Monomorphic epitheliotropic intestinal T cell lymphoma (MEITL) (formerly termed enteropathy-associated T cell lymphoma, type II) is an extremely rare
peripheral T-cell lymphoma that involves the malignant proliferation of a type of
lymphocyte, the
T cell, in the
gastrointestinal tract
The gastrointestinal tract (GI tract, digestive tract, alimentary canal) is the tract or passageway of the digestive system that leads from the mouth to the anus. The GI tract contains all the major organ (biology), organs of the digestive syste ...
(i.e. GI tract).
Over time, these T cells commonly spread throughout the
mucosa
A mucous membrane or mucosa is a membrane that lines various cavities in the body of an organism and covers the surface of internal organs. It consists of one or more layers of epithelial cells overlying a layer of loose connective tissue. It is ...
l lining of a portion of the GI tract
(particularly the jejunum and ileum of the small intestine
), lead to GI tract nodules and ulcerations, and cause symptoms such as abdominal pain, weight loss, diarrhea,
obstruction,
bleeding, and/or
perforation.
In 2008, the
World Health Organization defined a specific type of lymphoma,
enteropathy-associated T cell lymphoma (EATL), as having two different types: EATL type I, a lymphoma occurring in patients with the chronic,
autoimmune GI tract disorder,
celiac disease, and EATL type II, a similar bowel lymphoma that was not associated with celiac disease. However, subsequent studies found significant clinical, pathologic, and pathophysiological differences between these two types of lymphoma. Consequently, the World Health Organization (2016) redefined these lymphomas as separate entities, terming the celiac disease-associated lymphoma as enteropathy-associted T cell lymphoma (EATL) and the lymphoma not associated with celiac disease as monomorphic epitheliotropic intestinal T cell lymphoma (MEITL).
MEITL is only 1/5 to 1/10 as common as EATL.
The Organization (2016) also termed a third type of intestinal T cell lymphoma that could not be classified as ATL or MEITL as intestinal T cell lymphoma, not otherwise specified.
MEITL is a highly aggressive GI tract lymphoma
which typically has had very short survival times following its diagnosis.
The disease often occurs in elderly patients who are afflicted with other ailments and consequently have little tolerance for the standard
chemotherapy regimens that are used to treat other types of lymphomas. Moreover, these therapeutic regimens have shown little effectiveness in treating MEITL. To date, the best but still only marginally effective therapeutic interventions for the disease have been treatments that incorporate
hematopoietic stem cell transplantation into chemotherapy plus surgical (when needed to treat local bowel issues such as obstruction or perforation) regimens.
Presentation
MEITL has been seen more often in Asians and individuals of
Hispanic descent, in males (male to female ratio of ~2 to 1), and in mature or elderly individuals (median age ~60 years).
Patients may present with irregular bowel movements, abdominal pain,
hematochezia
Haematochezia is the passage of fresh blood through the anus path, usually in or with stools (contrast with melena). The term is from Greek αἷμα ("blood") and χέζειν ("to defaecate"). Hematochezia is commonly associated with lower gastro ...
(i.e. the anal passage of fresh blood),
B symptoms (i.e. fever,
night sweats, weight loss),
loss of appetite,
and/or bowel
perforations and/or
obstructions.
Pathophysiology
The malignant T cells in MEITL can be identified by: their expression of
cluster of differentiation (i.e. CD)
cell surface molecules
CD3,
CD8, and
CD56; by their failure to express
CD4
In molecular biology, CD4 (cluster of differentiation 4) is a glycoprotein that serves as a co-receptor for the T-cell receptor (TCR). CD4 is found on the surface of immune cells such as T helper cells, monocytes, macrophages, and dendritic ...
,
CD5, or
CD30; and, in particular, by their overexpression of
megakaryocyte-associated tyrosine kinase. They are not infected with the
Epstein-Barr virus and therefore do not express this virus's products (e.g.
EBER1 or EBER2).
In most individuals with the disease, these T cells are
γδ rather than αβ T-cells based on their expression of γδ rather than αβ
T-cell receptors
A T cell is a type of lymphocyte. T cells are one of the important white blood cells of the immune system and play a central role in the adaptive immune response. T cells can be distinguished from other lymphocytes by the presence of a T-cell r ...
. They also commonly express
cytotoxic T cell
A cytotoxic T cell (also known as TC, cytotoxic T lymphocyte, CTL, T-killer cell, cytolytic T cell, CD8+ T-cell or killer T cell) is a T lymphocyte (a type of white blood cell) that kills cancer cells, cells that are infected by intracellular pa ...
activation markers such as
TIA1
TIA1 or Tia1 cytotoxic granule-associated rna binding protein is a 3'UTR mRNA binding protein that can bind the 5'TOP sequence of 5'TOP mRNAs. It is associated with programmed cell death ( apoptosis) and regulates alternative splicing of the ge ...
,
granzyme B, and
perforin and therefore may have derived from or be related to
cytotoxic T cell
A cytotoxic T cell (also known as TC, cytotoxic T lymphocyte, CTL, T-killer cell, cytolytic T cell, CD8+ T-cell or killer T cell) is a T lymphocyte (a type of white blood cell) that kills cancer cells, cells that are infected by intracellular pa ...
lymphocytes. However, in up to 25% of cases the malignant cells in MEITL also express markers of
B cell
B cells, also known as B lymphocytes, are a type of white blood cell of the lymphocyte subtype. They function in the humoral immunity component of the adaptive immune system. B cells produce antibody molecules which may be either secreted or ...
lymphocytes. Detection of these "
tumor marker" molecules on or in the lymphocytes of diseased tissues is critical for diagnosing MEITL; however, it does not clearly establish the original type of lymphocytes which became MEITL's malignant cells. This issue requires further studies.
MEITL is thought to arise from
intraepithelial lymphocytes that normally reside in the
epithelial lining of the GI tract and over time acquire abnormalities that promote their survival, proliferation, avoidance of the
immune system, and thereby malignancy. These cells are not infected with the Epstein-Barr virus and therefore have not become malignant as a consequence of this
virus's malignancy-producing effects on lymphocytes as it does in other types of GI tract lymphomas. Rather, the malignant T cells in MEITL bear various genetic abnormalities that may promote their malignancy.
Restriction fragment length polymorphism studies indicate that these cells have abnormal gains in
minisatellites, i.e. repetitive small DNA sequences, in
chromosomes 1, 5, 7, 8, 9, 13, 16, and 18. These minisatellites disrupt the production of some genes but the potential relevancies of these disruptions have not been defined.
Genetic abnormalities commonly found in MEITL that do have potentially pro-malignant effects include:
* Losses on the short (i.e. "p") arm around position 21.3 on one of the two inherited chromosomes 9. This results in a
loss of heterozygosity for two genes, the ''
CDKN2A'' gene which encodes cyclin-dependent kinase Inhibitor 2A, a protein that regulates cell proliferation and the ''
CDKN2B
Cyclin-dependent kinase 4 inhibitor B also known as multiple tumor suppressor 2 (MTS-2) or p15INK4b is a protein that is encoded by the ''CDKN2B'' gene in humans.
Function
This gene lies adjacent to the tumor suppressor gene CDKN2A in a region ...
'' gene which encodes multiple tumor suppressor 2, a protein that regulates cell death and tumor formation.
* A similar loss of heterzygosity on the p arm of chromosome 17 at positions 12 through 13.2. This results in the loss of one of the inherited ''
TP53'' genes. ''TP53'' encodes tumor suppressor p53, a protein that regulates cell proliferation, death, and tumor formation.
* Mutations in
JAK-STAT signaling pathway genes (i.e. ''
JAK3
Tyrosine-protein kinase JAK3 is a tyrosine kinase enzyme that in humans is encoded by the ''JAK3'' gene.
Janus kinases
Janus kinase 3 is a tyrosine kinase that belongs to the janus family of kinases. Other members of the Janus family include ...
'' and ''
STAT5B
Signal transducer and activator of transcription 5B is a protein that in humans is encoded by the ''STAT5B'' gene. ''STAT5B'' orthologs have been identified in most placentals for which complete genome data are available.
Function
The protein e ...
''). This pathway regulates cell proliferation, death, and tumor formation.
* Mutations in
MAPK/ERK pathway
The MAPK/ERK pathway (also known as the Ras-Raf-MEK-ERK pathway) is a chain of proteins in the cell that communicates a signal from a receptor on the surface of the cell to the DNA in the nucleus of the cell.
The signal starts when a signaling ...
genes (i.e. ''
BRAF'' and ''
KRAS''). This pathway regulates cellular proliferation.
* Mutations in the ''
GNA12'' gene. This gene encodes Gα12, a
G alpha subunit
G alpha subunits are one of the three types of subunit of guanine nucleotide binding proteins, which are membrane-associated, heterotrimeric G proteins.
Background
G proteins and their receptors (GPCRs) form one of the most prevalent signalling ...
that is required for stimuli to regulate cell function through Gα12-coupled
receptors.
* Mutations in the
chromatin remodeling
Chromatin remodeling is the dynamic modification of chromatin architecture to allow access of condensed genomic DNA to the regulatory transcription machinery proteins, and thereby control gene expression. Such remodeling is principally carried out ...
gene, ''
SETD2''. This gene encodes SET domain containing 2, a protein that acts to reduce the occurrence of
gene deletions and tumor formation.
* Mutations in the ''CREBBP'' gene. This gene encodes
CREB-binding protein
Cyclic adenosine monophosphate Response Element Binding protein Binding Protein (CREB-binding protein), also known as CREBBP or CBP or KAT3A, is a coactivator encoded by the ''CREBBP'' gene in humans, located on chromosome 16p13.3. CBP has intrin ...
, a protein that activates various
transcription factors some of which are implicated in tumor development.
* Increased expression of the ''
Myc''
proto-oncogene. When over-expressed, this genes product, the
transcription factor, MYC, stimulates other genes to make their products, some of which stimulate cell proliferation.
Further studies are required to determine which, if any, of these genetic abnormalities play a role in the development and/or progression of MEITL and therefore are therapeutic targets for treating the disease.
Diagnosis
The symptoms of MEITL are generally non-specific. The diagnosis depends on
endoscopic findings in the GI tract, histological findings on biopsied specimens from involved areas of the GI tract, evidence of disease involvement outside of the GI tract, and the differentiation of MEITL from other GI tract lymphomas and benign lymphoproliferative diseases. Endoscopy typically shows multiple raised and/or ulcerated lesions involving the
jejunum or
ileum, and less commonly, the
duodenum
The duodenum is the first section of the small intestine in most higher vertebrates, including mammals, reptiles, and birds. In fish, the divisions of the small intestine are not as clear, and the terms anterior intestine or proximal intestine m ...
,
stomach, or
colon.
These lesions may occur at multiple sites or spread throughout large areas of the GI tract. Biopsied tissues show abnormally broad
intestinal villi caused by the infiltration of sheets of uniformly-sized lymphocytes. These lymphocytes may also infiltrate and disrupt the architecture of nearby
intestinal crypt
In histology, an intestinal gland (also crypt of Johann Nathanael Lieberkühn, Lieberkühn and intestinal crypt) is a gland found in between villi in the intestinal epithelium lining of the small intestine and large intestine (or colon). The gland ...
s and the
epithelial lining
Epithelium or epithelial tissue is one of the four basic types of animal Tissue (biology), tissue, along with connective tissue, muscle tissue and nervous tissue. It is a thin, continuous, protective layer of compactly packed Cell (biology), ...
. Unlike celiac disease-associated EATL, the lesions usually have little evidence of inflammatory cells (particularly lymphoplasmacytoid cells, i.e. cells showing a mixture of
B cell
B cells, also known as B lymphocytes, are a type of white blood cell of the lymphocyte subtype. They function in the humoral immunity component of the adaptive immune system. B cells produce antibody molecules which may be either secreted or ...
and
plasma cell
Plasma cells, also called plasma B cells or effector B cells, are white blood cells that originate in the lymphoid organs as B lymphocytes and secrete large quantities of proteins called antibodies in response to being presented specific substan ...
morphological features) or of infiltration of the epithelium lining by the types of lymphocytes seen in celiac disease.
The lymphocytes in these lesions are T cells expressing the marker molecules and genetic abnormalities given in the above Pathophysiology section.
CT scan
A computed tomography scan (CT scan; formerly called computed axial tomography scan or CAT scan) is a medical imaging technique used to obtain detailed internal images of the body. The personnel that perform CT scans are called radiographers ...
s commonly reveal involvement of
mesenteric lymph nodes.
Advanced cases have involvement of the
bone marrow
Bone marrow is a semi-solid tissue found within the spongy (also known as cancellous) portions of bones. In birds and mammals, bone marrow is the primary site of new blood cell production (or haematopoiesis). It is composed of hematopoietic ce ...
and/or dissemination into other organs.
Differential diagnosis
MEITL must be
differentiated from the following GI tract disorders with which it shares some common features.
*
Enteropathy-associated T cell lymphoma (EATL): By definition, MEITL differs from EATL in that EATL specifically occurs in patients with celiac disease. In cases where the presence of celiac disease is not obvious, EATL is differentiated from MEITL by: its occurrence primarily in individuals of Northern European descent, the presence of inflammatory plasmacytoid cells in its lesions,
by the tendency of its lesions to consist of γδ rather than αβ T-cell receptor-expressing lymphocytes, by its T cells that express CD30 but not CD56 or megakaryocyte-associated tyrosine kinase.
and by most (95%) individuals with EATL being of either the
HLA-DQ2 or
HLA-DQ8 rather than other HLA-DQ
haplotype
A haplotype ( haploid genotype) is a group of alleles in an organism that are inherited together from a single parent.
Many organisms contain genetic material ( DNA) which is inherited from two parents. Normally these organisms have their DNA or ...
s.
*
Extranodal NK/T cell lymphoma, nasal type (ENKTCL-NT): ENKTCL-NT is a lymphoma that usually involves nasal and
oropharyngeal airways but may involve lower areas of the GI tract with lesions that mimic MEITL. Unlike MEITL, it is more commonly due to the proliferation of
NK rather than T cell lymphocytes, in all cases is caused by lymphocytes that are infected with the
Epstein-Barr virus and therefore express this virus's products,
and in almost all cases is caused by lymphocytes that do not express
CD3 and have not rearranged their T cell receptors.
*
Anaplastic large cell lymphoma, ALK positive (ALCL,ALK+): ALCL,ALK+ is a subtype of
anaplastic large cell lymphoma. It commonly involves the malignant proliferation of T cells in tissues outside of the GI tract but in some cases the disease involves primarily the GI tract.
Unlike MEITL, ALCL,ALK+ occurs most commonly in young individuals and individuals from Western Countries and most often involves tissue infiltrates of large,
anaplastic-appearing T cells which express a
fusion gene involving the ALK gene (which encodes
Anaplastic lymphoma kinase),
but do not express CD3, CD8, or CD56.
*
Peripheral T-cell lymphoma not otherwise specified (PTCL-NOS): PTCL-NOS is a heterogenous group of T cell lymphomas that involves lymph nodes, bone marrow, liver, spleen, and/or GI tract. Rarely this lymphoma may present in the GI tract without overt evidence of involvement of other tissues. Unlike MEITL, the T cells in this disease exhibit genetic abnormalities in ''
TET2,
IDH2,
DNMT3A,
RHOA,
CD28
CD28 (Cluster of Differentiation 28) is one of the proteins expressed on T cells that provide co-stimulatory signals required for T cell activation and survival. T cell stimulation through CD28 in addition to the T-cell receptor ( TCR) can provid ...
'', and ''
VAV1'' genes
but in general do not have the genetic abnormalities or express the molecular markers found in MEITL.
*
Natural killer cell enteropathy
Natural killer cell enteropathy, also termed NK cell enteropathy (NKCE), and a closely related disorder, lymphomatoid gastropathy (LG), are non-malignant diseases in which one type of lymphocyte, the natural killer cell (i.e. NK cell), proliferat ...
(NKCE): NKCE is a benign disease of the GI tract which has GI tract lesions and symptoms that mimic MEITL. Unlike MEITL, NKCE involves the proliferation of non-clonal NK cell lymphocytes which exhibit activation markers (e.g.
granzyme B,
perforin, and
T-cell intracellular antigen-1) but no genetic abnormalities.
*
Indolent T cell lymphoproliferative disorder of the gastrointestinal tract (ITCLD-GT): ITCLD-GT is a generally benign disease of the GI tract that has in some cases progressed to an aggressive lymphoma. It presents with clinical signs and GI tract lesions which may mimic MEITL.
These lesions involve infiltrations of
T-cells that unlike the T cells in MEITL proliferate slowly, are homogenously small-sized, CD56-negative, may express
CD4
In molecular biology, CD4 (cluster of differentiation 4) is a glycoprotein that serves as a co-receptor for the T-cell receptor (TCR). CD4 is found on the surface of immune cells such as T helper cells, monocytes, macrophages, and dendritic ...
,
and usually do not express CD8.
Treatment
There is no standard treatment for MEITL. Most individuals have been treated by surgical resections of involved areas with or without
anthracycline-based
chemotherapy. In these cases, responses have been short-lived and/or poor with 1 year overal survival rates, 1 year progression free survival rates, and median survival times of 36%, 21%, and 7 months, respectively.
A retrospective study of patients treated with resection, chemotherapy and
autologous hematopoietic stem cell transplantation had a higher 1-year and 5-year overall survival (100%, 33%) compared to one-year survival (73%) and five-year survival (14%) without transplantation; a second retrospective study supported the usefulness of transplantation in that high-dose lymphoma chemotherapy followed by transplantation and standard-dose lymphoma chemotherapy with or without surgical resection increased 5-year overall survival from 22 to 60% and 5-year disease progression-free survival from 22 to 52%.
While further studies, particularly
randomized controlled trials, are needed to investigate the best treatments for MEITL, the use of lymphoma chemotherapy, hematopoietic stem cell transplantation, and, where needed, surgical resections are the currently recommended treatments for MEITL.
References
{{Reflist
Lymphocytes
T cells
Lymphocytic disorders
Gastrointestinal tract disorders
Lymphoma
Non-Hodgkin lymphoma