Methods: Between March 2011 and May 2022, a total of 13 patients (7 males, 6 females; mean age: 52.6±13.0 years; range, 30 to 69 years) who underwent pulmonary endarterectomy and diagnosed with a pulmonary artery sarcoma were retrospectively analyzed. The diagnosis was confirmed histopathologically in all patients. Data including demographics, clinical characteristics, intra- and postoperative complications, length of hospital stay, morbidity, mortality, and short-term and long-term outcomes were recorded. Operative mortality was defined as death in the hospital or within 30 days of surgery.
Results: Mortality was observed in one patient due to massive hemoptysis. Morbidity developed in two patients due to acute respiratory distress. Pulmonary vascular resistance improved significantly from 508 dyn/s/cm-5 to 191 dyn/s/cm-5 (p<0.004). All patients received chemotherapy following surgery. Median follow-up was 14 months. Median survival for the entire series was 18 months. One-year and three-year survival rates were 60.6% and 30.3%, respectively. Median survival for leiomyosarcomas (n=6) was seven months, while it was 44 months for intimal sarcomas (p=0.004). Three-year survival was 66.7% for intimal sarcomas and 0% for leiomyosarcomas.
Conclusion: Pulmonary artery sarcoma may mimic chronic thromboembolic pulmonary hypertension. Patients with a suspected diagnosis of pulmonary artery sarcoma should be referred to expert pulmonary endarterectomy centers for surgery where a multidisciplinary team is available. Pulmonary endarterectomy has both diagnostic and therapeutic value and may improve survival and quality of life. Patients with intimal sarcoma have longer survival compared to those with leiomyosarcoma.
Despite novel imaging and interventional techniques, it remains difficult to diagnose PAS. Although, surgery still is the mainstay of management of patients with PAS, there is no widely accepted surgical approach until now. Surgery includes PEA, lobectomy, or pneumonectomy, based on the extension of the disease and patient clinical conditions. Surgery can provide a median survival of up to eight to 36 months; however, the prognosis of PAS is very poor with a median survival of 1.5 months without surgery.[1,3]
In the present study, we aimed to describe our experience with PAS in patients who underwent PEA, and evaluate clinical features, treatment, outcomes, and survival rates according to the histological subtypes of this malignant disease.
The diagnosis of CTEPH was established by the presence of mismatched perfusion defects on ventilation-perfusion scan combined with evidence of pulmonary hypertension, despite adequate anticoagulation for at least three months. Pulmonary function tests, computed tomography pulmonary angiography (CTPA), six-minutes walk test (6MWT), and right heart catheterization were routinely performed as a standard preoperative evaluation. All patients were assessed by our multidisciplinary team of CTEPH experts including expert PEA surgeons, pulmonologists, cardiologists, radiologists, as well as rheumatologists., and all care was provided including detailed diagnostics and all forms of CTEPH therapy. In our center, the following tests are routinely performed during assessment for surgery: complete blood count, blood chemistry, urinalysis, and acute inflammatory markers. For patients with suspected PAS or systemic vasculitis, fluorine-18-fluorodeoxyglucose positron emission tomography/computed tomography (PET/CT) was used. The definitive diagnosis was made based on a detailed histopathological examination. In nine patients, PET/CT was also performed, as malignancy was suspected. Our indications for PEA surgery can be listed as follows: patients with a mean pulmonary artery pressure (mPAP) of >20 mmHg, pulmonary vascular resistance (PVR) of 300 dyn/s/cm-5 or 3 Wood units, surgically accessible disease demonstrated in CTPA, and a World Health Organization (WHO)/ New York Heart Association (NYHA) functional class greater than II. Institutional standard protocols for management of perioperative anesthesia and postoperative care were followed for each patient. In-hospital complications were measured following surgery.
Our surgical technique was described previously.[5] Briefly, median sternotomy and cardiopulmonary bypass was performed. Most tumors were observed in the dorsal region of the main pulmonary artery often with a polypoid or fingerlike form, extending to the bifurcation of the main pulmonary artery. Following a proximal incision of the main pulmonary artery, a circumferential dissection plane was established between the gross tumoral mass with intimal and the medial layer of the pulmonary artery and extended to the distal segmental and subsegmental branches. A true endarterectomy plan was found and bilateral PEA was performed in all patients under deep hypothermia (20°C) and total circulatory arrest with intermittent cross-clamping of the aorta. Prolene sutures were used to close arteriotomy lines. No additional materials such as pericardial patch or grafts were required for pulmonary artery reconstruction. Concomitant surgical procedures were performed during re-warming period. Early postoperative hemodynamic measurements were completed in the operating room, before the patients were transferred to intensive care unit (ICU). No surgical margin was defined, since no resection was performed. No lung resection was done for PAS.
During follow-up, all patients were seen in our PEA outpatients' clinic at one, three, and six months. Patients were assessed with a 6MWT and echocardiography and were, then, classified functionally according to the WHO/NYHA functional class at each follow-up visit.
All patients had a histopathological diagnosis after surgery, and all survivors received adjuvant chemotherapy after recovering from the postoperative course. Recurrence and disease progression were defined as evidence of a new lesion on PA and metastasis to another part of the body, respectively.
Statistical analysis
Statistical analysis was performed using IBM
SPSS for Windows version 25.0 software (IBM Corp.,
Armonk, NY, USA). Continuous data were expressed in
mean ± standard deviation (SD) or median (min-max),
while categorical data were expressed in number and frequency. Pre- and postoperative measurements were
tested by the Wilcoxon signed-rank test. Survival
analysis was performed using the Kaplan-Meier
method. The log-rank test was used to compare survival probabilities between two groups (i.e., those
with the diagnosis of intimal sarcoma [IS] and those
with leiomyosarcoma [LM]). A p value of < 0.05 was
considered statistically significant.
Table 1. Baseline and demographic characteristics of patients
Following surgery, the patients were kept intubated and transferred to the ICU, and both postoperative hemodynamic parameters and mean mPAP and PVR were closely monitored and calculated from the first postoperative day until transfer from the ICU to the ward. Intra- and postoperative data are summarized in Table 2. The 30-day mortality was observed in one patient (7.6%) who had massive hemoptysis following PEA.[6] Despite pacing on venous arterial extracorporeal membrane oxygenation (VA-ECMO) as a salvage therapy, the patient died on postoperative Day 10 due to right heart failure and reperfusion injury. In addition, two patients developed acute respiratory distress syndrome in the early postoperative period, and VA-ECMO was initiated. The patients were weaned from VA-ECMO on postoperative Day 5 and 9, respectively and were discharged without any problem.
The mPAP decreased from 30.9±16.1 (range, 18 to 75) mmHg to 28.1±5.4 (range, 21 to 35) mmHg after surgery (p=0.182). A significant difference was found in the mean PVR, which decreased from 508±324.7 (range, 168 to 1,200) dyn/s/cm-5 to 191.5±74.7 (range, 120 to 344) dyn/s/cm-5 after surgery (p=0.004). The median follow-up was 14 (range, 7 to 75) month. The median survival for the entire series was 18 (range, 6 to 82) months (95% confidence interval [CI]: 3.90-32.09). The one-year and three-year survival rates were 60.6% and 30.3%, respectively. While the median survival for LM (n=6) was seven months (95% CI: 4.85-9.14), patients with IS had a median survival of 44 months (95% CI: 23.19- 64.80; (p=0.004).
Table 2. Intra- and postoperative data of patients
Figure 2 shows the Kaplan-Meier overall survival curve. While six of the cases were diagnosed as LM, as they had histomorphological smooth muscle differentiation and positive immunoexpression of smooth muscle markers (such as desmin and smooth muscle actin), six other patients were classified as IS. One patient was also diagnosed as an undifferentiated sarcoma, as he had malignant pleomorphic spindle cells without any differentiation (Figure 3). According to the survival estimations, the median survival for LM was seven months, while the patients with IS had a median survival of 44 months. For LM and IS, the one-year survival rates were 20% and 100%, respectively. Figure 4 shows the histology-specific survival curve. In addition, the three-year survival rate was 66.7% for IS and 0% for LM.
Figure 2. The Kaplan-Meier overall survival curve.
Apart from the patient who died in the postoperative 30-day period, six patients died during follow-up until the cut-off date of the study. Five of them died due to disease progression or recurrence, and one patient unfortunately died due to novel coronavirus disease 2019 (COVID-19). One patient required pneumonectomy for recurrence at four months after PEA and died at 44 months. The other six patients are still alive. The treatment and outcomes are shown in Table 3.
Pulmonary artery sarcoma is a rare condition with an incidence of 0.001 to 0.03% and its diagnosis is difficult due to its clinical similarity to acute or chronic pulmonary thromboembolism.[7,8] In our study, all patients with a possible diagnosis of CTEPH were treated, and all received effective anticoagulant therapy preoperatively for at least three months. The similarity between CTEPH and PAS complicates the diagnosis, management, and treatment. The tumor originating from the central pulmonary artery leads to progressive obstruction that impedes blood flow from the right ventricle to the pulmonary vascular bed. The CTPA is commonly used to distinguish between PAS and CTEPH, and although both show enhancement on CTPA, IS tends to present as a unilateral, central, lobulated, PA filling defect which increases in size along with the increasing diameter of the PAs and has acute angles with the vessel wall, in contrast to the pulmonary embolism. Moreover, IS shows heterogeneous densities due to areas of necrosis, hemorrhage, and ossification within the mass.[9] In addition, PET/CT can be used in the differential diagnosis of pulmonary sarcoma and CTEPH, as the standard pathology uptake values are different.[10] The CTPA is a routine practice in our center; however, nine patients underwent PET/CT in this study, five of whom had positive uptake. There was no significant difference between the histological types in terms of maximum standard uptake value (SUVmax) (p=0.629).
Pulmonary artery sarcoma is divided into two main types: intimal and intramural.[11] The former presents an intraluminal polypoid growth pattern.[12,13] On the other hand, the latter is different from IS and is classified separately as in soft tissue sarcoma (LM).[13] Since intimal PAS is more common than intramural PAS, PAS is often referred to as IS.[13] An IS resembles mucoid or gelatinous clots that fill vascular lumens, and the distal extension of the tumor may have firm fibrotic regions, be bony or gritty, and chondromyxoid foci may be present in mural lesions.[14] An IS may arise from the pluripotent mesenchymal cells of the intima artery, that is, the inner membrane of the pulmonary artery.[15] Therefore, PAS may have a variety of pathological types. Cox et al.[12] reported the pathological results of 138 cases of PAS, of which 43 were undifferentiated sarcomas. The typical histological features and immunohistochemical staining for PAS are important for classifying the different pathological types. Under the microscope, IS exhibits proliferation of spindle cells in a myxoid background.[16,17] The tumor may be also associated with large regional myxoid tissues and local necrosis, and typical spindle cells are arranged like a woven mat or striated, as in LM. Pulmonary artery IS is a malignant tumor that progresses rapidly. If the intervention is delayed, the prognosis is extremely poor and the recurrence rate is high.[18] Pulmonary artery LM is a rare disease. More recent reviews have suggested a predominance of two to one in women, with a median age at the time of diagnosis, ranging between 49 and 52 years.[17] Median survival w ithout surgery is one and a half months, and mortality is usually due to right-sided heart failure.
In the current study, survival probabilities were significantly different according to the histological type (p=0.004). The median survival time for LM was seven months, while IS had a median survival time of 44 months. In addition, the one-year survival rate was 20% for LM and 100% for IS.
There is no established treatment protocol for PAS. Currently, the main treatment for PAS is resection of sarcoma. Compared to isolated tumor resection, PEA seemed to yield a better survival rate and alleviate symptoms.[7,8,17,18] Although there is no consensus on surgical treatment, PEA and pneumonectomy are the two most common surgical procedures. Grazioli et al.[18] compared PEA and pneumonectomy in the surgical treatment of 13 patients PAS and reported a median survival of 6.6 months and 26.8 months, respectively. On the other hand, Jamieson[19] reported that pneumonectomy was not always beneficial in the treatment of the disease, as most cases are bilateral. We performed PEA to perform complete tumor resection in all patients, and the surgical approach was performed according to our published technique.[5] Pulmonary artery sarcoma usually arises within the main pulmonary arteries or around the pulmonary valve and often invades adjacent structures, such as the right ventricular outflow tract. This proximal extent of the tumor makes PEA more technically challenging compared to PEA for CTEPH. In addition, the consistency of the tumor can vary, presenting as either gelatinous or rigid material, and both variations lead to difficulty in finding the correct plane of dissection (Figure 5).
Mussot et al.[8] r eported 31 p atients w ith PAS. I n this study, 25 patients were treated with PEA and five patients with pneumonectomy. In addition, one patient required right pulmonary artery replacement. The 30-day mortality was 13% and one-, three-, and five-year survival rates were 63%, 29%, and 22%, respectively. In our study, only one patient had 30-day mortality (7.6%), and the median survival for the entire series was 18 months. Our one-year survival rate is 60.6%, consistent with previous studies.
Even after complete surgery, the prognosis of IS is poor due to frequent relapses, more often local than distant. A significant symptomatic improvement among PAS patients with endarterectomy has been well established and accepted. On the other hand, the knowledge on the benefit of adjuvant and/or neo-adjuvant therapy is still controversial. Some researchers believe that chemotherapy or radiotherapy has no effect on long-term survival, whereas the others suggest that it can prolong survival.[1,8,20] Adjuvant therapy is often used either alone or in combination with radiotherapy. As in lung cancer, if lung resection is planed surgical approach, neoadjuvant treatment with radiotherapy and/or chemotherapy may be considered to decrease tumor size and improve resectability. Xu et al.[21] reported a meta-analysis including 275 cases. Although surgical resections were different, patients who received adjuvant and/or neo-adjuvant therapy had longer survival rates. In addition, patients with complete resection or without metastasis had longer postoperative overall survival compared to incomplete resection or with metastasis. It has been reported that chemotherapy prolongs the postoperative survival in patients who had incomplete resection and metastasis [18] While Mussot et al.[8] found no significant difference between the patients with and without postoperative chemotherapy in their series, Blackmon et al.[22] reported better outcomes in the patients treated with a combination of chemotherapy and radiotherapy. Wang et al.,[23] also reported similar results. We preferred cisplatin as the chemotherapeutic agent for adjuvant therapy in all our patients in the study, and none of them received radiotherapy postoperatively, since no lung resection was performed. Even if treated, the postoperative survival rates are still poor, with a median overall survival ≤18 months.
Due to the shorter follow-up and the limited number of patients in our series, we cannot definitively prove that patients with IS had longer survival compared to LM. Nonetheless, although this is a retrospective study, our data represent a valuable contribution to the literature, considering how rare this disease is and how little experience there is with its treatment.
In conclusion, pulmonary artery sarcoma is a very rare vascular tumor with a poor prognosis. Its remarkable clinical and radiological similarity to chronic thromboembolic pulmonary hypertension makes diagnosis difficult. Although pulmonary endarterectomy is the mainstay of treatment, aggressive adjuvant therapy after surgery is necessary to improve survival and quality of life. Therefore, all patients suspected of pulmonary artery sarcoma should be referred to a referral center to be examined by an experienced multidisciplinary team. Although, both intimal sarcoma and leiomyosarcoma have a poor prognosis, the intimal sarcoma subtype seems to have a better short-term outcome. Further well-designed, large-scale, prospective studies are needed to develop an established treatment algorithm in this patient population.
Ethics Committee Approval: The study protocol was approved by the Kartal Kosuyolu High Specialization Training and Research Hospital Clinical Research Ethics Committee (date: 09.02.2021, no: 2016-KAEK-112-475). The study was conducted in accordance with the principles of the Declaration of Helsinki.
Patient Consent for Publication: A written informed consent was obtained from each patient.
Data Sharing Statement: The data that support the findings of this study are available from the corresponding author upon reasonable request.
Author Contributions: Idea/concept,design, data collection and processing, literature review, writing the article: V.B.; Idea/concept,design, control/supervision, data collection and processing, analysis and interpretation, literature review, writing the article, critical review, references, materials: N.O.E.; Idea/concept, design, control/supervision, writing the article, critical review: Ş.O.Y.; Data collection and processing, analysis and interpretation, writing the article: E.B.; Data collection and processing, analysis and interpretation, writing the article, critical review: Ö.E.; Control/supervision, writing the article, critical review: B.M.; Idea/concept,design, control/ supervision, writing the article, critical review: D.K.; Data collection and processing, analysis and interpretation, writing the article: G.N.B.; Odea/concept,design, data collection and processing, literature review, writing the article: S.T.; Control/ supervision, writing the article, critical review: H.S.; Odea/ concept,design, data collection and processing, literature review, writing the article: K.A.; Control/supervision, writing the article, critical review: S.K.; Idea/concept,design, control/ supervision, data collection and processing, analysis and interpretation, literature review, writing the article, critical review, references, materials: B.Y.
Conflict of Interest: The authors declared no conflicts of interest with respect to the authorship and/or publication of this article.
Funding: The authors received no financial support for the research and/or authorship of this article.
1) Deng L, Zhu J, Xu J, Guo S, Liu S, Song Y. Clinical
presentation and surgical treatment of primary pulmonary
artery sarcoma. Interact Cardiovasc Thorac Surg 2018;26:243-7. doi: 10.1093/icvts/ivx318.
2) Mandelstam M. Über primäre Neubildungen des Herzens.
Virchows Arch 1923;245:43-54.
3) Barmpas A, Giannakidis D, Fyntanidou V, Koulouris C,
Mantalobas S, Pavlidis E, et al. Intimal sarcoma of the
pulmonary artery, a diagnostic enigma. AME Case Rep
2019;3:32. doi: 10.21037/acr.2019.07.02.
4) Simonneau G, Montani D, Celermajer DS, Denton CP, Gatzoulis
MA, Krowka M, et al. Haemodynamic definitions and updated
clinical classification of pulmonary hypertension. Eur Respir J
2019;53:1801913. doi: 10.1183/13993003.01913-2018.
5) Yıldızeli B, Taş S, Yanartaş M, Kaymaz C, Mutlu B,
Karakurt S, et al. Pulmonary endarterectomy for chronic
thrombo-embolic pulmonary hypertension: An institutional
experience. Eur J Cardiothorac Surg 2013;44:e219-27. doi:10.1093/ejcts/ezt293.
6) Coskun U, Sinan UY, Calpar I, Yildizeli B, Yanartas M,
Filinte D, et al. Pulmonary artery sarcoma masquerading
as chronic pulmonary thromboembolism. Tex Heart Inst J
2014;41:518-22. doi: 10.14503/THIJ-13-3598.
7) Bandyopadhyay D, Panchabhai TS, Bajaj NS, Patil PD,
Bunte MC. Primary pulmonary artery sarcoma: A close
associate of pulmonary embolism-20-year observational
analysis. J Thorac Dis 2016;8:2592-601. doi: 10.21037/
jtd.2016.08.89.
8) Mussot S, Ghigna MR, Mercier O, Fabre D, Fadel E, Le
Cesne A, et al. Retrospective institutional study of 31 patients
treated for pulmonary artery sarcoma. Eur J Cardiothorac
Surg 2013;43:787-93. doi: 10.1093/ejcts/ezs387.
9) Yi CA, Lee KS, Choe YH, Han D, Kwon OJ, Kim S. Computed
tomography in pulmonary artery sarcoma: Distinguishing
features from pulmonary embolic disease. J Comput Assist
Tomogr 2004;28:34-9. doi: 10.1097/00004728-200401000-
00005.
10) Lee EJ, Moon SH, Choi JY, Lee KS, Choi YS, Choe YS,
et al. Usefulness of fluorodeoxyglucose positron emission
tomography in malignancy of pulmonary artery mimicking
pulmonary embolism. ANZ J Surg 2013;83:342-7. doi:10.1111/j.1445-2197.2012.06205.x.
11) Soft tissue and bone tumours. WHO Classification of
Tumours. 5th ed. Vol. 3. Lyon: International Agency for
Research on Cancer; 2020.
12) Cox JE, Chiles C, Aquino SL, Savage P, Oaks T. Pulmonary
artery sarcomas: A review of clinical and radiologic
features. J Comput Assist Tomogr 1997;21:750-5. doi:10.1097/00004728-199709000-00018.
13) Keel SB, Bacha E, Mark EJ, Nielsen GP, Rosenberg AE.
Primary pulmonary sarcoma: A clinicopathologic study of
26 cases. Mod Pathol 1999;12:1124-31.
14) Mattoo A, Fedullo PF, Kapelanski D, Ilowite JS. Pulmonary
artery sarcoma: A case report of surgical cure and 5-year
follow-up. Chest 2002;122:745-7. doi: 10.1378/chest.122.2.745.
15) Burke AP, Virmani R. Sarcomas of the great vessels.
A clinicopathologic study. Cancer 1993;71:1761-73.
doi: 10.1002/1097-0142(19930301)71:5<1761::aidcncr2820710510>
3.0.co;2-7.
16) Nonomura A, Kurumaya H, Kono N, Nakanuma Y, Ohta G,
Terahata S, et al. Primary pulmonary artery sarcoma. Report
of two autopsy cases studied by immunohistochemistry and
electron microscopy, and review of 110 cases reported in
the literature. Acta Pathol Jpn 1988;38:883-96. doi: 10.1111/
j.1440-1827.1988.tb02360.x.
17) Akram K, Silverman ME, Voros S. A unique case of
pulmonary artery leiomyosarcoma. J Natl Med Assoc
2006;98:1995-7.
18) Grazioli V, Vistarini N, Morsolini M, Klersy C, Orlandoni
G, Dore R, et al. Surgical treatment of primary pulmonary
artery sarcoma. J Thorac Cardiovasc Surg 2014;148:113-8.
doi: 10.1016/j.jtcvs.2013.07.054.
19) Jamieson SW. Pulmonary artery sarcoma. Eur J Cardiothorac
Surg 2013;43:793-4. doi: 10.1093/ejcts/ezs362.
20) Yin K, Zhang Z, Luo R, Ji Y, Zheng D, Lin Y, et al. Clinical
features and surgical outcomes of pulmonary artery sarcoma.
J Thorac Cardiovasc Surg 2018;155:1109-15.e1. doi: 10.1016/j.
jtcvs.2017.10.101.
21) Xu L, Lu W, Li J, Wang C. Additional treatment prolonged
survival of pulmonary artery sarcoma after surgical
resection. Transl Cancer Res 2020;9:2618-26. doi: 10.21037/
tcr.2020.02.80.