to their illness.

Of the patients who had sub-massive PE, 64% of them received thrombolytic therapy. Unlike patients with massive PE treated with thrombolytic therapy, in-hospital mortality was not affected by the administration of thrombolytic therapy in the sub-massive group. There is a clear discordance between the major societal guidelines in the management of sub-massive PE.^10,23 A large, randomized trial, PEITHO – Pulmonary Embolism International Thrombolysis Trial has shown that fibrinolytic therapy decreased hemodynamic decompensation, while increasing the risk of major hemorrhage and stroke when compared with anticoagulation alone in patients with high-risk sub-massive PE ²⁴ without any effect on mortality. Therefore, bleeding risk associated with thrombolytic therapy is an important factor that warrants consideration in patients with PE.

Higher mortality in patients with massive PE especially in those who had not received the thrombolytic therapy may be inherently biased by the critical status of the patients which were shown by a higher PESI score compared with those who had received thrombolytic therapy. Also, a delay in clinical presentation, failure to administer thrombolytic agents, and associated co-morbid illnesses may add to the increased mortality observed in the overall population.

VTE-associated pulmonary embolism should be given equal importance as myocardial infarction and acute stroke considering the poor outcomes noticed in less-industrialized countries like India. Institution of regional centers which serve patients with PE, and an active pulmonary embolism response team (PERT) which consists of a multi-pronged, collaborative approach among various subspecialties in order to effectively coordinate the care of patients with massive PE has been associated with improved outcomes.^25–27

Conclusion

In our study, acute PE presented more than a decade earlier in Indian patients compared with their western counterparts and was associated with a very high mortality if left undetected or untreated. Thrombolytic therapy was associated with significantly reduced in-hospital mortality in patients with massive PE. Public education of this illness, promptly recognizing acute pulmonary thromboembolism and the concept of Pulmonary Embolism Response Team (PERT)with the creation of regional centers of excellence serving such patients will likely be instrumental in achieving improved patient outcomes.

Limitations

This was a single-center study done at a teaching hospital in Chennai, India. Therefore, the results of this study may not apply to other types of practice and other regions. Also, this was a retrospective, observational study dependent on the medical records and a computer-based patient database system; therefore, all possible limitations of a retrospective study hold true.

Supplemental Material

sj-pdf-1-pul-10.1177_2045894021992678 - Supplemental material for Clinical profile and management of patients with acute pulmonary thromboembolism – a single centre, large observational study from India

Supplemental material, sj-pdf-1-pul-10.1177_2045894021992678 for Clinical profile and management of patients with acute pulmonary thromboembolism – a single centre, large observational study from India by Thoddi Ramamurthy Muralidharan, Sankaran Ramesh, Balakrishnan Vinod Kumar, Aditya V. Ruia, Mohan Kumar, Akshaya Gopalakrishnan, Gurpreet S. Johal, Amit Hooda, Rohit Malhotra, Reza Masoomi, Mahalakshmi Ramadoss, Vinodhini Subramanian, Maria J. Kalsingh, Panchanatham Manokar, Jebaraj Rathinasamy, Shanmugasundram Sadhanandham, Jayanthy V. Balasubramaniyan, Preetam Krishnamurthy, Jayanthy S. Murthy, Sadagopan Thanikachalam and Nagendra Boopathy Senguttuvan in Pulmonary Circulation

Footnotes

Acknowledgements

We thank SRIHER for the facilities and support provided to conduct this study. We would like to thank all the staffs and fellows of the department of Cardiology and the members of the central research facility, SRIHER.

Conflict of interest

The author(s) declare that there is no conflict of interest.

Funding

This research received no specific grant from any funding agency in the public, commercial, or not-for-profit sectors.

Ethical approval

The study was approved by the Institute’s Ethics Committee. Informed consent was not obtained from the patients, as this study was a retrospective study which was based on a database

Guarantor

T.R Muralidharan.

Authors’ contributions

▪

ORCID iDs

Balakrishnan V. Kumar

Aditya V. Ruia

Nagendra B. Senguttuvan

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Clinical profile and management of patients with acute pulmonary thromboembolism – a single centre,large observational study from India

Abstract

Keywords

Introduction

Methods

Study design

Data collection

Statistical analysis

Results

Baseline characteristics

Univariate and multivariate analysis

Subgroup analysis

Use of thrombolytic therapy and its clinical effects

Use of catheter-directed therapy and other medications

Discussion

Conclusion

Limitations

Supplemental Material

sj-pdf-1-pul-10.1177_2045894021992678 - Supplemental material for Clinical profile and management of patients with acute pulmonary thromboembolism – a single centre, large observational study from India

Footnotes

Acknowledgements

Conflict of interest

Funding

Ethical approval

Guarantor

Authors’ contributions

ORCID iDs

References