Published online Dec 24, 2021. doi: 10.5306/wjco.v12.i12.1157
Peer-review started: April 28, 2021
First decision: June 16, 2021
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Accepted: November 25, 2021
Article in press: November 25, 2021
Published online: December 24, 2021
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Primary vascular tumours of the kidney are rare and may pose diagnostic difficulties because of their similar clinical, morphological, and immunohistochemical features. This article summarizes the clinical and pathological features of primary renal angiosarcoma and anastomosing haemangioma of the kidney including epidemiology, genetics, and prognosis. Renal anastomosing haemangiomas are benign neoplasms characterized by anastomosing capillary-sized vascular channels. These tumours are rare, with about 75 cases reported in the literature. Most anastomosing haemangiomas are found incidentally on ultra
Primary renal angiosarcomas are malignant tumours showing endothelial differentiation. To date, 76 cases have been described in the literature. Primary renal angiosarcomas are frequently symptomatic. The clinical features of renal an
Core Tip: Primary vascular tumours of the kidney are extremely rare. This article summarizes the clinical and pathological features of primary renal angiosarcoma and anastomosing haemangioma of the kidney.
- Citation: Omiyale AO. Primary vascular tumours of the kidney. World J Clin Oncol 2021; 12(12): 1157-1168
- URL: https://www.wjgnet.com/2218-4333/full/v12/i12/1157.htm
- DOI: https://dx.doi.org/10.5306/wjco.v12.i12.1157
Although vascular tumours are relatively common in the skin and soft tissue, they are extremely rare in the kidney, ranging from benign to malignant neoplasms that may be diagnostically challenging because of the overlapping clinical, morphological and immunohistochemical features.
These tumours include renal angiosarcomas and renal haemangiomas. Various subtypes of haemangioma have been described in the kidney including cavernous, capillary, and anastomosing haemangiomas[1-4]. However, the most common subtype is anastomosing haemangioma[1,2,5].
This article provides an overview of the clinical and pathological features of anastomosing haemangioma of the kidney and primary angiosarcoma of the kidney, and discusses the epidemiology, genetics, and prognosis.
Renal anastomosing haemangiomas are benign neoplasms characterized by anasto
The aetiology and risk factors for renal anastomosing haemangiomas are unknown. Some cases have been reported in the setting of end stage renal disease[11,12].
The vast majority of anastomosing haemangiomas are found incidentally on radiological evaluation for other purposes. Common symptoms include abdominal pain, haematuria, and abdominal mass[5,10].
The imaging findings are non-specific. On computed tomography, these tumours are often circumscribed, hyperdense, and heterogeneous due to fatty or non-enhancing hypodense areas and show post-contrast enhancement[13].
Renal anastomosing haemangiomas are characterized by recurrent mutations in GNAQ and GNA14 genes[14,15]. GNAQ gene encodes guanine nucleotide-binding protein G (q) subunit alpha (Gαq protein) that activates signalling pathways that regulates cell proliferation, survival, development, and function of blood vessels[14-16].
Grossly, anastomosing haemangiomas are typically small ranging from 0.1 cm to 12 cm (mean, 2.2 cm)[5,10,17]. These tumours are often well-demarcated spongy maho
Histologically, anastomosing haemangiomas consist of anastomosing capillary-sized blood vessels, reminiscent of splenic sinusoids. The blood vessels are lined by bland endothelial cells. Typically, these tumours lack endothelial cell multilayering, papillary tufting, cytologic atypia, necrosis, and prominent mitotic figures. They may show extramedullary haematopoiesis, hyaline globules, and mild lymphocytic infil
Rarely, renal anastomosing haemangiomas may infiltrate perinephric fat, renal sinus fat[2,12], and the renal vein or its segmental branches[2,12,18,19]. The neoplastic cells are immunoreactive for CD31, CD34, ERG, FLI1, and factor VIII-related antigen (now rarely used)[5].
Renal anastomosing haemangiomas may co-exist with other renal neoplasms such as metanephric adenoma, papillary adenoma, papillary renal cell carcinoma, acquired cystic disease-associated renal cell carcinoma, and clear cell renal cell carcinoma[11,12].
Most patients with renal anastomosing haemangioma, described in the literature, were treated with radical nephrectomy, reflecting a tendency to overtreat these patients, probably because of inaccurate preoperative diagnosis (Table 1).
Ref. | Treatment | Follow-up (mo) | Outcome |
Bean et al[14] | Nephrectomy | 9 | NED |
Bean et al[14] | Nephrectomy | 84 | NED |
Bean et al[14] | Nephrectomy | 107 | NED |
Memmedoğlu and Musayev[41] | Nephrectomy | 12 | NED |
Memmedoğlu and Musayev[41] | Nephrectomy | 12 | NED |
Tahir and Folwell[42] | Nephrectomy | 1 | NED |
Pantelides et al[6] | Nephrectomy | 6 | NED |
Downes et al[7] | Nephrectomy | NA | NA |
Downes et al[7] | Biopsy | NA | NA |
Chandran et al[8] | Nephrectomy | NA | NA |
Cha et al[9] | Nephrectomy | 5 | NED |
Montgomery and Epstein[2] | Nephrectomy | 12 | NED |
Montgomery and Epstein[2] | Nephrectomy | 36 | NED |
Montgomery and Epstein[2] | Nephrectomy | NA | NA |
Montgomery and Epstein[2] | Excision | 8 | NED |
Heidegger et al[43] | Nephrectomy | 156 | NED |
Kryvenko et al[12] | Nephrectomy | NA | NA |
Kryvenko et al[12] | Nephrectomy | NA | NA |
Kryvenko et al[12] | Nephrectomy | NA | NA |
Kryvenko et al[12] | Nephrectomy | NA | NA |
Kryvenko et al[12] | Nephrectomy | NA | NA |
Kryvenko et al[12] | Nephrectomy | NA | NA |
Kryvenko et al[12] | Nephrectomy | NA | NA |
Kryvenko et al[12] | Nephrectomy | NA | NA |
Kryvenko et al[12] | Nephrectomy | NA | NA |
Kryvenko et al[12] | Nephrectomy | NA | NA |
Kryvenko et al[12] | Nephrectomy | NA | NA |
Kryvenko et al[12] | Nephrectomy | NA | NA |
Al-Maghrabi and Al-Rashed[44] | Partial nephrectomy | 12 | NED |
Caballes et al[17] | Nephrectomy | 18 | NED |
Büttner et al[11] | Nephrectomy | NA | NA |
Büttner et al[11] | Nephrectomy | NA | NA |
Büttner et al[11] | Nephrectomy | NA | NA |
Büttner et al[11] | Nephrectomy | NA | NA |
Büttner et al[11] | Nephrectomy | NA | NA |
Büttner et al[11] | Nephrectomy | NA | NA |
Büttner et al[11] | Nephrectomy | NA | NA |
Büttner et al[11] | Nephrectomy | NA | NA |
Lee et al[45] | Nephrectomy | NA | NA |
Zhao et al[46] | Nephrectomy | 12 | NED |
Kryvenko et al[18] | Nephrectomy | 7 | NED |
Kryvenko et al[18] | Nephrectomy | 6 | NED |
Kryvenko et al[18] | Nephrectomy | 3 | NED |
Kryvenko et al[18] | Nephrectomy | 122 | NED |
Tao et al[47] | Nephrectomy | 21 | NED |
Abboudi et al[48] | Nephrectomy | <1 | NED |
Silva et al[49] | Resection | NA | NA |
Berker et al[50] | Partial nephrectomy | 10 | NED |
Berker et al[50] | Nephrectomy | 4 | NED |
O'Neill et al[13] | NA | NA | NA |
O'Neill et al[13] | NA | NA | NA |
O'Neill et al[13] | NA | NA | NA |
O'Neill et al[13] | NA | NA | NA |
O'Neill et al[13] | NA | NA | NA |
O'Neill et al[13] | NA | NA | NA |
O'Neill et al[13] | NA | NA | NA |
Brown et al[1] | Nephrectomy | 72 | NED |
Brown et al[1] | Nephrectomy | 24 | NED |
Brown et al[1] | Partial nephrectomy | NA | NA |
Brown et al[1] | Nephrectomy | 24 | NED |
Brown et al[1] | Nephrectomy | NA | NA |
Perdiki et al[51] | Partial nephrectomy | 25 | NED |
Perdiki et al[51] | Nephrectomy | 14 | NED |
Wetherell et al[52] | Nephrectomy | 1 | DFUD |
Manohar et al[53] | Nephrectomy | 24 | NED |
Omiyale et al[19] | Nephrectomy | 10 | NED |
Johnstone et al[54] | Nephrectomy | NA | NA |
Mehta et al[4] | Nephrectomy | 3 | NED |
Mehta et al[4] | Nephrectomy | 12 | NED |
Mehta et al[4] | Nephrectomy | 3 | NED |
Tran and Pernicone[55] | Nephrectomy | NA | NA |
Zhang et al[56] | Partial nephrectomy | 16 | NED |
Cheon et al[57] | Nephrectomy | 6 | NED |
Chou et al[58] | Nephrectomy | 8 | NED |
Chou et al[58] | Nephrectomy | 14 | NED |
The prognosis of anastomosing haemangioma is excellent with no evidence of recurrence, metastasis or tumour-related death at an average follow-up of 24.8 mo (range, < 1-156 mo) (Table 1).
Renal angiosarcomas are malignant tumours showing endothelial differentiation. These tumours are very rare, with about 76 cases described in the literature as case series and reports[20-24]. There is a male-to-female ratio of 6:1, with patient age ranging from 24 years to 95 years (median, 62 years).
Although angiosarcomas arising in other anatomical sites have been associated with risk factors such as exposure to thorium dioxide, arsenic-based pesticides, polyvinyl chloride, and radiation therapy particularly for breast, endometrial and prostate cancers[25-27], no specific aetiology or risk factors have been established for primary angiosarcoma of the kidney[20,28].
The clinical features of renal angiosarcomas are identical to those of renal ana
Computed tomography imaging shows large masses with heterogeneous enhan
Angiogenesis-related genes and vascular-specific receptor tyrosine kinases such as KDR, TIE1, SNRK, TEK, and FLT1, are upregulated in angiosarcomas[31]. High-level MYC gene amplifications are seen in most radiation-induced and chronic lympho
Some primary angiosarcomas, typically in young adults, have recurrent CIC gene rearrangements, with or without concurrent CIC mutations, and are characterized by upregulation of CIC-target genes including ETV1, ETV4, and ETV5[34]. Angiosar
Primary renal angiosarcomas are usually large ranging from 3.6 cm to 30 cm (mean, 13 cm). Typically, they are ill-defined haemorrhagic spongy masses with necrosis[1,20].
Microscopically, these tumours range from well-formed vasoformative areas to areas with solid morphology showing sparse vasoformation. These patterns are often mixed within the same tumour. Vasoformative areas are composed of small to medium-sized anastomosing blood vessels, lined by epithelioid and/or spindled endothelial cells showing nuclear pleomorphism, endothelial papillary tufting, multilayering, intraluminal budding, and hobnailing[1,20,28]. Solid areas consist of sheets of malignant epithelioid and/or spindled cells with subtle vasoformation, cytologic atypia, and mitotic figures. Necrosis may be present. Angiosarcomas usually have a haemorrhagic background and extravasated red blood cells are seen within the tumour[1,20,28].
Epithelioid angiosarcomas are composed of sheets of large atypical polygonal or epithelioid cells with nuclear pleomorphism, high nuclear to cytoplasmic ratio, prominent central nucleoli, mitotic figures, and moderate amounts of cytoplasm. Epithelioid angiosarcomas may be mistaken for carcinoma, melanoma, or lymphoma[20,28,35-37].
The neoplastic cells are positive for CD31, ERG, FLI1, CD34, and factor VIII-related antigen[20,28,38,39]. Epithelioid angiosarcomas may be positive for epithelial markers including CK7, Cam5.2, AE1/AE3, and EMA, which may lead to a misdiagnosis of carcinoma[20].
Similar to angiosarcomas arising at other locations, renal angiosarcomas have a tendency for widespread metastasis at diagnosis or afterwards in the course of the disease. Approximately 66% of patients develop metastases, most commonly to the lung and liver. Other sites of metastasis include bone, lymph nodes, peritoneum, small bowel, soft tissue, and skin. Currently, there are no specific standardized treatment guidelines for primary renal angiosarcomas. These tumours are treated with radical nephrectomy, chemotherapy, radiotherapy, or targeted therapy (Table 2).
Ref. | Treatment | Follow-up (mo) | Outcome |
Costero-Barrios et al[59] | Nephrectomy, Chemo, RT | 12 | AWD |
Peters et al[60] | Nephrectomy | 2 | DOD |
Singh et al[35] | NA | NA | NA |
Kern et al[61] | Nephrectomy | 3 | DOD |
Kern et al[61] | Nephrectomy | 1.5 | DOD |
Aydogdu et al[62] | Nephrectomy | NA | NA |
Akkad et al[63] | Nephrectomy | 30 | NED |
Witczak et al[64] | nephrectomy | NA | NA |
Chaabouni et al[38] | Nephrectomy | 1 | DOD |
Johnson et al[65] | Rapid deterioration | NA | DOD |
Zenico et al[66] | Nephrectomy | 4 | DOD |
Nguyen et al[67] | Nephrectomy, Chemo | 18 | DOD |
Terris et al[68] | Nephrectomy, RT | 10 | DOD |
Matter et al[69] | Nephrectomy, Chemo, RT | 18 | DOD |
Yoshida et al[70] | Nephrectomy, Recombinant IL-2 | 13 | DOD |
Pauli and Strutton[71] | Nephrectomy, RT | 2 | DOD |
Martínez-Piñeiro et al[72] | Nephrectomy, S | 4 | DOD |
Bernstein et al[73] | NA | NA | NA |
Liu et al[36] | Nephrectomy, RT | 6 | NED |
Yau et al[74] | Nephrectomy, Chemo, RT | 3 | DOD |
Carnero López et al[75] | Nephrectomy, Chemo | 5 | DOD |
Kazaz et al[76] | Nephrectomy, Chemo | NA | NA |
Souza et al[77] | Nephrectomy | 1 | DFUD |
Detorakis et al[78] | Nephrectomy, Chemo | 11 | DOD |
Komoto et al[79] | Nephrectomy | 9.2 | DOD |
Boni et al[80] | Nephrectomy, Chemo | 15 | DOD |
Chang et al[81] | Nephrectomy, Chemo, RT | NA | NA |
Iannaci et al[82] | Nephrectomy | NA | DOD |
Subramanian et al[83] | Nephrectomy | NA | NA |
Waqas et al[84] | Nephrectomy, Chemo | NA | NA |
Gourley et al[85] | Nephrectomy | NA | DOD |
Su[86] | Nephrectomy, Chemo | NA | DOD |
López Cubillana et al[87] | Nephrectomy, Chemo | 5 | DOD |
Juan et al[88] | Nephrectomy, Chemo, RT | 9 | DOD |
Prince[21] | Nephrectomy, RT | NA | A and W |
Sesar et al[22] | Nephroureterectomy | NA | NA |
Testa et al[23] | Nephrectomy | 27 | DFUD |
Xuan[24] | Nephrectomy | NA | NA |
Brown et al[1] | NA | 6 | DOD |
Brown et al[1] | NA | 11 | DOD |
Brown et al[1] | NA | 1 | DOD |
Brown et al[1] | NA | NA | NA |
Brown et al[1] | NA | 1 | DOD |
Brown et al[1] | Nephrectomy | NA | NA |
Brown et al[1] | Nephrectomy | NA | NA |
Brown et al[1] | Nephrectomy | 2 | DFUD |
Hiratsuka et al[89] | Nephrectomy | 29 | NED |
Adjiman et al[90] | Nephrectomy | NA | DOD |
Limmer et al[91] | Nephrectomy | 1 | DOD |
Darlington et al[92] | Nephrectomy, Chemo | 12 | NED |
Allred et al[93] | Nephrectomy, Chemo | 3 | DOD |
Fukunaga et al[94] | Nephrectomy | 13 | DOD |
Desai et al[95] | Nephrectomy, Chemo | 4 | DOD |
Sabharwal et al[96] | Nephrectomy, Chemo | >1 | NA |
Aksoy et al[29] | Nephrectomy, S | 3 | DOD |
Heo et al[97] | Nephrectomy | NA | NA |
Mordkin et al[98] | Nephrectomy, Chemo, S | NA | NA |
Berretta et al[99] | Nephrectomy, Chemo | 8 | DOD |
Lodhi et al[100] | Chemo | NA | AWD |
Cason et al[101] | Nephrectomy, RT | 10 | DOD |
Askari et al[102] | Nephrectomy | 4 | DOD |
Guan et al[103] | Nephrectomy, Chemo | 4 | DOD |
Papadimitriou et al[104] | Nephrectomy | NA | A and W |
Celebi et al[105] | Nephrectomy, Chemo, TKI, VEGF Inhibitor | 13 | DOD |
Rüb et al[106] | Nephrectomy, Chemo | 12 | AWD |
Zhang et al[107] | Nephrectomy | NA | NA |
Tsuda et al[108] | Nephrectomy | 21 | DOD |
Grapsa et al[109] | NA | NA | NA |
Li et al[37] | NA | NA | NA |
Qayyum et al[110] | Palliative (patient's decision) | NA | NA |
Leggio et al[30] | Nephrectomy | 8 | DOD |
Garmendia et al[111] | Nephrectomy | NA | NA |
Sanyal et al[112] | Nephrectomy, RT | 24 | DOD |
Cerilli et al[113] | Nephrectomy, RT | 6 | DOD |
Douard et al[114] | Nephrectomy | 3 | DOD |
Yamamoto et al[115] | Nephrectomy, RT | 19 | NED |
Primary renal angiosarcomas are highly aggressive neoplasms with 76.3% of patients dying of tumour within 1 mo to 24 mo (mean, 7.5 mo), despite surgical and adjuvant therapy (Table 2). Poor prognostic factors for angiosarcomas occurring at other anatomic sites include age > 69 years, tumour size ≥ 5 cm, regional disease (vs localized disease), non-surgical treatment, and distant metastasis[40].
Primary vascular tumours of the kidney are rare neoplasms. Unlike primary renal angiosarcoma, the prognosis of renal anastomosing haemangioma is excellent with no evidence of recurrence or metastasis. These tumours share similar clinical, morphological and immunohistochemical features, and must be distinguished from each other. Features that favour angiosarcomas include the presence of malignant spindled and/or epithelioid cells with a variable degree of vasoformation, cytologic atypia, prominent mitotic figures, endothelial multilayering, papillary tufting, and necrosis.
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