Abstract
The sphenoid bone is an unpaired bone that contributes to the formation of the skull base. Despite the enormous progress in transnasal endoscopic visualisation, imaging techniques remain the cornerstones to characterise any pathological condition arising in this area. In the present review, we offer a bird’s-eye view of the developmental, inflammatory, and neoplastic alterations affecting the sphenoid body and clivus, with the aim to propose a practical diagnostic aid for radiologists based on clinico-epidemiological, computed tomography, and magnetic resonance imaging features.
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Introduction
The sphenoid (from the Greek “sphenoeides”, “wedgelike”) bone is a butterfly-shaped, median single structure that articulates with frontal, ethmoid, zygomatic, parietal, temporal, occipital, palatine, and vomer bones: it represents the key intersection of the anterior, middle, and posterior cranial fossa [1]. It is formed by the greater and lesser wings, the medial and lateral pterygoid processes, and by a variably pneumatized central body: the latter is located between the greater wings, and it houses the two sphenoidal sinuses along with a depression named “sella turcica” (from the Latin, “Turkish saddle”). The sphenoid bone is surrounded by many critical neurovascular structures such as the pituitary gland; the C3-C4-C5 segments of the internal carotid artery; the optic nerves and chiasm; cranial nerves III, IV, V1, V2, and VI; the sphenopalatine ganglion and artery; the cavernous sinus; and the ventral brainstem. It also contributes to the formation of fissures and foramina of the skull base such as the optic canal, superior and inferior orbital fissures, and foramen rotundum, lacerum, spinosum, and ovale; in addition, it contains important radiological and surgical landmarks such as the optic and maxillary struts and the Vidian canal (from the Florentine anatomist, Vidus Vidius) [2]. The clivus is the inclined midline surface of the skull base, just anterior to the foramen magnum, and which is formed by the sphenoid body and the basilar part of the occipital bone (basiocciput) [1].
The aim of this review is to summarise the clinico-epidemiological, computed tomography (CT), and magnetic resonance imaging (MRI) features of a wide variety of lesions involving the sphenoid body and the clivus. Such features may guide radiologists and skull base surgeons towards the most appropriate diagnostic and/or therapeutic approaches to the sphenoid/clival lesions.
Imaging techniques, classification, and clinico-epidemiological features of sphenoid/clival lesions
Radiological investigation techniques for the assessment of any lesion involving this area are nowadays represented by CT and MRI, which play a complementary role in the study of the whole skull base. The former is extremely useful in the identification of the sphenoid bone profile, erosions, sclerosis, lysis, intrasinusal content, and extra-sphenoid extension of disease. MRI is instead crucial to define both intracranial and extracranial soft tissue invasions, to evaluate the possible involvement of cranial nerves, and to further characterise intrasinusal contents [3]. Skull X-ray projections are currently considered an outdated examination with a significantly lower accuracy than CT and MRI; therefore, radiographs have no more indications in skull base radiology [4]. While FDG-PET/CT can be used as a support to CT and MRI, especially for staging purposes, its role in sphenoidal conditions falls beyond the scope of this paper.
From an epidemiological point of view, sphenoid lesions are quite uncommon, and they are classically classified into developmental, inflammatory, and neoplastic pathologies, each of them with extremely variable imaging patterns [5]. Traumatic sphenoid and/or clival lesions, which we have excluded from this classification, represent an emergency issue that is invariably associated with other craniofacial injuries and will not be further discussed. Benign and malignant tumoural pathologies primarily arising from the sphenoid body and clivus are rare with an estimated incidence rate of < 50 cases per 100,000 inhabitants [6]. This localization is also uncommon for inflammatory diseases, if we exclude secondary involvement of the sphenoid sinus in both acute and chronic rhinosinusitis: only 20% of all paranasal mycetomas, 1–2% of all paranasal mucoceles, and 2% of all cases of skull base osteomyelitis involve the sphenoid bone [7,8,9,10,11,12]. Regarding developmental alterations, it is not easy to define their prevalence since they often remain asymptomatic lifelong. Arrested pneumatisation of the sphenoid sinus is believed to be the most frequent developmental alteration; ecchordosis physaliphora is still one of the more frequent alterations since it can be found in 0.4–2% of autopsies [13]. Clinical manifestations of sphenoid/clival lesions are variable. Developmental lesions and haemangiomas are often incidental findings, whereas inflammatory lesions or tumours are almost always symptomatic. They may present with headache (40% of symptomatic cases), visual disturbances, and cranial neuropathies due to the critical neurovascular relationships with the aforementioned structures [14, 15]. Headache is typically described as deeply located and retro-orbital; visual disturbances can be grouped into three neurologically distinct syndromes: the sphenocavernous syndrome (deficits of cranial nerves III, IV, VI, V1, and V2, with or without the involvement of the optic nerve and the oculosympathetic fibres), an isolated abducens palsy (for only cranial nerve VI involvement, which runs in the narrow Dorello’s canal), and an isolated loss of visual function [14]. Ominous signs and symptoms such as facial numbness, facial pain, epistaxis, or anosmia are instead much rarer [14]. In Tables 1, 2 and 3 we have summarised the main clinical manifestations of each pathology.
The role of radiologists in the evaluation of sphenoid lesions
Radiologists play a central role in the diagnostic assessment of every sphenoid lesion since only a limited view of the anterior walls of its sinusal cavities can be performed in the office setting, even with modern transnasal endoscopy. Furthermore, its unfavourable anatomical location sometimes requires extensive surgical dissection in order to obtain a tissue sample by transnasal biopsy [4, 16, 17].
Multidisciplinary cooperation among radiologists, pathologists, neurosurgeons, and otolaryngologists is thus essential. Diagnostic imaging plays a central role in the process of differential diagnosis, especially between inflammatory and neoplastic lesions. The radiologist must provide diagnostic hypotheses for each condition by the identification of clues and features of malignancies [18]. Furthermore, some benign sphenoid bone alterations — such as neurenteric cyst, haemangioma, arrested pneumatization, or fibrous dysplasia — may be diagnosed only on the basis of their imaging features. For this reason, some authors have cleverly spoken of “do-not-touch” sphenoid lesions for these four entities [16]. Table 4 illustrates the most relevant CT and MRI features of sphenoid body and clival diseases.
Developmental lesions (Table 1)
Ecchordosis physaliphora
Ecchordosis physaliphora is a midline congenital gelatinous haemartoma not bigger than 2 cm, derived from notochordal remnants (Fig. 1). It is usually located in the intradural space of the prepontine cistern at the same level as the Dorello’s canal, and it is attached to the dorsal wall of the clivus by a small peduncle, the typical “stalk sign” [13]. CT features include a well-defined bony clival defect with cortical preservation and the bony (or cartilaginous) “stalk” projecting from the clivus. MRI shows an expansive lesion with low signal intensity (SI) on T1W images, high SI on T2W images, lack of contrast enhancement (CE), and facilitated diffusion on diffusion-weighted imaging (DWI) [19].
Differential diagnoses: Bony erosion — albeit this feature is reported to be extremely rare for notochordal remnants — joint with a restricted diffusion, should raise the suspicion of clival chordoma, which is considered to be the malignant counterpart of ecchordosis and its main mimicker [13]. Other differential diagnoses include dermoid cyst, a mass of the midline with no CE but high SI on T1W, and arachnoid cyst that can be distinguished because it presents the same SI as cerebrospinal fluid on all sequences [20].
Neurenteric cyst
Neurenteric cyst develops from the incomplete resorption of the canal of Kovalevsky (neurenteric canal), the embryological connection between the neural tube and foregut (Fig. 2). It is lined by mucin-secreting intestinal-type or respiratory epithelium [21]. CT density and MRI T1W SI are quite variable, but they are more often high because of the proteinaceous material within the cyst [21]. High SI on T2W images and facilitated diffusion on DWI are also generally observed [22]. Internal septa, enhanced walls, and bony alterations are not common.
Differential diagnoses: dermoid and the rare proteinaceous epidermoid cyst (“white epidermoids”), which show high SI on T1W as neurenteric cyst but moderate to striking diffusion restriction; arachnoid cyst, which follows cerebrospinal fluid SI on all sequences; nerve sheath tumours can be easily distinguished because they show a strong CE, and they are very unlikely to be located in the midline because of their association with cranial nerves [23].
Arrested pneumatisation of the sphenoid sinus
Arrested pneumatisation of the sphenoid sinus is basically a variant of skull base development (Fig. 3) which can be found in up to 7.4% of the population [24]. Although often it represents an incidental finding, it can sometimes be associated with nonspecific symptoms, mostly headache [25]. Physiologically, the sphenoid sinus is absent at birth, and its body is completely formed by the red bone marrow. From the second to the fourth month of life, a process of yellow bone marrow conversion and subsequent respiratory epithelium colonisation begins, and it ends only with adulthood [26, 27]. Incomplete pneumatisation occurs whenever, for unknown reasons, such a process is interrupted, and yellow marrow foci persist in adults. This phenomenon may actually involve other paranasal sinuses, such as the ethmoid [28]. Its non-expansive nature, the presence of osteosclerotic margins, linear calcifications in the matrix, and the absence of cortical breaches and of intralesional foci of fat on MRI representing yellow bone marrow are all very specific signs [29].
Differential diagnoses: fibrous dysplasia, which shows a “ground-glass” bone marrow appearance on CT and an expansile nature with possible involvement of neural foramina [29]; ossifying fibroma, which can be distinguished thanks to its a more expansile nature and because its matrix more closely resembles to the ground-glass pattern of fibrous dysplasia [29]; chordoma and chondrosarcoma tend to be expansile and destructive in nature, without central fat [29]; osteomyelitis and metastases usually show a variable pattern of bony destruction and a low T1 SI of bone marrow [29]; intraosseous lipoma shows instead a fatty matrix with microcalcifications and a variable degree of trabecular bone loss with associated cortical breach [30]; intraosseous haemangioma has a typical “sunburst appearance” and CE on CT, an expansile nature, and it does not necessarily contain fat, while it may reveal cortical breach [30].
Epidermoid cyst
Epidermoid cyst is a rare, slow-growing, benign lesion of ectodermal origin lined by squamous epithelium, and containing laminated keratin (Fig. 4). It differs from dermoid cysts for the lack of cutaneous adnexa or mesodermal elements such as hairs [31]. The cerebellopontine angle and suprasellar area are the most often involved sites. Paranasal sinus localization is exceedingly rare with only a few case reports [32]. Since sphenoidal epidermoid cysts are frequently located into the diploe, they are thought to originate mainly from congenital entrapments of ectodermal elements within the presphenoid fusion plates [32]. At CT, epidermoid cysts appear hypodense with a lack of CE or, sometimes, with a thin peripheral rim of enhancement. A scalloped or lobulated sclerotic rim is typical [33]. Epidermoid cysts appear similar to cerebrospinal fluid on MRI T1W (low SI) and T2W (high SI) images. High SI on T1W images and high density on CT may be rarely observed due to protein deposits (“white epidermoids”) [32]. Heterogeneous suppression of SI on fluid-attenuated inversion recovery (FLAIR) sequence, high SI on DWI, and low apparent diffusion coefficient (ADC) values — due to the intralesional squamous epithelium and keratinaceous debris that hinder the free water diffusion — are typical [34].
Differential diagnoses: arachnoid cysts, which follow cerebrospinal fluid SI without restricted diffusion [31]; abscess, which differentiates from epidermoid cyst for a ring CE with thicker walls and a surrounding oedema [35]; dermoid cysts, neurenteric cysts, or mucoceles are instead difficult to differentiate from a “white epidermoid” even though their clinical management does not differ in practice [32].
Fibrous dysplasia
Fibrous dysplasia is a congenital disease that is characterised by an altered osteoblastic differentiation resulting in the replacement of normal bone with poorly organised and structurally unhealthy fibrous tissues (Fig. 5) [36]. Monostotic (single bone) or polyostotic (multiple bones) forms are recognised. Fibrous dysplasia may be isolated or part of systemic conditions, especially “McCune-Albright syndrome” (fibrous dysplasia, café-au-lait skin spots, and precocious puberty) and “Mazabraud syndrome” (fibrous dysplasia plus intramuscular myxomas) [36]. Malignant transformation — most commonly into an osteosarcoma — occurs in up to 2.5% of cases [37]. CT is considered the diagnostic gold standard, and bony alterations can show three different patterns: ground-glass (56%), homogeneously dense (23%), and cystic (21%). The attenuation coefficient values typically vary from 70 to 130 Hounsfield unit [37]. Instead, MRI is less accurate, and it shows variable T1-T2 SI, depending on the content of the alterations: active lesions with metabolically active fibrous tissue show intermediate T1 SI and high T2 SI, whereas inactive lesions with highly mineralized matrix have low T1 and T2 SI [38]. Active lesions also show high SI on CE-T1W images, while DWI does not exhibit water diffusivity restriction [39].
Differential diagnoses: MRI can be very misleading, and especially when fibrous dysplasia alterations show T1 intermediate SI, T2 high SI, and vivid CE, it could resemble a skull base malignancy. In this circumstance, it is very useful to perform a CT that will solve any doubt by revealing the typical fibrous dysplasia bony changes [38]; Paget disease is a chronic, idiopathic progressive condition characterised by initial bone destruction followed by reparative processes. The sphenoidal involvement has been anecdotally reported in this condition, but the fact that other sinuses are usually spared, the rare and scarce cyst-like changes and the occurrence after the fifth decade are all useful features for differentiation from fibrous dysplasia [40]. Intraosseous meningioma — compared with fibrous dysplasia — shows feathering of lesions edges, soft tissue involvement and vivid homogenous CE [41]. Ossifying fibroma is a benign tumour with similar features, but it typically shows better-defined boundaries with osteosclerotic shells, whereas the periphery of fibrous dysplasia usually blends with the surrounding bone [42]. Malignant transformation of fibrous dysplasia into osteosarcoma should be suspected by the presence of periosteal response on CT and by areas of restricted diffusion on MRI, although these are not specific signs [39, 43].
Inflammatory lesions (Table 1)
Fungus ball (mycetoma)
Fungus ball is the most common form of non-invasive fungal rhinosinusitis in immunocompetent non-atopic patients (Fig. 6). It is probably related to a deficient mucociliary clearance that fosters the intraluminal extramucosal fungal proliferation, and Aspergillus fumigatus is the most commonly causative organism [44]. Fungus ball appears as a hyperdense mass — due to the conglomerated fungal hyphae — with linear or punctuate central calcifications on CT. Mucosa is thickened and vividly enhanced after contrast agent administration, whereas the intraluminal content shows no CE. The sinus may be expanded with sclerotic bony walls and bowing deformity [44]. Fungus ball shows a typical very low or “dark” SI on T2W images because of both calcifications and densely packed hyphae containing paramagnetic materials (iron and manganese) that induce areas of signal void. SI of fungus balls on T1W images is usually high [45], but intermediate or low intensities may be found [46]. On the other hand, the thickened sinus mucosa shows homogeneously hyperintense SI on T2W and CE-T1W images [44]. Paramagnetic metals, calcifications, and the absence of free water are the bases for the hypointensity of fungus balls on both DWI b1000 and ADC map [45, 46].
Differential diagnoses: mucocele, which can show variable T1 SI depending on protein contents (from low to high), typically appears hyperintense on T2W images, and it does not contain calcifications and metallic-density materials; sinonasal mucosal melanoma, which shows high T1 SI due to haemoglobin and melanin derivatives, but also CE of the internal component [47].
Mucocele
Mucocele presents as a complete opacification of one or more paranasal sinuses: most frequently, the maxillary and ethmoid sinuses are filled with mucus and their walls are lined by normal-appearing respiratory epithelium (Fig. 7) [9]. It is often associated with bony wall expansion and focal osseous resorption. The pathogenesis of mucocele remains unclear, but an altered mucociliary clearance, cystic dilatation of the mucosal glands, and cystic development from embryonic remnants are all contributing factors, often in the context of chronic rhinosinusitis. Radiation therapy can also lead to an isolated sphenoid mucocele as a consequence of fibrous tissue formation obstructing the natural ostium [9]. Mucocele appears as a completely mucous-filled and expanded sinus with a typical rim enhancement — sign of encapsulation — and lack of intralesional CE. CT density and MRI SI are variable, depending on the amount of water, mucus, and proteins. Most frequently, this lesion exhibits high water content with low density on CT, low SI on T1W, and high on T2W images; the high protein content results in high CT density, high SI on T1W, and low SI on T2W images [9]. DWI and ADC are highly variable. When viscous protein-rich secretions are present, it may have very low ADC values (< 0.5 × 10−3 mm2/s) [48].
Differential diagnoses: fungus ball, which shows very low or "dark" SI on T2W [45]; sphenoid mucus retention cyst, a more common condition that shows similar SI and density but without completely filling the sinus, it does not determine bony changes nor it shows recognisable walls [49]; sphenoid sinus inverted papilloma, a rare entity that shows — contrary to the mucocele — homogeneous CE, also of the internal component [50].
Osteomyelitis
Skull base osteomyelitis including the sphenoid bone (Fig. 8) may arise without associated external malignant otitis or chronic suppurative otitis media, as opposed to the temporal bone involvement [10]. The identification of clival anomalies on imaging techniques is crucial to making a timely diagnosis [51]. Patients with sphenoid osteomyelitis often have predisposing conditions such as diabetes mellitus, longstanding corticosteroid use, HIV infection, and chronic rhinosinusitis [10]. Unlike temporal bone infections, many organisms other than Pseudomonas aeruginosa may be involved from transnasal swabs [52]. CT shows diffuse bone erosion and demineralization; after the administration of contrast medium diffuses soft tissue swelling, obliteration of fat planes, involvement of the skull base foramina, and vascular complications (thrombosis, compression, pseudoaneurysm) can be highlighted [53]. Focal or diffuse clival hypointensity on T1W images due to the replacement of the normal fatty marrow is the most consistent MRI finding. XII cranial nerve palsy may manifest in case of infiltration of the hypoglossal canal [54]. In the worst cases, abnormal soft tissues in the cavernous sinus, narrowing/occlusion of the internal carotid artery, meningeal enhancement, intracranial extension, and involvement of lateral structures (parotid gland, temporomandibular joint) can also be observed [53]. This inflammatory tissue usually shows hyperintensity on DWI trace and low values on ADC map; however, several authors have observed that ADC values in osteomyelitis are higher than malignant neoplasms [53].
Differential diagnoses: imaging of skull base osteomyelitis is nonspecific, thus making difficult the differential diagnosis with malignancy [53]. Differential diagnosis includes nearly all sphenoid/clival malignancies, especially nasopharyngeal carcinoma. The imaging findings are very similar, with CE-CT and CE-MRI showing an enhancing mass associated with bone erosion and infiltration and restricted diffusion; therefore, biopsy is often essential for a proper diagnosis [53]. Goh et al. [55], however, have suggested some MRI features that are useful for differentiation: in detail, involvement of lateral structures, soft-tissue enhancement, oedema, and abscess formation are more typical of osteomyelitis. Metastases can have a similar appearance, but the medical history pinpoints to the correct diagnosis [53]. Non-tumoural conditions such as fibrous dysplasia and Paget disease can be easily differentiated for the absence of soft tissue involvement [53].
Benign tumours (Table 2)
Haemangioma
Primary intraosseous haemangioma (Fig. 9) is a slow-growing haemartoma of blood vessels. CT shows an expansive, well-circumscribed area of osteolysis in the sphenoid bone with the typical “sunburst appearance” in which thickened trabeculae adjacent to abnormal vascular channels converge on a central area, with preservation of the periosteum [56]. On MRI, haemangioma usually appears “mottled” and heterogeneous with high SI both on T1W and T2W images due to the fat deposition and presence of slow-moving and pooled venous blood, respectively. However, haemangioma may show an atypical low SI on T1W and/or T2W images. Enhancement in CE-T1W images is usually observed because of its vascular channels [56]. DWI does not show restriction, with high SI on DWI trace and high ADC values, similar to the other skull haemangiomas [57].
Differential diagnoses: arrested pneumatisation of the sphenoid sinus, a fat-containing lesion that does not show the “sunburst appearance” (see above). In general, intraosseous haemangioma can be easily differentiated on CT from other benign osteolytic conditions — such as fibrous dysplasia or lipoma — due to the presence of the typical “sunburst appearance.” Absence of cortical aggressiveness differentiates sphenoid haemangioma from malignant osteolytic conditions such as multiple myeloma or histiocytosis. [58].
Ossifying fibroma
Ossifying fibroma is a benign fibro-osseous tumour characterised by the replacement of normal bone with dense fibrous tissue with foci of mineralisation (Fig. 10) [59]. It typically affects the mandibular bone, whereas sphenoid involvement is rare [59]. Ossifying fibroma is characterised by rapid growth, high recurrence rate (30–56%), a tendency to invade surrounding tissues — including the orbits — and bony erosions [60]. Imaging appearance varies according to the fibrous/bone tissue ratio within the lesion: in the early stages, a thick peripheral bony rim is observed which surrounds a fibrous soft tissue centre, whereas in the later stages, a progressive filling of this centre with mature bone can be detected [61]. CT depicts an expansive mass with heterogeneous CE, a sclerotic shell, and variable amounts of intralesional calcifications. Concomitant aneurysmal bone cysts with fluid–fluid levels are frequently identified [59]. MRI is important to assess the tumour extension, and it generally shows a lesion with two components: a central fibrous area with low T1 SI and mixed low–high T2 SI and a peripheral ossified rim with both T1 and T2 low SI. SI on T2W images is mixed high-low in case of cysts or more pronounced fibrous tissue. Ossifying fibroma reveals a heterogeneous moderate-high enhancement on CE-T1W images [62]. This lesion can also appear as a largely calcified mass completely hypointense on T2W [61].
Differential diagnoses: fibrous dysplasia, which shows ill-defined boundaries (see the above paragraph); arrested pneumatisation of the sphenoid sinus, which does not show an expansile nature (see before); osteoma, which — contrary to ossifying fibroma — does not show soft tissue CE, does not have the sclerotic shell, and usually does not exhibit adherence to soft tissues (dura mater) [63]; malignant tumours such as osteosarcoma or chondrosarcoma, which manifest ill-defined margins, contrary to the well and sharply defined shell of the ossifying fibroma [63]. When the ossifying fibroma is completely calcified, it can show both T1 and T2 low SI, an appearance similar to neoplasms with a high nuclear-cytoplasmic ratio, such as lymphoma and sinonasal melanoma. The differential diagnosis is facilitated by observing a vivid CE of these malignant entities and, on CT, the absence of intralesional calcium [61].
Pituitary adenoma
Pituitary adenoma originates from the adenohypophysis and is classically divided by dimensions into micro- (< 10 mm) and macroadenoma (> 10 mm). The latter (Fig. 11) may cross the sellar floor and invade the skull base, especially into sphenoid and cavernous sinuses, clivus, orbits, dura mater, and subarachnoid, extradural, and nasopharyngeal spaces [64]. With their growth, they can show the typical “snowman sign” or “figure of 8”, given by the bilateral indentation of the macroadenoma by the diaphragma sellae [65]. Rarely, pituitary adenomas are entirely contained in the sphenoid body with the sellar floor intact since they originate from Rathke’s pouch ectopic remnants, trapped in the sphenoid ossification centres. Invasive macroadenoma appears as iso- or hypoattenuating compared to the brain tissue on CT, often with an inhomogeneous appearance due to cystic and/or haemorrhagic internal areas. These tumours are also associated with destructive bony involvement, well detectable on CT [66]. On MRI, macroadenoma presents medium–low SI on T1W images, medium-slightly high SI on T2W images, variable SI on DWI trace, and highly variable ADC values. CE is usually homogeneous [67].
Differential diagnoses: chordoma shows a higher T2 and DWI b1000 SI and higher ADC values than invasive macroadenoma, due to difference in histopathologic features (chordoma has an abundant myxoid stroma containing physaliferous cells with large cytoplasm, invasive macroadenoma shows highly crammed cells with large nuclei) [67]. Pituitary fossa meningioma could resemble a pituitary macroadenoma; nevertheless, two main aspects allow to distinguish these different conditions since meningioma reveals a more avid and homogeneous CE than adenoma [66], and in case of meningioma, the normal pituitary gland can still be recognised [65]. Moreover, meningioma does not show the “snowman sign” [65]. On the other hand, invasive macroadenoma may displace the cavernous segment of the internal carotid artery laterally, a non-detected pattern in meningiomas [68].
Sinonasal (Schneiderian) papilloma
Sinonasal papilloma is a benign tumour arising from the ectodermally derived Schneiderian membrane lining the nasal cavity and paranasal sinuses. Papillomas of the sphenoid sinuses are almost all of the inverted type (Fig. 12) [69, 70]. They show a typical endophytic growth pattern, invasive nature (70% of them cause bony erosion), high recurrence rates (20–50%), and a potential malignant transformation into squamous cell carcinoma (10%) [69, 71]. There is mounting evidence that some types of human papillomavirus represent a risk factor for malignant transformation [72]. Sinonasal papilloma presents as a soft tissue density mass which is often associated with bony resorption and remodelling (thinning and bowing) on CT. Focal hyperostosis (cone-shaped or plaque-like) into the sinus wall may indicate the site of tumour origin, and this must be surgically drilled so as to avoid recurrences. Calcifications within papilloma are rare. At MRI, this tumour appears isointense to muscle on T1W images [73], and it may show a typical “cerebriform” pattern on T2W and CE-T1W images, thanks to the alternating lines of high and low SI. The diffusion pattern is non-specific and does not reliably allow radiologists to separate the inverted papilloma from malignant lesions [73]; sometimes, intralesional carcinoma foci usually can be observed as areas of lower ADC values [74]. Differential diagnoses: sphenoid sinus mucocele, which does not show CE of the internal component (see “Mucocele” paragraph); spheno-choanal polyp, a unilateral inflammatory soft tissue mass arising from sphenoid sinus and extending through its drainage ostium and spheno-ethmoidal recess towards the choana and nasopharynx. The extension to the choana and the expansion of the sphenoid sinus ostium without bony erosions favour this latter diagnosis [75]; distinguishing an inverted papilloma from a sphenoid sinus malignancy on imaging is instead very complex. Despite high values on ADC map and typical “cerebriform” pattern are identified, an endoscopic biopsy is nonetheless necessary.
Malignant tumours (Table 3)
Chordoma
According to the 2021 WHO classification of central nervous system tumours, chordoma is classified as the only subtype of “notochordal tumours”, which belong to “chondro-osseous tumours” among other mesenchymal, non-meningothelial tumours [76]. It derives from undifferentiated, extradural remnants of the notochord, and four histological subtypes are recognised: conventional (most common, tumour cells embedded in hyaline cartilage-like stroma), chondroid (islands of cartilage formation), poorly differentiated, and dedifferentiated or sarcomatoid chordoma (chordoma associated with a high-grade sarcoma) [77] (Fig. 13). Intracranial chordoma accounts for around one-third of all chordomas [78]. It mostly arises from the clivus, whereas petrous apex, sella turcica, and sphenoid sinuses are often secondarily involved. Invasion of the prepontine cistern, foramen magnum, nasopharynx, chiasm, third ventricle, and jugular fossa are also common [79]. Clivus chordoma causes massive bony erosion, and it looks like a well-defined centrally located heterogeneous soft tissue density mass with hypodense foci of gelatinous degeneration on CT. Intralesional hyperdense foci are often found as calcified material — chondroid subtype — or sequestered/destroyed bone fragments [79]. Chordoma usually shows low-to-medium SI on MRI T1W images, and conventional chordoma shows typical features on T2W images, with high SI associated to hypointense intralesional septa which give a multilobulated appearance to the mass. Foci of calcification, blood, and mucus can be observed as well. Furthermore, dedifferentiated chordoma may show low SI on T2W images [78]. CE is very variable, and “honeycomb” appearance is frequently observed due to the presence of hypointense areas of necrosis and cartilage [79]. Regarding DWI, chordomas show a restricted diffusion, with the lowest ADC values found in dedifferentiated subtype (often < 1.0 × 10−3 mm2/s) [80]. However, DWI may primarily represent an important tool for differential diagnosis with chondrosarcoma (see below).
Differential diagnoses: ecchordosis physaliphora, which shows cortical preservation and higher ADC values (see “Ecchordosis physaliphora” paragraph); arrested pneumatisation of the sphenoid sinus, not expansile and with central fat; pituitary adenoma, which shows a lower T2 SI (see “Pituitary adenoma” paragraph); chondrosarcoma, a rare tumour which probably originates from malignant transformation of the cartilaginous cells of the synchondroses and that is composed of atypical chondrocytes with enlarged hyperchromatic nuclei set in an abundant cartilaginous matrix [81]. Features useful for differential diagnosis: chordoma is typically located more centrally, whereas chondrosarcoma arise laterally in the petro-clival synchondrosis; on CT, chondrosarcoma may show a typical “ring-and-arc” pattern of calcifications, due to endochondral mineralization of hyaline cartilage nodules; DWI reflects the differences in extracellular matrices of these entities: the cartilaginous stroma associated with variable grade of cellularity, typical of chondrosarcoma, is responsible of very high values in the ADC maps (often > 2.0 × 10−3 mm2/s), whereas chordomas usually show medium–low values [78].
Nasopharyngeal carcinoma
Nasopharyngeal carcinoma normally originates from the Rosenmüller fossa (Fig. 14) and is histologically divided into three subtypes: keratinizing squamous cell carcinoma, nonkeratinizing squamous cell carcinoma, and undifferentiated or poorly differentiated carcinoma [82]. The keratinizing-type is related to tobacco, alcohol, and dietary nitrosamines exposure, whereas the other two subtypes are usually linked to Epstein-Barr virus infection. Nasopharyngeal carcinoma is more frequent in the Asian population (70%) [82]. Involvement of sphenoid sinus upstages the tumour to cT3; retropharyngeal/laterocervical metastatic lymph nodes are almost invariably detectable [83]. On CT, these tumours appear as a soft-tissue density mass with heterogeneous CE [83]. CT has high sensitivity in the detection of the sphenoid cortical bony erosion, whereas MRI is crucial to detect bone marrow invasion, well depicted on T1W images as a focal area of low SI [83, 84]. Nasopharyngeal carcinoma usually shows a slightly higher SI than muscle on T2W images, low SI on T1W images, a lower degree of CE compared to normal mucosa [84], and restricted diffusion [85, 86]. In the case of sphenoid invasion, it is fundamental to distinguish the frequent inflammatory reaction next to the neoplastic mass, by defining a precise inflammation-tumour border. Inflammatory changes usually show high SI intensity on T2W images, a thin superficial CE, and a facilitated diffusion on DWI, whereas neoplastic tissue shows lower SI on T2W images, a solid CE, a restricted diffusion [87]. Perineural invasion mainly through the trigeminal nerve may be observed.
Differential diagnosis is with other large masses involving the sphenoid and nasopharyngeal areas. Lymphoma often originates in the midline; frequently involves parotid and submandibular nodes, rarely the retropharyngeal nodes; and has lower ADC values than nasopharyngeal carcinoma because of its higher cellularity (usually ≤ 0.60 × 10−3 mm2/s) [84, 86]. Adenoid-cystic carcinoma arising from ectopic salivary tissue in the sphenoid sinus mucosa or from minor salivary glands of the nasopharyngeal submucosa may invade neighbouring structures including the clivus. It has a greater tendency compared to nasopharyngeal carcinoma to show perineural invasion through cranial nerves V and VII [5]. Metastases are suspected in case of a primary neoplasm elsewhere, and osteomyelitis is another possible lesion to be considered.
Neuroendocrine tumour
Neuroendocrine tumour originates from neuroendocrine amine precursor uptake and decarboxylation cells (Fig. 15) [88]. It is categorised by cellular differentiation into well-differentiated (carcinoid), moderately differentiated (atypical carcinoid), and poorly differentiated (small cell neuroendocrine carcinoma) tumours [89]. The lower the degree of differentiation, the worse the patient’s prognosis. Paranasal sinus is an atypical location for a primitive neuroendocrine tumour, accounting for only 5% of cases. Small cell neuroendocrine carcinoma is the most frequent histotype found in the sphenoid sinus and the only one with sufficient CT-MRI data: it shows a homogeneous isodense or mild hyperdense appearance on CT given by the neuroendocrine “grana” characterised by closely packed cells. Calcifications and haemorrhage are very rare [90]. CT clearly shows the inevitably present bony destruction. Tumour growth usually shows a typical “pigeon” pattern with symmetrical involvement of the sphenoid, cavernous sinus, clivus, and internal carotid arteries (Fig. 16), and this is better detectable on T2W fat-suppressed images and T1W-CE images [90]. MRI shows low-intermediate SI on T1W and T2W images, with moderate and homogeneous CE [90]. DWI exhibits high SI in the trace with low ADC values [88].
Differential diagnoses: sphenoid sinus inverted papilloma, which shows a typically “cerebriform” pattern on MRI and may contain hyperdense foci on CT; sphenoid sinus squamous cell carcinoma, adenocarcinoma, and adenoid-cystic carcinoma are very difficult to distinguish only based on imaging because they often show bone erosions and intermediate SI on T2W, but also a more heterogeneous CE pattern with respect to neuroendocrine carcinoma; lymphoma exhibits similar SI on T1W and T2W and a similar homogenous CE (although not symmetrical or pigeon-like), but usually with lower ADC values than neuroendocrine tumour; olfactory neuroblastoma (esthesioneuroblastoma) can invade sphenoid bone, but it arises from the nasal cavity and shows peripheral areas of cystic degeneration and calcific foci [90].
Lymphoma
Primitive lymphoma of the sphenoid sinus (Fig. 17) is exceedingly rare, with only 20 cases described in the literature [15]. Non-Hodgkin diffuse large B-cell lymphoma is the most common histotype. Perineural spread, bony destruction, and dura mater, cavernous sinus, and intracranial involvement is often observed [91]. Unenhanced CT shows as a soft tissue mass without calcifications, chondroid, or osteoid matrix. It usually has higher density than other neoplasms due to the high nuclear-cytoplasmic ratio. Intralesional haemorrhage and necrosis are rare. Permeative lytic destruction and bony remodelling of sinus walls are recurrent [92]. Isointense SI on T1W, mildly hyperintense SI on T2W, and moderate enhancement on CE-T1W images are generally described on MRI [86, 93]. Lymphoma shows a restriction of diffusivity with very low ADC values (typical values suggestive of lymphoma: ≤ 0.60 × 10–3 mm2/s) [85, 86, 94].
Differential diagnoses: all the sphenoid neoplasms characterised by bony erosions and intermediate SI both on T1W and T2W images: nasopharyngeal carcinoma, neuroendocrine carcinoma, adenoid-cystic carcinoma, adenocarcinoma, and metastases. Very low ADC values [95], homogenous CE, multiple lymph nodes echelons involved are typical — yet unspecific — features of lymphoma. Sinonasal melanoma usually shows a typical high SI on T1W for melanin and/or haemorrhagic foci [96, 97]. A completely calcified ossifying fibroma can show both T1 and T2 low SI, but it is easier to diagnose thanks to the absence of any CE. Moreover, the evidence of calcium on CT excludes the diagnosis of lymphoma [61].
Multiple myeloma/plasmacytoma
Multiple myeloma and plasmacytoma are both characterised by malignant proliferations of a single plasma cell clone (Fig. 18) [98]. Multiple myeloma bone involvement has four different patterns: disseminated form with multiple round lytic lesions (the most frequent subtype in the skull), a disseminated form with diffuse osteopenia, solitary plasmacytoma, and osteosclerosing fibroma [99]. In the former case, bone CT shows multiple lytic foci without a sclerotic rim, and that tend to coalesce (“punched-out” lesions); extramedullary extensions can be observed as expansive adjacent masses with soft tissue density. Plasmacytoma usually is represented by a single lytic bone lesion associated with a soft tissue density mass, but it is very rare at skull base level [98]. Multiple myeloma rarely manifests as multiple hyperdense osteosclerotic lesions (osteosclerosing form) [98]. Five different patterns are recognised on MRI: normal marrow (no visible infiltration); focal pattern; diffuse disease; salt-and-pepper appearance; and combined focal-diffuse infiltration. Multiple myeloma lesions show low SI on T1W images, mildly high SI on T2W images, and homogeneous CE. Myeloma infiltration presents high SI on DWI and higher ADC values than normal bone marrow in which very low free water diffusion is normally found [99].
Differential diagnoses: osteolytic malignant lesions (prevalent pattern in multiple myeloma) as osteosarcoma, chondrosarcoma, malignant fibrous histiocytoma, bone Langerhans cell histiocytosis, and lymphoma [100]. Differential diagnosis on imaging is difficult; “salt and pepper” pattern on MRI associated with “punched-out” osteolysis on CT are the most specific features.
Metastases
Sphenoid bone metastases (Fig. 19) are very rare. Prostate adenocarcinoma, thyroid carcinoma, hepatocarcinoma, and breast cancer are the most common histological subtypes of tumour [101]. Sphenoid metastatic localization is almost often a late manifestation in multi-metastatic patients. Cancer cells reach the sphenoid and clivus mainly by venous route, reaching the basilar plexus in two different ways: through the Batson’s plexus, where the blood from the thoraco-abdominal district passes during the Valsalva manoeuvre, bypassing the caval venous system, or through the inferior petrosal sinus, which drains from the facial and ocular districts [102]. CT and MRI features are not specific and they may mimic a primary tumour.
Differential diagnoses: all the possible clival malignant neoplasms, especially chordoma, chondrosarcoma and plasmacytoma [102]. As already stated, CT/MRI features are not specific for metastasis; thus, a properly collected past history and the presence of multiple similar alterations in the cranio-facial area or elsewhere are necessary for the diagnosis [101].
Conclusions
The sphenoid bone and the clivus can be primarily or secondarily affected by a large spectrum of pathologic conditions. CT and MRI are nowadays the reference imaging techniques to characterise sphenoid and clival abnormalities. Both techniques are almost always necessary to study these bones since they are scarcely susceptible to clinical assessment. Furthermore, any invasive diagnostic or therapeutic procedure has to be carefully evaluated because of its delicate anatomical relationships. For these reasons, radiologists have the crucial task to:
-
1) Identify the sphenoid/clival lesions that can be characterised with certainty by imaging techniques such as the “do-not-touch lesions”.
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2) Provide a list of differential diagnosis between inflammatory and neoplastic lesions in order to identify or rule out malignancies.
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3) Cooperate with skull base surgeons and pathologists to reach the correct diagnosis of those lesions that may be characterised by imaging techniques alone.
We are confident that, with a sound knowledge of imaging features, a correct non-invasive identification of lesions arising in this complex area will be possible in most cases.
Data availability
All data provide in the submitted work come from University Hospital of Careggi in Florence. All data are made available to the editors and reviewers.
Code availability
No specific software was used to carry out the submitted work.
Abbreviations
- MRI :
-
Magnetic resonance imaging
- CT :
-
Computed tomography
- SI :
-
Signal intensity
- CE :
-
Contrast enhancement
- DWI :
-
Diffusion weighted imaging
- ADC :
-
Apparent diffusion coefficient
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Nardi, C., Maraghelli, D., Pietragalla, M. et al. A practical overview of CT and MRI features of developmental, inflammatory, and neoplastic lesions of the sphenoid body and clivus. Neuroradiology 64, 1483–1509 (2022). https://doi.org/10.1007/s00234-022-02986-x
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DOI: https://doi.org/10.1007/s00234-022-02986-x