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= X-linked lymphoproliferative disease = X-linked lymphoproliferative disease (also known as Duncan disease: 86  or Purtilo syndrome, and abbreviated as XLP (Panchal et al. 2018)) is a lymphoproliferative disorder, usually caused by SH2DIA gene mutations in males. XLP-positive individuals experience immune system deficiencies that render them unable to effectively respond to the Epstein-Barr virus (EBV) [4], a common virus in humans that typically induces mild symptoms or infectious mononucleosis (IM) in patients (cdc.gov). There are two currently known variations of the disorder, known as XLP1 (XLP Type 1) and XLP2. Thanks to therapies such as chemotherapy and stem cell transplants, the survival rate of XLP1 has increased dramatically since its discovery in the 1970s (Panchal et al. 2018, Sumegi et al. 2002).

Presentation[edit]
In boys with X-linked lymphoproliferative disorder, the inability to mount an immune response to EBV, which often leads to death from bone marrow failure, irreversible hepatitis, and malignant lymphoma. may lead to death via hemophagocytic lymphohistiocytosis (HLH). Patients may also develop dysgammaglobulinemia and malignant non-Hodgkin lymphoma, even without exposure to EBV. Other observed symptoms of XLP include aplastic anemia, vasculitis, chronic gastritis, and skin lesions, as well as IM (Panchal et al. 2018, Pende et al. 2019).

Nearly half of XLP patients express humoral immune anomalies, which can include diminished responses to vaccines and low levels of immunoglobulin G (IgG).

However, the connection between EBV and X-linked lymphoproliferative disorder is yet to be determined.

Patients also produce insufficient numbers of CD27 memory B cells.

XLP1[edit]
XLP1 is caused by mutations in the SH2D1A gene, which is located at position Xq25 on the X-chromosome (Pende et al. 2019). This gene codes for an SH2 domain on a signal transducing protein called signaling lymphocyte activation molecule (SLAM)-associated protein, or SAP (Pende et al. 2019). A variety of mutations have been implicated in XLP1 expression, including deletions, single nucleotide changes, and incorrect splicing, although a correlation between the type of mutation and the severity of the disorder has not been established (Pende et al. 2019).

These defects in SAP fundamentally change the function of two SLAM receptors, 2B4 (CD244) and NTB-A (SLAMF6). Typically, after the receptors bind to their associated ligands, the immunoreceptor tyrosine-based switch motifs (ITSMs) in their cytoplasms are phosphorylated, which activates cell-activating signaling pathways. In an XLP patient, the defects in SAP cause these receptors to induce an inhibitory, rather than activating effect. Ligand binding thus fails to activate Natural Killer (NK) and Cytotoxic T cells that typically eliminate EBV infection, leading to cytokine overproduction and tissue damage (Pende et al. 2019).

The term "SH2" domain stands for src-homology 2 domain, which is a three-dimensional domain structure of about 100 amino acid residues. These domains are present in many signaling proteins because they permit specific, non-covalent bonding to proteins that contain phosphotyrosines. The amino acid residues adjacent to the phosphotyrosine on the target protein are what determine the unique binding specificity.

XLP2[edit]
A second form is associated with XIAP. Any instance of XLP caused by a mutation not in SHD21A is categorized as XLP2. XLP2 patients express different features from those typically found in XLP1 patients, such as splenomegaly and colitis (Panchal et al. 2018). This variation is closely associated with HLH,  (Panchal et al. 2018), so much so that some sources classify this condition as "X-linked familial hemophagocytic lymphohistiocytosis" instead of X-linked lymphoproliferative disease.

Treatment
Chemotherapy and hematopoietic stem-cell transplantation (HSCT) therapies have shown great success in treating XLP. The development of the two therapies, alongside more efficient monitoring techniques and supportive care, has reduced the overall mortality of the disease from 75% to 29% (Panchal et al. 2018). Care differs depending on the phenotype of XLP expressed, with treatments varying between those experiencing HLH or lymphoma, and whether or not they have been infected with EBV.

Still, a bone marrow transplant that includes CD34+ hematopoietic stem cells is the only known treatment for the disorder as a whole. Patients who cannot find a bone marrow donor have a survival rate of less than 20%. In addition to the typical restrictions imposed on donor-recipient matches, XLP1 patients who have been infected with EBV typically receive transplants from EBV-positive donors (Panchal et al. 2018).

Eponym[edit]
XLP is also known as Duncan Disease, after 6 of 18 males in the Duncan family died of lymphoproliferative disease, including fulminant infectious mononucleosis and lymphoma. It is also called "Purtilo's Syndrome", after Dr. David Theodore Purtilo (1939–1992), a pioneering Pathologist and Immunologist at the American Army Center for Pathology in Washington, who discovered it in the early 1970s. A native of Duluth, Minnesota, he pioneered the research for this condition after discovering it in one of his patients. In the late 1980s, he resided in Omaha, Nebraska and died on September 28, 1992, in Florida, after suffering a stroke before he could deliver a speech to a forum.