Renal cell carcinomaC64

Last updated on: 23.02.2021

Dieser Artikel auf Deutsch

Requires free registration (medical professionals only)

Please login to access all articles, images, and functions.

Our content is available exclusively to medical professionals. If you have already registered, please login. If you haven't, you can register for free (medical professionals only).


Requires free registration (medical professionals only)

Please complete your registration to access all articles and images.

To gain access, you must complete your registration. You either haven't confirmed your e-mail address or we still need proof that you are a member of the medical profession.

Finish your registration now

HistoryThis section has been translated automatically.

Grawitz was the first to describe clear cell renal carcinoma in 1883, which has since also been referred to as "Grawitz tumor". In the 19th century, terms such as "hypernephroma" and "hypernephroid carcinoma" appeared, which are now considered obsolete (Wittig 2012). Robson was the first to describe radical nephrectomy as a curative procedure for localized renal cell carcinoma in 1969 (Doehn 2020).

DefinitionThis section has been translated automatically.

Renal cell carcinoma (RCC or RCC) is a heterogeneous group of tumors that have specific histopathological, genetic and clinical characteristics. They can be benign or highly malignant and occur unilaterally or bilaterally (Kasper 2015).

ClassificationThis section has been translated automatically.

The classification of RCC is based on histopathological criteria and molecular characteristics according to the WHO of 2016 (Ahrens 2020) and is divided as follows:

  • Clear cell renal cell carcinoma: It represents the most common type of tumor with 60 % - 70 %.
  • Papillary carcinoma: This occurs in 5 % - 15 % and tends to multifocal and bilateral involvement of the kidneys.
  • Chromophobe carcinoma: Chromophobe carcinoma is found in 5 % - 10 % of cases and is characterized by an inconspicuous clinical course.
  • Oncocytoma: This is also rare with 5 % - 10 % and is considered to be rather benign. It can also occur as a hybrid tumour together with a chromophobe carcinoma. Oncocytomas can also be precursors of a chromophobe carcinoma (Kraus 2014).
  • Ductal Bellini carcinoma: Ductal Bellini carcinoma (also known as collecting duct carcinoma) is very rare (< 1%) and highly aggressive (Kasper 2015).

Described as a separate tumor entity in previous WHO classifications:

  • Medullary carcinoma: Medullary carcinoma occurs very rarely and is highly aggressive (Golbeck 2013). It is found exclusively in patients with sickle cell disease (Herold 2020).
  • Multilocular cystic renal cell carcinoma: This tumor shows a close association with clear cell RCC (see above). It is only mildly malignant. Metastatic cases have not been reported so far (Golbeck 2013).

An additional classification is the Vancouver classification of the International Society of Urological Pathology (ISUP). It applies in particular to new categories of epithelial tumors such as:

  • tubulocystic renal cell carcinoma
  • papillary renal cell carcinoma (type 1 and type 2)
  • clear cell renal cell carcinoma
  • translocation-associated renal cell carcinoma
  • renal cell carcinoma associated with acquired cystic kidney disease
  • Renal cell carcinoma associated with hereditary leiomyomatosis (Doehn 2020)

Tumor classification

RCC are classified as follows according to the Union for International Cancer Control (UICC) 2017:

T 0: Primary tumor not detectable.

  • T 1: Tumor up to 7 cm in size and confined to the kidney.
  • T 1 a: < 4 cm in size
  • T 1 b: 4 - 7 cm in size
  • T 2 a: tumour > 7 cm - 10 cm
  • T 2 b: > 10 cm in size
  • T 3 a: Invasion of the renal vein or infiltration perirenally
  • T 3 b: Invasion of the V. cava below the diaphragm
  • T 3 c: Invasion of the vena cava above the diaphragm
  • T 4: Breakthrough of the Gerota fascia

  • N 0: No evidence of lymph node metastasis
  • N 1: Evidence of metastasis in 1 regional lymph node
  • N 2: Evidence of metastasis in > than 1 lymph node

  • M 0: No evidence of distant metastases
  • M 1: Evidence of distant metastases

TNM- stage classification of the Union for International Cancer- Control = UICC, 2010):

Stage I: T1 N0 M0

Stage II: T2 N0 M0

Stage III: T1 N1 M0

or: T2 N1 M0

or: T3 N0 M0

or: T3 N1 M0

Stage IV: T1 N2 M0

or: T2 N2 M0

or: T3 N2 M0

or: T4 N0 M0

or: T4 N1 M0

or: T4 N2 M0

or: any T, any N, M1

Venous invasion in RCC: There are four different levels:

  • Level I: The tumor reaches the renal vein.
  • Level II: The tumor reaches the v. cava below the liver.
  • Level III: The tumor extends below the diaphragm into the intrahepatic vena cava. A two-cavity operation is necessary to squeeze out the tumor.
  • Level IV: A tumor thrombus is found above the diaphragm. This requires a two-cavity procedure with a heart-lung machine. (Manski 2020)

Occurrence/EpidemiologyThis section has been translated automatically.

Renal cell carcinoma accounts for approximately 2 % - 4 % of all malignant neoplasms in adults (Delecluse 2020) and represents the most common malignant kidney tumour in adults, accounting for 90 % (Manski 2020).

As a rule, RCC grows unilaterally, but can also be present bilaterally in 1% (Herold 2020).

Medullary RCC is found on the right side in approximately 75 % of those affected (Golbeck 2013).

EtiopathogenesisThis section has been translated automatically.

The cause of RCC is as yet unknown. However, several risk factors are known to promote disease. These include:

  • Smoking (2 x higher risk (Keller 2010)
  • secondary renal cysts in chronic renal insufficiency (this increases the risk by a factor of 30 [Keller 2020])
  • terminal renal failure
  • tuberous sclerosis (autosomal dominant inherited phakomatosis [Pantelis 2007])

(Kasper 2015)

  • Analgesic- nephropathy due to several years of use of mixed analgesics or NSAIDs (with the exception of ASA).

(Wolf 2020)

A familial cluster is found in about 4% of all RCC. For first- or second-degree relatives, the risk of also developing RCC increases by a factor of 2 - 4 (Doehn 2020).

PathophysiologyThis section has been translated automatically.

RCC originates from the epithelium of various nephron segments of the mature renal parenchyma (Manski 2020):

  • clear cell renal cell carcinoma from the proximal tubule
  • papillary RCC from proximal tubule
  • oncocytoma from the cortical collecting tube
  • chromophobic carcinoma also from the cortical collecting tube
  • Ductus Bellini carcinoma from the medullary collecting duct in the renal medulla (Kasper 2015).

Germline mutations can be detected in 1% - 4% of all RCC.

Currently, four molecularly defined syndromes are known to be associated with an increased risk of developing RCC:

[Doehn 2020)

In addition, in:

  • CNS- Hemangioblastoma (rare benign tumor of the posterior fossa or other parts of the nervous system [Dützmann 2018]).
  • Angiomatosis retinae (Herold 2020).

ManifestationThis section has been translated automatically.

RCC can occur at any age, but the incidence increases significantly with age (Kasper 2015). An exception is medullary RCC, the average age of which is 19 years (Golbeck 2013).

The male sex is affected twice as often as the female sex (Kasper 2015).

The peak age of disease is 68 years for men and 71 years for women (Doehn 2020).

Clinical featuresThis section has been translated automatically.

The leading clinical symptoms of RCC are:

Haematuria : Haematuria is found in about 60% of all patients. It is caused by a herniation of the renal pelvis, which occurs relatively early in RCC (Herold 2020).

Abdominal pain: occurs in about 40 % (Herold 2020).

Palpable tumour in the flank area: If the tumour is already palpable, it is usually inoperable (Herold 2020).

However, these typical symptoms exist in only 10 % - 20 % of patients. Further symptoms can be:

  • unclear fever
  • weight loss
  • Anemia

varicocele, especially of the left testis (if it breaks into the left renal vein (Kasper 2015)

paraneoplastic syndromes: they are caused by tumor-induced hormone production, such as

  • hypertension (due to renin)
  • hypercalcemia (due to parathyroid hormone-related protein = PTHrP)
  • Polyglobulia (due to erythropoietin)
  • Stauffer's syndrome (liver dysfunction caused by the tumor with increased AP)

The above-mentioned symptoms usually occur only facultatively or only at a late stage.

Initially, the symptoms are mostly unspecific or rather point to a systemic disease. This is why RCC is also referred to as the "urological chameleon" (Ganten 2002). However, most RCC (60 % - 70 %) are still discovered as an incidental finding during sonography, as no typical symptoms are present in the early stages. (Herold 2020)

Metastasis: Ifmetastasis has already occurred, the following symptoms may also exist, for example:

  • Icterus
  • Cough
  • Dyspnoea
  • bone pain
  • neurological deficits (Manski 2020)

DiagnosticsThis section has been translated automatically.

Inspection and physical examination

  • sometimes palpable, respiratory displaceable abdominal mass at the lower renal pole
  • mainly left-sided varicocele which does not empty when the patient is lying down (Keller 2010)
  • arterial hypertension (Herold 2020)

ImagingThis section has been translated automatically.

Sonography: Tumours with a diameter of approx. 2 cm or more can be visualised by sonography (Keller 2010).

Benign tumours, such as angiomyolipoma, are increasingly presented echogenically as a smoothly delineated mass, whereas renal cell carcinoma and oncocytoma both show an inhomogeneous echo pattern (Kuhlmann 2015).

Visualization of possible metastases to the liver (Manski 2020).

Further investigations should be performed to clarify the dignity of the tumor and metastases (see below). (Keller 2010)

Color duplex sonography: In RCC, a basket-like displacement of the intrarenal vessels can be visualized, which is also referred to as a so-called parenchymal hump or pseudotumor (Keller 2010).

Chest X-ray: A chest X-ray should be performed to exclude pulmonary metastases. If tumors > 3 cm are found or if pulmonary symptoms exist, a chest CT is recommended for further diagnosis (Manski 2020).

CT abdomen. CT can be used to:

  • the renal function of the opposite side can be assessed
  • a lymphadenopathy of > 1 cm indicates a lymphogenic metastasis (Manski 2020)
  • For the planning of organ-preserving surgery, the vascularisation of the tumour can be visualised with the aid of contrast medium:
    • papillary renal cell carcinoma is less vascularized
    • the clear cell tumor is stronger
    • a benign tumor presents hypo- or avascular (Kuhlmann 2015).

CT- Thorax: In case of radiological evidence of > 3 cm pulmonary metastases or pulmonary symptoms, a CT of the thorax should be performed (Manski 2020).

MRI: According to the guideline, an additional MRI should always be performed if the tumor shows vein involvement or protrudes into the inferior vena cava, as an MRI can be used to more accurately assess tumor extension (Doehn 2020).

Accurate determination of invasion is important for surgical planning (Manski 2020). The exact staging s. b. Venous invasion in RCC under "Classification."

In addition, MRI is required in patients with known contrast allergy (Kuhlmann 2015).

Cranial MRI: Cranial MRI should be performed in cases of suspected brain metastases (Manski 2020).

Bone scintigraphy: Bone scintigraphy is indicated in:

  • advanced RCC
  • elevated AP
  • Bone pain
  • Evidence of other metastases (Manski 2020).

Fine-needle biopsy: A preoperative fine-needle biopsy should be performed as a punch-cylinder biopsy under ultrasound or CT control if it would influence the choice of therapy (Doehn 2020). This may be the case, for example, in the presence of:

  • Renal abscess
  • Lymphoma
  • metastases
  • before systemic therapy in advanced stages of the disease. If there is no histopathological finding so far, a biopsy from the primarius or from the metastasis is recommended (Doehn 2020). (Manski 2020)

Biopsy of cystic tumors is considered contraindicated because the probability of detecting the solid portions (and thus the possibility of excluding a malignant tumor) in a cystic tumor is too low (Doehn 2020).

False negative histology is found in 5%-15% (Manski 2020).

LaboratoryThis section has been translated automatically.

The following laboratory abnormalities may exist in RCC:

  • Anemia
  • Erythrocytosis (found in about 3% at the time of initial diagnosis) (Kasper 2015).
  • Thrombocytosis
  • Hypercalcemia
  • Liver dysfunction (also without liver metastases as so-called "Stauffer syndrome", see above "Clinical picture" [Herold 2020])
  • Increase in alkaline phosphatase
  • Disorders of hormone balance (e.g. erythropoietin, glucagon, PTHrP, renin, ACTH-like hormone, gonadotropins, insulin) (Keller 2010)
  • increased inflammation values
  • impaired blood coagulation (Manski 2020)

To date, there are no molecular markers in RCC that could provide evidence of metastasis (Doehn 2020).

Differential diagnosisThis section has been translated automatically.

Differential diagnosis of hematuria:

Differential diagnosis to renal tumor are e.g.:

  • inflammatory tumors:
  • Tumors of immature renal parenchyma:
  • Tumors of mature renal parenchyma:
    • adenoma
  • Tumors of the renal pelvis:
    • Papilloma
    • Urothelial carcinoma
    • Adenocarcinoma
    • Squamous cell carcinoma
    • cystic kidney tumours
  • renal tumors of the vascular system:
    • Hamartoma
    • Hemangioma
    • Lymphangioma
    • Angiomyolipoma
  • Mesenchymal renal tumors:
    • Fibroma
    • Fibrosarcoma
    • Lipoma
    • Liposarcoma
    • Leiomyoma
    • Leiomyosarcoma
  • Renal tumors of the nervous system:
    • Neuroblastoma
    • Schwannoma
    • Sympathicoblastoma
  • perirenal tumors:
    • retroperitoneal sarcoma
    • Lymphoma
    • Neuroblastoma
    • Lymph node metastasis (e.g. from testicular tumours)
    • Teratoma
  • renal metastases from:
    • Bronchial carcinoma
    • breast carcinoma
    • gastrointestinal carcinoma
    • malignant melanoma
    • lymphoma (Manski 2020)

Complication(s)This section has been translated automatically.

Metastases

Hematogenous metastasis occurs primarily - usually first to the lungs - and then to the bones, adrenal gland, liver and CNS.

Lymphogenic metastasis occurs via the regional lymph nodes, the cysterna chyli or the thoracic duct, followed by local metastasis (Keller 2010).

Metastases of renal cell carcinoma are often found in the following area:

  • lung and mediastinum (55 %)
  • regional lymph nodes such as renal hilus, abdominal, paraaortic, paracaval (34 %)
  • liver (33 %)
  • skeletal system (32 %)
  • adrenal glands (19 %)
  • contralateral kidney (11 %)
  • CNS (6 %)

(Keller 2010)

  • in the area of the oral cavity, preferably the gingiva.

In approximately 23 %, oral cavity metastases represent the first sign of a malignant event. Metastases of an RCC in the area of the oral cavity occur in women in 8.5 % and in men in 11 %.

(Wittig 2012)

General therapyThis section has been translated automatically.

The treatment of renal cell carcinoma is primarily surgical and is also carried out depending on the stage (for tumour classification, see "Classification"). Neoadjuvant therapy is not clinically relevant.

In certain cases, the following can be used:

  • Immunotherapy (e.g. in the case of multiple metastases)
  • radiotherapy (e.g. for bone metastases)
  • ablative procedures such as cryo- or radiofrequency ablation for small RCC and high comorbidity or limited life expectancy) (Doehn 2020).

Internal therapyThis section has been translated automatically.

Clear cell RCC: Clear cell RCC is almost completely resistant to common cytotoxic or cytostatic agents.

In advanced stages or in the presence of metastases, human monoclonal antibodies (such as a combination of pembrolizumab plus axitinib) can be used for first-line therapy (Doehn 2020).

Multiple metastases: For multiple metastases, palliative therapy (with the exception of metastatic clear cell RCC [Doehn 2020]) is possible with:

- giogenesis inhibitors e.g. Bevacizumab combined with Interferon- alpha

- rosine kinase inhibitors, so-called VEGFR inhibitors, e.g. sorafenib, sunitinib

- TOR inhibitors such as temsirolimus, everolimus

- mune checkpoint inhibitors such as PD-1 inhibitor Nivolumab (Herold 2020)

Bone metastases: In this case, treatment can be carried out with bisphosphonates or local radiotherapy (Herold 2020).

Operative therapieThis section has been translated automatically.

Stage I (see "Classification"): Currently, organ-preserving partial kidney resection is considered the standard for patients in stage I or T1. Depending on the anatomical conditions, this can be performed open or laparoscopically (Kasper 2015). In laparoscopic procedures, blood loss is generally lower and the inpatient stay shorter (Doehn 2020).

Stage ≥ II (see "Classification"): From stage II and higher, radical nephrectomy is the standard procedure.

The operation is performed using the so-called no-touch technique, i.e. before manipulation of the kidney, the blood vessels supplying and draining the kidney are cut off. In radical nephrectomy, the kidney with perirenal fat capsule, Gerota's fascia, ipsilateral adrenal gland, ureter and the spermatic and ovarian vessels are resected en bloc, as well as the paracaval and paraaortic lymph vessels and any cone from the vena cava (for stages of vein invasion, see "Classification"). (Herold 2020)

Bilateral tumors: In bilateral tumors, the primary goal should be partial renal resection. If this is not possible, it is recommended to perform partial resection on the technically simpler side first. The residual function of the operated kidney should be evaluated p.o. after about one month.

If the function is sufficient, a tumor nephrectomy can be performed on the other side.

If function is insufficient, the options are imperative partial kidney resection or tumor nephrectomy followed by dialysis. (Manski 2020)

Lymphadenectomy: Systematic lymphadenectomy is not recommended with unremarkable preoperative imaging and unremarkable intraoperative findings (Doehn 2020).

Solid distant metastases: Solid distant metastases from e.g. liver or lung can also be surgically removed or minimally invasively destroyed (Herold 2020).

Multiple metastases: see above "Internal therapy".

Note: If there are contraindications to surgery, local ablative procedures such as radiofrequency or crypto-ablation can be used (see above "Therapy, general" (Herold 2020).

Progression/forecastThis section has been translated automatically.

Preoperatively and postoperatively, various formulas can be used to calculate the risk of recurrence.

For example, preoperative formulas include:

  • Cindolo formula
    • ≤ 1.2 = low risk with a 2- and 5-year recurrence-free rate of 96% and 93%, respectively.
    • > 1.2 = high risk with a 2- and 5-year recurrence-free rate of 83% and 68%, respectively.
  • Yaycioglu- Formula
    • ≤ 3 = low risk with a 2- and 5-year relapse-free rate of 98% and 92%, respectively.
    • > 3 = high risk with a 2- and 5-year recurrence-free rate of 67% and 57%, respectively (Doehn 2020).

Postoperative formulas include, for example:

  • UCLA Integrated Staging System (UISS- Model).
    • Stage I: 2- and 5-year recurrence-free rates of 96% and 94%, respectively (equivalent to TNM I).
    • Stage II: 2- and 5-year recurrence-free rates of 89 % and 67 % respectively (corresponds to TNM I, II, III)
    • Stage III: 2- and 5-year recurrence-free rate of 66 % and 39 % respectively (corresponds to TNM III and IV))
    • Stage IV: 2- and 5-year recurrence-free rate of 42 % and 23 % respectively (corresponds to TNM IV)
    • Stage V: 2- and 5-year relapse-free rate of 9 % and 0 %, respectively (corresponds to TNM IV) (Doehn 2020 / Kraus 2014).

A good prognosis has:

  • papillary renal cell carcinoma
  • multilocular cystic renal cell carcinoma (Golbeck 2013)
  • oncocytoma (Kraus 2014)

A poor prognosis:

  • clear cell RCC
  • Ductus Bellini carcinoma
  • Renal medullary RCC (in this case, distant metastases are already found at initial diagnosis in about 95% of cases [Golbeck 2013]). (Herold 2020)

Mortality: The prognosis of RCC is relatively favorable compared to other malignancies. In men, the relative 5-year survival rate is 75% and in women 77%. Depending on the tumor stage, the 5-year survival rate is:

  • Stage I: 97 %
  • Stage II: 87 %
  • Stage III: 60 % without lymph node involvement / 30 % with lymph node involvement (Herold 2020)
  • Stage IV: 30 % if solitary metastases removed, < 5 % in all other cases (Herold 2020) (Doehn 2020).

Metastatic RCC: Prognosis is markedly variable in metastatic RCC. Patients have a poor prognosis if the following factors are present:

  • No nephrectomy
  • KPS (Karnofsky Performance Status) < 80
  • low Hb value
  • high corrected calcium
  • abnormally high LDL levels

Patients had a median survival at:

  • no factor of 24 mon.
  • 1 - 2 factors by 12 mon.
  • ≥ 3 factors by 5 mon (Kasper 2015).

AftercareThis section has been translated automatically.

Depending on the stage of the disease, patients are divided into 3 different groups:

  • 1. Low risk pT1a / b, cN0, cM0, G1 - 2
  • 2. medium risk (Intermediate risk)
    • pT1a / b, cN0, cM0, G 3
    • pT2 c / pN0, cM0, G1 - 2
    • ablative therapy or R1-situation (residual tumor) of a low-risk carcinoma
  • 3. High risk
    • pT2 c / pN0, cM0, G3
    • pT3 - 4 and / or pN + (Doehn 2020)

Since even in early stages of RCC sonography, excretory urogram and angiography do not allow reliable staging, the following procedure is recommended:

1. patients with Low risk: In these patients the following examinations should be performed at intervals of 3, 6, 12, 18, 24, 36 and 48 months:

  • clinical examination
  • Determination of laboratory parameters such as blood count, creatinine, CRP, ESR (the increase in nonspecific inflammatory parameters may indicate metastasis).
  • Sonography of the abdomen in examinations where no CT or MRI is performed
  • CT or MRI of the abdomen pelvis and bone window (after 3, 12, 24 and 48 months)
  • CT or MRI of the thorax (after 12, 24 and 48 months) (Doehn 2020)

2. patients with intermediate risk: The examinations that are performed in patients with low risk are also performed. However, the time intervals are different: 3, 6, 12, 18, 24, 36, 48, 60, 84, 108 months.

CT of the thorax should be done at 6, 12, 24 months and then at each subsequent examination.

CT of the abdomen at (3), 12, 36, 60 months and then at each subsequent examination. (Doehn 2020)

Patients with high risk: The examinations that are carried out in patients with low risk are also carried out here. The time intervals are as for intermediate risk 3, 6, 12, 18, 24, 36, 48, 60, 84, 108 months. However, CT of the thorax should be performed for the first time at 6 months and then at each subsequent examination. CT of the abdomen is recommended at (3), (6), 12, 24, 60 months and subsequently at each subsequent examination. (Doehn 2020)

LiteratureThis section has been translated automatically.

  1. Ahrends M et al (2020) What is new in the diagnosis and therapy of renal cell carcinoma? Dtsch Med Wochenschr (145)11 734 - 739
  2. Delecluse S et al (2020) Classification and drug therapy of renal cell carcinoma. Onco- Nephrology 163 - 187
  3. Doehn C et al. (2020) Guidelines program oncology (German Cancer Society, German Cancer Aid, AWMF): Diagnostics, therapy and follow-up of renal cell carcinoma, long version 2.0, 2020, AWMF register number: 043/017OL, https://www.leitlinienprogramm-on- kologie.de/leitlinien/nierenzellkarzinom/
  4. Dützmann S (2018) Basics neurosurgery. Elsevier Publishers 46
  5. Ertl- Wagner B (2007) Pediatric neuroradiology. Springer Verlag 74
  6. Ganten D et al (2002) Renal cell carcinomas. Molecular medical basis of non-hereditary tumor diseases. Springer Verlag 257 - 289
  7. Golbeck S V (2013) Comparison of survival in metastatic renal cell carcinoma using two historical comparative cohorts- cytokine therapy versus targeted agents. Diploma thesis for the degree of doctor of all medicine (Dr. med. univ.) at the Medical University of Graz.
  8. Herold G et al (2020) Internal medicine. Herold Publishers 654 - 656
  9. Kasper D L et al (2015) Harrison's Principles of Internal Medicine. Mc Graw Hill Education 578 - 579
  10. Kasper D L et al (2015) Harrison's internal medicine. Georg Thieme Publishers 849 - 852
  11. Keller C K et al (2010) Practice of nephrology. Springer Verlag 95 - 104
  12. Kraus S (2014) The prognostic value of preoperative platelet count and thrombocytosis in patients with surgically treated renal cell carcinoma. Dissertation for the degree of Doctor of Medicine at the Medical Faculty of the Ludwig-Maximilians-University of Munich 20.
  13. Kuhlmann U et al. (2015) Nephrology: pathophysiology - clinic - renal replacement procedures. Thieme Verlag 64 - 65
  14. Manski D (2020) The urology textbook. de Dirk Manski Verlag 278 - 301.
  15. Pantelis A et al (2007) Tuberous cerebral sclerosis: laser dermabrasion and fibrin sealant of facial angiofibromas. ResearchGate ENT (13) 55
  16. Wittig J et al. (2012) Oral metastasis of renal cell carcinoma: a case report of initial manifestation of renal cell carcinoma as osseous metastasis in the mandible. Schweiz Monatsschr Zahnmed (122) 619 - 623
  17. Wolf G et al (2020) Elsevier Essentials Nephrology eBook: The essentials for physicians of all specialties. Urban and Fischer Publishers 61

Last updated on: 23.02.2021