In 1882, the French physician Ernest Gaucher identified ‘his’ disease in his thesis as a typical enlargement of the spleen, easily seen as an epithelioma but not as leukaemia or any other kind of cancer. Nowadays, we know it comes with an increased risk of haematological malignancies like multiple myeloma and hepatocellular carcinoma. If left untreated, at least.
Lately, there has been a new kid in the world of Gaucher Disease (GD): Gaucheroma. What is it? In this post, I will try to get myself an answer.
Lesions
A century after Ernest Gaucher’s thesis, in 1982, the esteemed and beloved pathologist Robert E. Lee published a roundup of 275 cases of GD, 100 of which had had their spleens removed.
He described:
“In addition to the fibrosis associated with small or large infarcts there are nodular lesions that are related to vascular malformations of the red pulp. These may measure up to 10.0 cm in diameter and they are dark purple nodules that bulge when sectioned. The parenchyma in these nodules is composed of numerous round spaces that contain Gaucher cells as well as blood cells and fibrous areas usually develop as the vascular areas become organized. … Any of these previously described nodules may be incorrectly considered to be neoplastic when in reality they are the result of distortion of splenic architecture by Gaucher cells.”
Lee continued that liver involvement in GD type 3 is a form of fibrosis that converts the parenchyma into small nodules. In the fibrous areas, there are numerous Gaucher cells. Others have described these cases as cirrhosis. In his view, adenopathy is not a feature of clinical illness. Lee closes his article with
“As we enter the second century of our knowledge of this disease we should keep Dr. Gaucher’s talent of making clinicopathological observations in mind as we search for clues to the better understanding of the various clinical forms of the disease.”
Other publications mentioned these nodular lesions in spleens and livers, which are increasingly seen with imaging techniques like ultrasound and MRI.
In 2009, Poll and Von Dahl found an extensive accumulation of Gaucher cells within liver sinusoids and labelled it hepatic Gaucheroma (Gaucher-cell pseudotumor).
Masses and lymphadenopathy
In 2002, Lim et al. reported the case of a child with GD type 3 on ERT with a 5 cm mesenteric mass. A surgical biopsy revealed that it was a collection of lymph nodes infiltrated with Gaucher’s cells at the base of the mesentery, also confirmed histologically to be Gaucher’s cell infiltrates.
Fowler et al. presented two children with persistent abdominal lymphadenopathy in 2006 while receiving ERT. Needle core biopsies contained macrophages that did not form granulomas or classic Gaucher cells on light microscopy. This was assumed to be incomplete clearance, incomplete/partial enzyme replacement, or possibly an unusual response to a relatively small amount of storage material.
Another child with GD (type 3) was reported the following year by Burrow et al. as having developed progressive mesenteric and mediastinal lymphadenopathy. They interpreted it as poorly accessible, differentially responsive compartments in patients with Gaucher disease who receive enzyme therapy.
Yağci et al. followed in 2009 with a 5-year-old with GD type 3 on ERT. She was initially presented with an ill-defined abdominal mass of 10 cm, palpable in the umbilical area. Ultrasound revealed multiple conglomerating mesenteric lymphadenopathies, some of which contained necrotic regions. Histopathological examination revealed diffuse infiltration of Gaucher cells.
Abdelwahab and SeifEldien reported eight cases in 2015, some developing lymphadenopathy associated with type 1 GD. Their cohort developed mesenteric and mediastinal lymphadenopathy while on therapy for an average duration of 3 years.
In 2019, Tseng et al. reported a 3.5 × 2.3 cm hypointense under T1 lobulated mass at S5 and S6 in the liver from a regular abdominal MRI exam of a 3-year-old. Clustered enlarged lymph nodes at the mesenteric and inguinal regions were also discovered during the regular checkup.
In 2022, Tantawy et al. recently studied fifty children on ERT, of whom 26 (60 GD1, 20 GD3) were confirmed to have abdominal lymphadenopathy (ALN). Their size was significantly correlated with the disease severity (SSI) and LysoGB1. Histology was not determined. ALN was found in 80% of splenectomized children. They postulate that ALN can be considered a marker of GD severity and regard it as a potential sequel of a high disease burden.
So, what is it?
To my understanding, nodular lesions in the spleen and liver are clusters of Gaucher cells, occasionally affecting the surrounding tissues. I wonder if the clusters are formed at sites that normally represent lymph nodes inside an organ. These “pseudotumor” disturbances are thought to increase the occurrence of local neoplasia, but I have not seen statistics of patients on treatment until now.
Gaucheromas outside the spleen and liver are only seen in patients on Gaucher treatment, which, so far, is ERT. In general, these soft-tissue masses are regarded as lymphadenopathies.
Overlooking gaucheromas inside and outside organs, I believe they should only be named as such when Gaucher cells are seen in them. Preferably, we forget the term gaucheroma and only use the terms Gaucher cell clusters or masses, as Ramaswami et al. suggest.
The lesions and masses in Gaucher patients can be considered common and understandable, implying no reason for biopsy. Suspicion of neoplasia, of course, changes that. Also, as masses, they can cause other serious complications, including protein-losing enteropathy.
Their clinical relevance lies in their substrate storage; only systemic intervention may influence that. (Additional) As Yano et al. suggest, SRT or a chaperone might also be an option.
I also wonder if these Gaucher cells can be released from the sites by somehow affecting their bonding to others or the structure. Kim et al. seem to support this view.
References
Disclaimer
I am not a clinician nor otherwise medically educated. If you relate this post to your own health, please talk with your clinician about that.
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