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Giant-cell carcinoma of the lung

December 15, 2023

Giant-cell carcinoma of the lung (GCCL) is a rare histological form of large-cell lung carcinoma, a subtype of undifferentiated lung cancer, traditionally classified within the non-small-cell lung carcinomas (NSCLC).

Giant cell carcinoma of the lung
Pulmonary giant cell carcinoma represents a rare variety of non-small cell lung carcinoma that is characterized by the presence of numerous tumor giant cells and an influx of inflammatory cells that are mostly polymorphonuclear leukocytes admixed with macrophages. The dense oval aggregates of polymorphonuclear leukocytes seen in this image are probably located in the cytoplasm of tumor giant cells (emperiopolesis) that have been sectioned in a plane that does not include their nuclei.
SpecialtyOncology 

The characteristic feature of this highly lethal malignancy is the distinctive light microscopic appearance of its extremely large cells, which are bizarre and highly pleomorphic, and which often contain more than one huge, misshapen, pleomorphic nucleus ("syncytia"), which result from cell fusion.

Although it is common in the lung cancer literature to refer to histologically mixed tumors containing significant numbers of malignant giant cells as "giant-cell carcinomas", technically a diagnosis of "giant-cell carcinoma" should be limited strictly to neoplasms containing only malignant giant cells (i.e. "pure" giant-cell carcinoma).[1]

Aside from the great heterogeneity seen in lung cancers (especially those occurring among tobacco smokers), the considerable variability in diagnostic and sampling techniques used in medical practice, the high relative proportion of individuals with suspected GCCL who do not undergo complete surgical resection, and the near-universal lack of complete sectioning and pathological examination of resected tumor specimens prevent high levels of quantitative accuracy.

Classification edit

For several decades, primary lung cancers were consistently dichotomously classified for treatment and research purposes into small-cell lung carcinomas (SCLCs) and non-small-cell lung carcinomas (NSCLCs), based on an oversimplified approach that is now clearly outmoded. The new paradigm recognizes that lung cancers are a large and extremely heterogeneous family of malignant neoplasms,[2] with over 50 different histological variants included in the 4th (2004) revision of the World Health Organization typing system, the most widely used lung cancer classification scheme ("WHO-2004").[1] These variants are increasingly appreciated as having different genetic, biological, and clinical properties, including prognoses and responses to treatment regimens, and therefore, that correct and consistent histological classification of lung cancers are necessary to validate and implement optimum management strategies.[3][4]

About 1% of lung cancers are sarcomas, germ cell tumors, and hematopoietic tumors, while 99% of lung cancers are carcinoma. Carcinomas are tumors composed of transformed, abnormal cells with epithelial tissue architecture and/or molecular characteristics, and which derive from embryonic endoderm.[5] Eight major taxa of lung carcinomas are recognized within the WHO-2004 classification:[1]

  1. Small-cell carcinoma
  2. Squamous cell carcinoma
  3. Adenocarcinoma
  4. Large-cell carcinoma
  5. Adenosquamous carcinoma
  6. Sarcomatoid carcinoma
  7. Carcinoid
  8. Salivary gland-like carcinoma

The subclassification of GCCL among these major taxa has undergone significant changes in recent decades. Under the 2nd revision (1981) of the WHO classification, it was considered a subtype of large-cell carcinoma.[6] In the 3rd (1999) revision,[7] it was placed within a taxon called "Carcinomas with Pleomorphic, Sarcomatoid, or Sarcomatous Elements", along with pleomorphic carcinoma, spindle cell carcinoma, carcinosarcoma, and pulmonary blastoma, which are (arguably) related variants. While the 4th revision ("WHO-2004") retained the same grouping of lesions as the 3rd revision, the name of the major taxon was shortened to "sarcomatoid carcinomas".[1]

The current rules for classifying lung cancers under WHO-2004, while useful and improved, remain to some extent fairly complex, ambiguous, arbitrary, and incomplete.[1] Although it is fairly common for mixed tumors that are seen to contain malignant giant cells to be called "giant-cell carcinomas", accurate classification of a pulmonary tumor as a GCCL requires that the entire tumor consists only of malignant giant cells. Therefore, complete sampling of the entire tumor — obtained via a surgical resection — is absolutely necessary for a definitive diagnosis of GCCL to be made.[1]

Cytology edit

The background contained numerous lymphocytes and neutrophils. The shape of the tumor cell was spindle or pleomorphic, and the sizes of the tumor cells varied by more than 5-fold. The tumor cells had an abundant, thick and well-demarcated cytoplasm. The location of the nucleus was centrifugal, and the nucleus was oval or irregularly shaped. Multinucleated giant cells were frequently observed. The size of the nucleus was more than 5 times that of normal lymphocytes, and its size also varied by more than 5-fold. The nuclear membrane was thin, and nuclear chromatin was coarsely granular, while the nucleolus was single and round.

In cytological preparations, giant cells typically appear as single cells or in flat loose clusters, and occasionally in fascicles.[8]

GCCL are considered a member of the most common type of lung cancer, called "non-small-cell carcinomas". This group of lethal neoplasms make up approximately 85% of all lung cancers.[1] By the definition of "large-vs.-small-cell carcinoma", the diameter of GCCL cells must be considerably greater than three times that of a resting (i.e. unstimulated) lymphocyte. Also by definition, GCCL do not contain any amount of these small, neurosecretory granule-containing, neuroendocrine cells that are characteristic of small-cell carcinomas — when they do, the tumor should be classified as a combined small-cell carcinoma.[1]

Compared to most other lung cancer variants, cells comprising GCCL tend to be much larger (up to 150 micrometers diameter, or even larger),[9] Both cells and nuclei show extreme variation in size distribution and shape. Carcinomatous giant cells carcinoma nuclei have been reported to average 5 times the size of lymphocyte nuclei.[8]

The cells from giant-cell carcinomas are anaplastic, and show no evidence of cell maturation or differentiation, lacking the cytological and tissue architectural characteristics of squamous cell carcinoma, adenocarcinoma, neuroendocrine carcinomas, or other more differentiated lung cancer cell types. They tend to be highly pleomorphic (i.e. variable in characteristics), but are most often round and/or polygonal in shape, with a relatively low nuclear-to-cytoplasmic ratio. When associated with spindle cells, as they very frequently are in tumors with mixed histology, malignant giant cells tend to form loosely cohesive aggregate structures on cytological examination. However, when a biopsy sample consists purely of malignant giant cells, the cells tend to be single and disaggregated.[1]

Case series suggest that the relative number of giant cells in a given tumor are generally directly proportional to the size of the tumor, and to the relative amount of necrosis.[10]

Giant cells in a lung cancer are highly associated with the presence of spindle cells.[11]

The chromatin of malignant giant cells tends to be hyperchromatic and coarsely clumped. Nucleoli are usually multiple and prominent.[9]

Subcellular characteristics often noted in the malignant giant cells of GCCL cases include abundant mitochondria, concentric whorls of tonofilament-like fibrils, and aggregates of several pairs of centrioles.[12]

Both "tumor cell-tumor cell" and "leukocyte-tumor cell" emperipolesis (i.e. active penetration of the latter by the former) is very commonly seen in cases of GCCL.[12]

Tissue architectural features edit

In mixed tumors, giant cells are more likely to be found in higher proportions at the edge of a tumor.[11] When extensive necrosis is present, it is possible for a giant-cell tumor to have only a thin rim of viable cells remaining at the perimeter of the mass.[citation needed]

In one early case series, abundant production of loose malignant giant cells were noted to fill the alveoli of patients without destroying, infiltrating, or disturbing the normal underlying architecture, a pathologic behavior that bears some resemblance to the pneumonic variant of bronchioloalveolar carcinoma.[13]

Extensive tumor necrosis and hemorrhage is extremely common in GCCL.[13]

Although the issue has not been extensively studied in a controlled fashion, GCCLs have been noted to contain significantly elevated levels of VEGF.[14] However, in one study where a giant-cell carcinoma tumor that had been completely excised was sectioned and examined, no qualitative or quantitative abnormalities in tissue vascularization were noted.[9]

GCCL have been noted to be encapsulated, and to be divided via septa into "pseudolobules", by a highly fibrous stroma, suggested to be produced commensurately with tumor growth. The capsule is typically infiltrated with malignant giant cells.[15]

Macroscopic features edit

Giant-cell carcinomas of the lung frequently show extensive necrosis[15] and myxoid degeneration.[11]

A trend toward less vascularity and tissue density (with lower contrast enhancement on CT) has been noted toward the center of these lesions, especially in larger tumors, and even in tumors without a significant volume of gross necrosis.[16]

Grossly, the cut surfaces of these malignancies are often gray-white or tan, and frequently show myxoid, necrotic, and/or hemorrhagic foci.[16] These sorts of areas often show low levels of contrast enhancement on CT scanning.[citation needed]

Low encapsularity and high levels of tissue collagen tend to be observed, with high contrast enhancement in these areas.[16]

GCCL have been seen to develop from/in emphysematous bullae.[17]

Staining and immunohistochemistry edit

A case of a brain metastasis from a giant-cell lung carcinoma (both "pure") tested positive for cytokeratins AE1/AE3, and negative for CK-7, CK-20, TTF-1, and GFAP.[18]

GCCL cells often stain intensely by Periodic acid-Schiff reagent, suggesting the presence of significant amounts of glycogen in the cell cytoplasm.[15]

Differential diagnosis edit

Under light microscopy, the giant malignant pleomorphic cells making up a GCCL resemble those found in choriocarcinoma,[1] angiosarcoma,[19] and some forms of true sarcoma,[1] such as malignant fibrous histiocytoma[1] and rhabdomyosarcoma.[9] In some instances, they can also bear considerable resemblance to "activated" histiocytes seen in some inflammatory conditions.[9]

A rare and potentially difficult differential diagnostic dilemma occurs when GCCLs must be separated from pulmonary or mediastinal choriocarcinomas, a critical distinction to be made because while there is a known standard of care for treating choriocarcinoma, as yet there is no generally accepted specific standard treatment for GCCL. Careful review of cell morphology is key to their delineation — while GCCLs show great variation in cell size distributions and morphologies in tumors, choriocarcinomas consistently contain only syncytiotrophoblasts and cytotrophoblasts.[20] GCCL and primary pulmonary choriocarcinoma can also be differentiated on the basis of ultrastructural features by electron microscopy, although EM is not yet widely applicable.[21]

Occasionally, a bone metastasis of a GCCL could potentially be mistaken for a primary giant-cell tumor of bone[22] — the latter entity can behave as a neoplasm of benign, frankly malignant,[23] or borderline[24] in its clinical behavior.[25]

Sites of metastasis edit

GCCLs are particularly notable among lung cancers for their extremely unusual tendency to metastasize to the small intestine, occasionally causing obstruction, severe bleeding, and/or intussusception. This clinical characteristic of GCCL has been seen in cases spanning over half a century in time.[26][27]

Within the small bowel, the jejunum seems to be a preferred site for metastasis of GCCL.

GCCL also often metastasizes to bone,[22] adrenal, brain,[18] lung, liver, kidney,

Brain metastases from GCCL are particularly likely to cause significant cerebral hemorrhages as compared to other lung cancer variants, probably due to greatly increased rates of endothelial proliferation and neovascularization, tumor tissue growth, extensive necrosis, and aggressive local infiltrative character of GCCL cells.[18]

Pathogenesis edit

Several studies, both in giant-cell tumor specimens and in cell lines, have identified rearrangement and amplification of the c-myc oncogene, sometimes in combination with mutations of the K-ras gene.[28][29]

Overexpression of vascular endothelial growth factor (VEGF) has been shown to occur in GCCL and is thought to be related to the high metastatic potential of this lung cancer variant.[14]

Malignant giant cells identical to those found in GCCL commonly occur in lung cancer cases with a prominent major or minor clear-cell carcinoma pattern (for a discussion about this variant, see for example[30]). They have been hypothesized to derive from an undifferentiated multipotent malignant stem cell precursor that is generated in distal bronchioles via an as yet unknown oncogenetic pathway or oncogenetic driver.[12]

Ultrastructurally, malignant giant cells often contain accumulations of microfilaments arranged in whorls near the cell nucleus. These entities appear similar in structure to microfilaments and bundles found in the D1 cell of the gastro-entero-pancreatic endocrine system, and it has been proposed that these D1 cells may be the cancer stem cell for at least some GCCLs. Identically appearing whorled filament structures have also been produced in certain airway cells of animals after treatment with carcinogenic nitrosamines.[31]

Ultrastructural studies have suggested that the malignant giant cells in GCCL are of endodermal lineage.[32]

Remarkably fast growing tumors.[18]

Combined/multiphasic tumors containing giant cells edit

Malignant giant cells are commonly found — and vary in relative proportion to a greater or lesser degree — in both primary tumors and metastatases of many different variants of lung carcinomas. A number of authors have noted that bizarre malignant giant cells occur more commonly in primary and secondary tumors — including any remaining tumor "deposits" — that have previously been treated with chemotherapy and/or radiation therapy in adjuvant or neoadjuvant protocols.[32]

Imaging characteristics edit

GCCL often presents as a large peripheral mass that is severely cavitated.[33]

In a radiographic study of almost 2,000 lung cancer patients published 50 years ago, 3.4% of lung carcinomas proved to be cavitated masses,[34] most of which were squamous cell carcinoma.

In a number of cases of severe cavitation, the resected tumor remnant consists of only a thin rim of proliferating cells.[citation needed]

Positron emission tomography scanning edit

On positron emission tomography (PET) scanning, GCCL has been found to have exceedingly high standardized uptake values (SUV) for radioactive glucose, values that are statistically significantly higher than in other histological variants of lung cancer.[35]

Metabolic pathways edit

PET scanning suggests that GCCL are tumors with particularly rapid metabolism, and that the metabolic pathways of GCCL may be unusually dependent on, or interlinked to, glycolysis.[35]

Paraneoplastic syndromes edit

GCCL have been long known[36] for secretion of the beta subunit of human chorionic gonadotropin (beta-HCG), often in large amounts, which can lead to very high levels of estrogen and painful gynecomastia (breast enlargement) in males as paraneoplastic signs.[37]

Giant-cell lung cancers are well known for their paraneoplastic production and secretion of granulopoietic colony stimulating factor (G-CSF)[29][38]

GCCL has also been reported to produce plasminogen activator as a paraneoplastic phenomenon.[9]

Treatment edit

Because of its rarity, there have been no randomized clinical trials of treatment of GCCL, and all information available derives from small retrospective institutional series or multicenter metadata.[39]

Prognosis edit

Giant-cell lung cancers have long been considered to be exceptionally aggressive malignancies[40][15][41] that grow very rapidly[29] and have a very poor prognosis.[42]

Many small series have suggested that the prognosis of lung tumors with giant cells is worse than that of most other forms of non-small-cell lung cancer (NSCLC),[11] including squamous cell carcinoma,[42] and spindle cell carcinoma.[42]

The overall five-year survival rate in GCCL varies between studies but is generally considered to be very low. The (US) Armed Forces Institute of Pathology has reported a figure of 10%,[43] and in a study examining over 150,000 lung cancer cases, a figure of 11.8% was given.[5] However, in the latter report the 11.8% figure was based on data that included spindle cell carcinoma, a variant which is generally considered to have a less dismal prognosis than GCCL.[11] Therefore, the likely survival of "pure" GCCL is probably lower than the stated figure.

In the large 1995 database review by Travis and colleagues, giant-cell carcinoma has the third-worst prognosis among 18 histological forms of lung cancer. (Only small-cell carcinoma and large-cell carcinoma had shorter average survival.)[5]

Most GCCL have already grown and invaded locally and/or regionally, and/or have already metastasized distantly, and are inoperable, at the time of diagnosis.[15]

Epidemiology edit

The true incidence, prevalence, and mortality of GCCL is generally unknown due to a lack of accurate cancer data on a national level. It is known to be a very rare tumor variant in all populations examined, however. In an American study of a database of over 60,000 lung cancers, GCCL comprised between 0.3% and 0.4% of primary pulmonary malignancies, with an age-adjusted incidence rate of about 3 new cases per million persons per year.[5] With approximately 220,000 total lung cancers diagnosed in the US each year,[44] the proportion suggests that approximately 660 and 880 new cases are diagnosed in Americans annually.[5][45]

However, in a more recent series of 4,212 consecutive lung cancer cases, only one (0.024%) lesion was determined to be a "pure" giant-cell carcinoma after complete sectioning of all available tumor tissue.[35] While some evidence suggests GCCL may have been considerably more common several decades ago, with one series identifying 3.4% of all lung carcinomas as giant-cell malignancies,[46] it is possible that this number reflect

Most published case series and reports on giant cell-containing lung cancers show that they are diagnosed much more frequently in men than they are in women,[16][42] with some studies showing extremely high male-to-female ratios (12:1 or more). In a study of over 150,000 people with lung cancer in the US, however, the gender ratio was just over 2:1, with women actually having a higher relative proportion of giant-cell cancers (0.4%) than men (0.3%).[5]

Giant-cell carcinomas have been reported to be diagnosed in a significantly younger population than all non-small-cell carcinomas considered as a group.[16][40] Like nearly all lung carcinomas, however, GCCs are exceedingly rare in very young people: in the US SEER program, only 2 cases were recorded to occur in persons younger than 30 years of age between 1983 and 1987.[5] The average age at diagnosis of these tumors has been estimated at 60 years.[16]

The vast majority of individuals with GCCL are heavy smokers.[16]

Although the definitions of "central" and "peripheral" can vary[16] between studies, GCCL are consistently diagnosed much more frequently in the lung periphery.[16] In a review of literature compiled by Kallenburg and co-workers, less than 30% of GCCLs arose in the hilum or other parts of the "central" pulmonary tree.[40]

A significant predilection for genesis of GCCL in the upper lobes of patients has also been postulated.[16]

History edit

Most sources credit Nash and Stout with publishing the first detailed report in the medical literature recognizing GCCL as a distinct clinicopathological entity in 1958.[47] However, there is some evidence that suggests this tumor phenotype was described as early as 1951.[13] In a report on 3 cases of giant-cell lung carcinoma published in 1961 by Z.M. Naib, the author cites 2 previous studies related to GCCL — one published in 1951 by M.M. Patton and co-workers,[48] and one published in 1955 by Walton and Pryce.[49] In 1969, Dr. Alexander Kennedy, in a case series of 3 GCCL Kennedy published in 1969,[15] credited Hadley and Bullock with the first usage of the term "giant-cell carcinoma" 16 years prior.[50]

GCCL was first confirmed as an epithelial tumor (and not a dedifferentiated pleomorphic sarcoma) in 1961.[51] In 1964–65, theories were postulated that GCCLs were dediffentiated adenocarcinomas[52] and, in some cases, were thought to derive from clear-cell adenocarcinomas.[30]

References edit

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External links edit

  • . World Health Organization Classification of Tumours. Archived from the original on 2015-11-15. Retrieved 2010-06-02. (Download Page).
  • "Lung cancer page". National Cancer Institute.

December 15, 2023
giant, cell, carcinoma, lung, this, article, needs, editing, comply, with, wikipedia, manual, style, particular, problems, with, using, medmos, please, help, improve, content, june, 2018, learn, when, remove, this, template, message, gccl, rare, histological, . This article needs editing to comply with Wikipedia s Manual of Style In particular it has problems with not using MEDMOS Please help improve the content June 2018 Learn how and when to remove this template message Giant cell carcinoma of the lung GCCL is a rare histological form of large cell lung carcinoma a subtype of undifferentiated lung cancer traditionally classified within the non small cell lung carcinomas NSCLC Giant cell carcinoma of the lungPulmonary giant cell carcinoma represents a rare variety of non small cell lung carcinoma that is characterized by the presence of numerous tumor giant cells and an influx of inflammatory cells that are mostly polymorphonuclear leukocytes admixed with macrophages The dense oval aggregates of polymorphonuclear leukocytes seen in this image are probably located in the cytoplasm of tumor giant cells emperiopolesis that have been sectioned in a plane that does not include their nuclei SpecialtyOncology The characteristic feature of this highly lethal malignancy is the distinctive light microscopic appearance of its extremely large cells which are bizarre and highly pleomorphic and which often contain more than one huge misshapen pleomorphic nucleus syncytia which result from cell fusion Although it is common in the lung cancer literature to refer to histologically mixed tumors containing significant numbers of malignant giant cells as giant cell carcinomas technically a diagnosis of giant cell carcinoma should be limited strictly to neoplasms containing only malignant giant cells i e pure giant cell carcinoma 1 Aside from the great heterogeneity seen in lung cancers especially those occurring among tobacco smokers the considerable variability in diagnostic and sampling techniques used in medical practice the high relative proportion of individuals with suspected GCCL who do not undergo complete surgical resection and the near universal lack of complete sectioning and pathological examination of resected tumor specimens prevent high levels of quantitative accuracy Contents 1 Classification 2 Cytology 3 Tissue architectural features 4 Macroscopic features 5 Staining and immunohistochemistry 6 Differential diagnosis 7 Sites of metastasis 8 Pathogenesis 9 Combined multiphasic tumors containing giant cells 10 Imaging characteristics 11 Positron emission tomography scanning 12 Metabolic pathways 13 Paraneoplastic syndromes 14 Treatment 15 Prognosis 16 Epidemiology 17 History 18 References 19 External linksClassification editFor several decades primary lung cancers were consistently dichotomously classified for treatment and research purposes into small cell lung carcinomas SCLCs and non small cell lung carcinomas NSCLCs based on an oversimplified approach that is now clearly outmoded The new paradigm recognizes that lung cancers are a large and extremely heterogeneous family of malignant neoplasms 2 with over 50 different histological variants included in the 4th 2004 revision of the World Health Organization typing system the most widely used lung cancer classification scheme WHO 2004 1 These variants are increasingly appreciated as having different genetic biological and clinical properties including prognoses and responses to treatment regimens and therefore that correct and consistent histological classification of lung cancers are necessary to validate and implement optimum management strategies 3 4 About 1 of lung cancers are sarcomas germ cell tumors and hematopoietic tumors while 99 of lung cancers are carcinoma Carcinomas are tumors composed of transformed abnormal cells with epithelial tissue architecture and or molecular characteristics and which derive from embryonic endoderm 5 Eight major taxa of lung carcinomas are recognized within the WHO 2004 classification 1 Small cell carcinoma Squamous cell carcinoma Adenocarcinoma Large cell carcinoma Adenosquamous carcinoma Sarcomatoid carcinoma Carcinoid Salivary gland like carcinomaThe subclassification of GCCL among these major taxa has undergone significant changes in recent decades Under the 2nd revision 1981 of the WHO classification it was considered a subtype of large cell carcinoma 6 In the 3rd 1999 revision 7 it was placed within a taxon called Carcinomas with Pleomorphic Sarcomatoid or Sarcomatous Elements along with pleomorphic carcinoma spindle cell carcinoma carcinosarcoma and pulmonary blastoma which are arguably related variants While the 4th revision WHO 2004 retained the same grouping of lesions as the 3rd revision the name of the major taxon was shortened to sarcomatoid carcinomas 1 The current rules for classifying lung cancers under WHO 2004 while useful and improved remain to some extent fairly complex ambiguous arbitrary and incomplete 1 Although it is fairly common for mixed tumors that are seen to contain malignant giant cells to be called giant cell carcinomas accurate classification of a pulmonary tumor as a GCCL requires that the entire tumor consists only of malignant giant cells Therefore complete sampling of the entire tumor obtained via a surgical resection is absolutely necessary for a definitive diagnosis of GCCL to be made 1 Cytology editThe background contained numerous lymphocytes and neutrophils The shape of the tumor cell was spindle or pleomorphic and the sizes of the tumor cells varied by more than 5 fold The tumor cells had an abundant thick and well demarcated cytoplasm The location of the nucleus was centrifugal and the nucleus was oval or irregularly shaped Multinucleated giant cells were frequently observed The size of the nucleus was more than 5 times that of normal lymphocytes and its size also varied by more than 5 fold The nuclear membrane was thin and nuclear chromatin was coarsely granular while the nucleolus was single and round In cytological preparations giant cells typically appear as single cells or in flat loose clusters and occasionally in fascicles 8 GCCL are considered a member of the most common type of lung cancer called non small cell carcinomas This group of lethal neoplasms make up approximately 85 of all lung cancers 1 By the definition of large vs small cell carcinoma the diameter of GCCL cells must be considerably greater than three times that of a resting i e unstimulated lymphocyte Also by definition GCCL do not contain any amount of these small neurosecretory granule containing neuroendocrine cells that are characteristic of small cell carcinomas when they do the tumor should be classified as a combined small cell carcinoma 1 Compared to most other lung cancer variants cells comprising GCCL tend to be much larger up to 150 micrometers diameter or even larger 9 Both cells and nuclei show extreme variation in size distribution and shape Carcinomatous giant cells carcinoma nuclei have been reported to average 5 times the size of lymphocyte nuclei 8 The cells from giant cell carcinomas are anaplastic and show no evidence of cell maturation or differentiation lacking the cytological and tissue architectural characteristics of squamous cell carcinoma adenocarcinoma neuroendocrine carcinomas or other more differentiated lung cancer cell types They tend to be highly pleomorphic i e variable in characteristics but are most often round and or polygonal in shape with a relatively low nuclear to cytoplasmic ratio When associated with spindle cells as they very frequently are in tumors with mixed histology malignant giant cells tend to form loosely cohesive aggregate structures on cytological examination However when a biopsy sample consists purely of malignant giant cells the cells tend to be single and disaggregated 1 Case series suggest that the relative number of giant cells in a given tumor are generally directly proportional to the size of the tumor and to the relative amount of necrosis 10 Giant cells in a lung cancer are highly associated with the presence of spindle cells 11 The chromatin of malignant giant cells tends to be hyperchromatic and coarsely clumped Nucleoli are usually multiple and prominent 9 Subcellular characteristics often noted in the malignant giant cells of GCCL cases include abundant mitochondria concentric whorls of tonofilament like fibrils and aggregates of several pairs of centrioles 12 Both tumor cell tumor cell and leukocyte tumor cell emperipolesis i e active penetration of the latter by the former is very commonly seen in cases of GCCL 12 Tissue architectural features editIn mixed tumors giant cells are more likely to be found in higher proportions at the edge of a tumor 11 When extensive necrosis is present it is possible for a giant cell tumor to have only a thin rim of viable cells remaining at the perimeter of the mass citation needed In one early case series abundant production of loose malignant giant cells were noted to fill the alveoli of patients without destroying infiltrating or disturbing the normal underlying architecture a pathologic behavior that bears some resemblance to the pneumonic variant of bronchioloalveolar carcinoma 13 Extensive tumor necrosis and hemorrhage is extremely common in GCCL 13 Although the issue has not been extensively studied in a controlled fashion GCCLs have been noted to contain significantly elevated levels of VEGF 14 However in one study where a giant cell carcinoma tumor that had been completely excised was sectioned and examined no qualitative or quantitative abnormalities in tissue vascularization were noted 9 GCCL have been noted to be encapsulated and to be divided via septa into pseudolobules by a highly fibrous stroma suggested to be produced commensurately with tumor growth The capsule is typically infiltrated with malignant giant cells 15 Macroscopic features editGiant cell carcinomas of the lung frequently show extensive necrosis 15 and myxoid degeneration 11 A trend toward less vascularity and tissue density with lower contrast enhancement on CT has been noted toward the center of these lesions especially in larger tumors and even in tumors without a significant volume of gross necrosis 16 Grossly the cut surfaces of these malignancies are often gray white or tan and frequently show myxoid necrotic and or hemorrhagic foci 16 These sorts of areas often show low levels of contrast enhancement on CT scanning citation needed Low encapsularity and high levels of tissue collagen tend to be observed with high contrast enhancement in these areas 16 GCCL have been seen to develop from in emphysematous bullae 17 Staining and immunohistochemistry editA case of a brain metastasis from a giant cell lung carcinoma both pure tested positive for cytokeratins AE1 AE3 and negative for CK 7 CK 20 TTF 1 and GFAP 18 GCCL cells often stain intensely by Periodic acid Schiff reagent suggesting the presence of significant amounts of glycogen in the cell cytoplasm 15 Differential diagnosis editUnder light microscopy the giant malignant pleomorphic cells making up a GCCL resemble those found in choriocarcinoma 1 angiosarcoma 19 and some forms of true sarcoma 1 such as malignant fibrous histiocytoma 1 and rhabdomyosarcoma 9 In some instances they can also bear considerable resemblance to activated histiocytes seen in some inflammatory conditions 9 A rare and potentially difficult differential diagnostic dilemma occurs when GCCLs must be separated from pulmonary or mediastinal choriocarcinomas a critical distinction to be made because while there is a known standard of care for treating choriocarcinoma as yet there is no generally accepted specific standard treatment for GCCL Careful review of cell morphology is key to their delineation while GCCLs show great variation in cell size distributions and morphologies in tumors choriocarcinomas consistently contain only syncytiotrophoblasts and cytotrophoblasts 20 GCCL and primary pulmonary choriocarcinoma can also be differentiated on the basis of ultrastructural features by electron microscopy although EM is not yet widely applicable 21 Occasionally a bone metastasis of a GCCL could potentially be mistaken for a primary giant cell tumor of bone 22 the latter entity can behave as a neoplasm of benign frankly malignant 23 or borderline 24 in its clinical behavior 25 Sites of metastasis editGCCLs are particularly notable among lung cancers for their extremely unusual tendency to metastasize to the small intestine occasionally causing obstruction severe bleeding and or intussusception This clinical characteristic of GCCL has been seen in cases spanning over half a century in time 26 27 Within the small bowel the jejunum seems to be a preferred site for metastasis of GCCL GCCL also often metastasizes to bone 22 adrenal brain 18 lung liver kidney Brain metastases from GCCL are particularly likely to cause significant cerebral hemorrhages as compared to other lung cancer variants probably due to greatly increased rates of endothelial proliferation and neovascularization tumor tissue growth extensive necrosis and aggressive local infiltrative character of GCCL cells 18 Pathogenesis editSeveral studies both in giant cell tumor specimens and in cell lines have identified rearrangement and amplification of the c myc oncogene sometimes in combination with mutations of the K ras gene 28 29 Overexpression of vascular endothelial growth factor VEGF has been shown to occur in GCCL and is thought to be related to the high metastatic potential of this lung cancer variant 14 Malignant giant cells identical to those found in GCCL commonly occur in lung cancer cases with a prominent major or minor clear cell carcinoma pattern for a discussion about this variant see for example 30 They have been hypothesized to derive from an undifferentiated multipotent malignant stem cell precursor that is generated in distal bronchioles via an as yet unknown oncogenetic pathway or oncogenetic driver 12 Ultrastructurally malignant giant cells often contain accumulations of microfilaments arranged in whorls near the cell nucleus These entities appear similar in structure to microfilaments and bundles found in the D1 cell of the gastro entero pancreatic endocrine system and it has been proposed that these D1 cells may be the cancer stem cell for at least some GCCLs Identically appearing whorled filament structures have also been produced in certain airway cells of animals after treatment with carcinogenic nitrosamines 31 Ultrastructural studies have suggested that the malignant giant cells in GCCL are of endodermal lineage 32 Remarkably fast growing tumors 18 Combined multiphasic tumors containing giant cells editMalignant giant cells are commonly found and vary in relative proportion to a greater or lesser degree in both primary tumors and metastatases of many different variants of lung carcinomas A number of authors have noted that bizarre malignant giant cells occur more commonly in primary and secondary tumors including any remaining tumor deposits that have previously been treated with chemotherapy and or radiation therapy in adjuvant or neoadjuvant protocols 32 Imaging characteristics editGCCL often presents as a large peripheral mass that is severely cavitated 33 In a radiographic study of almost 2 000 lung cancer patients published 50 years ago 3 4 of lung carcinomas proved to be cavitated masses 34 most of which were squamous cell carcinoma In a number of cases of severe cavitation the resected tumor remnant consists of only a thin rim of proliferating cells citation needed Positron emission tomography scanning editOn positron emission tomography PET scanning GCCL has been found to have exceedingly high standardized uptake values SUV for radioactive glucose values that are statistically significantly higher than in other histological variants of lung cancer 35 Metabolic pathways editPET scanning suggests that GCCL are tumors with particularly rapid metabolism and that the metabolic pathways of GCCL may be unusually dependent on or interlinked to glycolysis 35 Paraneoplastic syndromes editGCCL have been long known 36 for secretion of the beta subunit of human chorionic gonadotropin beta HCG often in large amounts which can lead to very high levels of estrogen and painful gynecomastia breast enlargement in males as paraneoplastic signs 37 Giant cell lung cancers are well known for their paraneoplastic production and secretion of granulopoietic colony stimulating factor G CSF 29 38 GCCL has also been reported to produce plasminogen activator as a paraneoplastic phenomenon 9 Treatment editBecause of its rarity there have been no randomized clinical trials of treatment of GCCL and all information available derives from small retrospective institutional series or multicenter metadata 39 Prognosis editGiant cell lung cancers have long been considered to be exceptionally aggressive malignancies 40 15 41 that grow very rapidly 29 and have a very poor prognosis 42 Many small series have suggested that the prognosis of lung tumors with giant cells is worse than that of most other forms of non small cell lung cancer NSCLC 11 including squamous cell carcinoma 42 and spindle cell carcinoma 42 The overall five year survival rate in GCCL varies between studies but is generally considered to be very low The US Armed Forces Institute of Pathology has reported a figure of 10 43 and in a study examining over 150 000 lung cancer cases a figure of 11 8 was given 5 However in the latter report the 11 8 figure was based on data that included spindle cell carcinoma a variant which is generally considered to have a less dismal prognosis than GCCL 11 Therefore the likely survival of pure GCCL is probably lower than the stated figure In the large 1995 database review by Travis and colleagues giant cell carcinoma has the third worst prognosis among 18 histological forms of lung cancer Only small cell carcinoma and large cell carcinoma had shorter average survival 5 Most GCCL have already grown and invaded locally and or regionally and or have already metastasized distantly and are inoperable at the time of diagnosis 15 Epidemiology editThe true incidence prevalence and mortality of GCCL is generally unknown due to a lack of accurate cancer data on a national level It is known to be a very rare tumor variant in all populations examined however In an American study of a database of over 60 000 lung cancers GCCL comprised between 0 3 and 0 4 of primary pulmonary malignancies with an age adjusted incidence rate of about 3 new cases per million persons per year 5 With approximately 220 000 total lung cancers diagnosed in the US each year 44 the proportion suggests that approximately 660 and 880 new cases are diagnosed in Americans annually 5 45 However in a more recent series of 4 212 consecutive lung cancer cases only one 0 024 lesion was determined to be a pure giant cell carcinoma after complete sectioning of all available tumor tissue 35 While some evidence suggests GCCL may have been considerably more common several decades ago with one series identifying 3 4 of all lung carcinomas as giant cell malignancies 46 it is possible that this number reflectMost published case series and reports on giant cell containing lung cancers show that they are diagnosed much more frequently in men than they are in women 16 42 with some studies showing extremely high male to female ratios 12 1 or more In a study of over 150 000 people with lung cancer in the US however the gender ratio was just over 2 1 with women actually having a higher relative proportion of giant cell cancers 0 4 than men 0 3 5 Giant cell carcinomas have been reported to be diagnosed in a significantly younger population than all non small cell carcinomas considered as a group 16 40 Like nearly all lung carcinomas however GCCs are exceedingly rare in very young people in the US SEER program only 2 cases were recorded to occur in persons younger than 30 years of age between 1983 and 1987 5 The average age at diagnosis of these tumors has been estimated at 60 years 16 The vast majority of individuals with GCCL are heavy smokers 16 Although the definitions of central and peripheral can vary 16 between studies GCCL are consistently diagnosed much more frequently in the lung periphery 16 In a review of literature compiled by Kallenburg and co workers less than 30 of GCCLs arose in the hilum or other parts of the central pulmonary tree 40 A significant predilection for genesis of GCCL in the upper lobes of patients has also been postulated 16 History editMost sources credit Nash and Stout with publishing the first detailed report in the medical literature recognizing GCCL as a distinct clinicopathological entity in 1958 47 However there is some evidence that suggests this tumor phenotype was described as early as 1951 13 In a report on 3 cases of giant cell lung carcinoma published in 1961 by Z M Naib the author cites 2 previous studies related to GCCL one published in 1951 by M M Patton and co workers 48 and one published in 1955 by Walton and Pryce 49 In 1969 Dr Alexander Kennedy in a case series of 3 GCCL Kennedy published in 1969 15 credited Hadley and Bullock with the first usage of the term giant cell carcinoma 16 years prior 50 GCCL was first confirmed as an epithelial tumor and not a dedifferentiated pleomorphic sarcoma in 1961 51 In 1964 65 theories were postulated that GCCLs were dediffentiated adenocarcinomas 52 and in some cases were thought to derive from clear cell adenocarcinomas 30 References edit a b c d e f g h i j k l Travis WD Brambilla E Muller Hermelink HK Harris CC eds 2004 Pathology and Genetics of Tumours of the Lung Pleura Thymus and Heart PDF World Health Organization Classification of Tumours Lyon IARC Press ISBN 92 832 2418 3 Archived from the original PDF on 21 July 2011 Retrieved 27 March 2010 Roggli VL Vollmer RT Greenberg SD McGavran MH Spjut HJ Yesner R 1985 Lung cancer heterogeneity a blinded and randomized study of 100 consecutive cases Hum Pathol 16 6 569 79 doi 10 1016 s0046 8177 85 80106 4 PMID 2987102 Rossi G Marchioni A 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pulmonary pleomorphic and giant cell carcinomas Acta Cytol 55 2 173 9 doi 10 1159 000320860 PMID 21325803 S2CID 39144324 a b c d e f Davidson JF McNicol GP Frank GL Anderson TJ Douglas AS January 1969 Plasminogen activator producing tumour Br Med J 1 5636 88 91 doi 10 1136 bmj 1 5636 88 PMC 1982019 PMID 5761832 Cacic M Oberman B Dvornik G December 1989 Investigation of the applicability of histological classification of bronchial carcinoma according to the World Health Organization Tumori 75 6 580 2 doi 10 1177 030089168907500613 PMID 2482566 S2CID 11142517 a b c d e Matsui K Kitagawa M May 1991 Spindle cell carcinoma of the lung A clinicopathologic study of three cases Cancer 67 9 2361 7 doi 10 1002 1097 0142 19910501 67 9 lt 2361 aid cncr2820670925 gt 3 0 co 2 3 PMID 1707339 a b c Wang NS Seemayer TA Ahmed MN Knaack J January 1976 Giant cell carcinoma of the lung A light and electron microscopic study Hum Pathol 7 1 3 16 doi 10 1016 s0046 8177 76 80003 2 PMID 172430 a b c Naib ZM 1961 Giant cell carcinoma of the lung cytological study of the exfoliated cells in sputa and bronchial washings Dis Chest 40 69 73 doi 10 1378 chest 40 1 69 PMID 13727525 S2CID 19208368 a b Jiang DF Lu YL Qiu ZY et al 2003 Study of differential expression of molecules affecting the metastatic potential between highly and poorly metastatic human lung giant cell carcinoma Zhonghua Zhong Liu Za Zhi 25 131 4 a b c d e f Kennedy A May 1969 Pathology and survival in operable cases of giant cell carcinoma of the lung J Clin Pathol 22 3 354 60 doi 10 1136 jcp 22 3 354 PMC 474089 PMID 5784984 a b c d e f g h i j Kim TH Kim SJ Ryu YH et al August 2004 Pleomorphic carcinoma of lung comparison of CT features and pathologic findings Radiology 232 2 554 9 doi 10 1148 radiol 2322031201 PMID 15215543 Shirakusa T Shigematsu N Koga T Yamagata Y 1980 Giant cell carcinoma arising in a pulmonary bulla Scand J Thorac Cardiovasc Surg 14 3 307 9 doi 10 3109 14017438009101017 PMID 7221506 a b c d Hagihara N 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Simpson JA March 1953 Carcinomatous abscess of the lung Thorax 8 1 11 26 doi 10 1136 thx 8 1 11 PMC 1019223 PMID 13038734 a b c Park JS Lee Y Han J et al 2011 Clinicopathologic outcomes of curative resection for sarcomatoid carcinoma of the lung Oncology 81 3 4 206 13 doi 10 1159 000333095 PMID 22076573 S2CID 25558721 Dailey JE Marcuse PM August 1969 Gonadotropin secreting giant cell carcinoma of the lung Cancer 24 2 388 96 doi 10 1002 1097 0142 196908 24 2 lt 388 aid cncr2820240222 gt 3 0 co 2 7 PMID 5796783 S2CID 3506191 Yaturu S Harrara E Nopajaroonsri C Singal R Gill S 2003 Gynecomastia attributable to a human chorionic gonadotropin secreting giant cell carcinoma of the lung Endocr Pract 9 3 231 5 doi 10 4158 EP 9 3 233 PMID 12917067 Kameda T Kodama T Shimosato Y 1982 Shimosato Y Melamed MR Nettesheim P eds Morphogenesis of Lung Cancer Vol 2 Boca Raton Florida CRC Press pp 107 29 Bae HM Min HS Lee SH Kim DW Chung DH Lee JS Kim YW Heo DS October 2007 Palliative chemotherapy for pulmonary pleomorphic carcinoma Lung Cancer 58 1 112 5 doi 10 1016 j lungcan 2007 05 006 PMID 17574296 a b c Kallenberg F Jaque J 1979 Giant cell carcinoma of the lung Clinical and pathological assessment Comparison with other large cell anaplastic bronchogenic carcinomas Scand J Thorac Cardiovasc Surg 13 3 343 6 doi 10 3109 14017437909100576 PMID 542838 Razzuk MA Urschel HC Albers JE Martin JA Paulson DL June 1976 Pulmonary giant cell carcinoma Ann Thorac Surg 21 6 540 5 doi 10 1016 s0003 4975 10 63926 4 PMID 1275605 a b c d Zhao ZL Song N Huang QY Liu YP Zhao HR February 2007 Clinicopathologic features of lung pleomorphic spindle giant cell carcinoma a report of 17 cases Clinicopathologic features of lung pleomorphic spindle giant cell carcinoma a report of 17 cases AI Zheng in Chinese 26 2 183 8 PMID 17298750 Chinese text Archived 2013 01 15 at archive today Colby TV Koss MN Travis WD 1995 Tumors of the lower respiratory tract In Rosai J Sobin LH eds Atlas of Tumor Pathology Washington DC Armed Forces Institute of Pathology pp 259 75 Fact Sheet Cancer of the Lung and Bronchus National Cancer Institute SEER Program Retrieved February 24 2012 Martin LW Correa AM Ordonez NG et al September 2007 Sarcomatoid carcinoma of the lung a predictor of poor prognosis Ann Thorac Surg 84 3 973 80 doi 10 1016 j athoracsur 2007 03 099 PMID 17720411 Hellstrom HR Fisher ER 1963 Giant cell carcinoma of lung Cancer 16 8 1080 8 doi 10 1002 1097 0142 196308 16 8 lt 1080 aid cncr2820160816 gt 3 0 co 2 v PMID 14050012 Nash AD Stout AP 1958 Giant cell carcinoma of the lung report of 5 cases Cancer 11 2 369 76 doi 10 1002 1097 0142 195803 04 11 2 lt 369 aid cncr2820110222 gt 3 0 co 2 8 PMID 13511359 S2CID 40340336 Patton MM McDonald JR Moersch HJ 1951 Bronchogenic large cell carcinoma J Thorac Cardiovasc Surg 22 1 88 93 PMID 14851490 Walter JB Pryce DM June 1955 The histology of lung cancer Thorax 10 2 107 16 doi 10 1136 thx 10 2 107 PMC 1019475 PMID 14396845 Hadley GG Bullock WK December 1953 Autopsy reports of pulmonary carcinoma survey in Los Angeles County Hospital for 1951 Calif Med 79 6 431 3 PMC 1521859 PMID 13106728 Ozzello L Stout AP 1961 The epithelial origin of giant cell carcinoma of the lung confirmed by tissue culture Report of a case Cancer 14 5 1052 6 doi 10 1002 1097 0142 196109 10 14 5 lt 1052 aid cncr2820140521 gt 3 0 co 2 d PMID 13731858 S2CID 6846264 Friedberg EC February 1965 Giant Cell Carcinoma of the Lung A dedifferentiated Adenocarcinoma Cancer 18 2 259 64 doi 10 1002 1097 0142 196502 18 2 lt 259 aid cncr2820180219 gt 3 0 co 2 f PMID 14254083 S2CID 12195106 External links edit Pathology and Genetics of Tumours of the Lung Pleura Thymus and Heart World Health Organization Classification of Tumours Archived from the original on 2015 11 15 Retrieved 2010 06 02 Download Page Lung cancer page National Cancer Institute Retrieved from https en wikipedia org w index php title Giant cell carcinoma of the lung amp oldid 1179998036, wikipedia, 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