Double-hit lymphoma is an aggressive form of cancer that develops from white blood cells and carries specific genetic changes that make it more challenging to treat. This rare subtype affects a small percentage of people with certain types of lymphoma and requires specialized approaches to diagnosis and treatment.
Understanding Double-Hit Lymphoma
Double-hit lymphoma, also known as high-grade B-cell lymphoma (a term describing fast-growing, aggressive lymphoma), is a type of cancer that originates in specialized white blood cells called B lymphocytes or B cells. These cells are part of the body’s immune system and normally help fight infections. When these cells become cancerous, they can grow and spread rapidly throughout the body[1].
The name “double-hit” comes from the presence of two specific genetic problems within the cancer cells. These genetic changes involve pieces of chromosomes breaking off and combining in abnormal ways, a process called a translocation (when parts of genes switch places within chromosomes). In double-hit lymphoma, one of these changes involves a gene called MYC, and the other involves either the BCL2 gene or, less commonly, the BCL6 gene[3].
This condition is considered a distinct type of non-Hodgkin lymphoma (a category of cancers that develop in the lymphatic system). In recognition of its unique characteristics, the World Health Organization officially designated high-grade B-cell lymphoma with these specific gene rearrangements as its own category of B-cell non-Hodgkin lymphoma in 2016[3].
Epidemiology and Who Is Affected
Double-hit lymphoma is relatively rare compared to other types of lymphoma. It affects approximately 5 percent of people diagnosed with diffuse large B-cell lymphoma (DLBCL), which is one of the most common types of non-Hodgkin lymphoma[4]. Among people with Burkitt lymphoma, another type of B-cell cancer, the proportion is higher, with estimates ranging from 32 to 78 percent having the gene rearrangements that would classify them as having high-grade B-cell lymphoma[3].
The disease primarily affects older adults, though it can occur at any age. Research indicates that it is slightly more common in males than in females[4]. Because comprehensive molecular testing is needed to identify the specific gene rearrangements, the true incidence of double-hit lymphoma may only become clear when all patients undergo detailed genetic analysis of their cancer cells[5].
Causes and Genetic Basis
The development of double-hit lymphoma is rooted in specific genetic changes that occur within B cells. In healthy cells, DNA is organized into structures called chromosomes. When pieces of chromosomes break off and reconnect incorrectly, this creates translocations that can disrupt normal cell function[4].
In double-hit lymphoma, the most common pattern involves rearrangements of both the MYC gene and the BCL2 gene. These genes normally serve important functions in controlling cell behavior. The MYC gene promotes cell multiplication and growth, while BCL2 helps regulate cell death, ensuring that cells die when they should. When both genes are disrupted through translocations, the result is too much cell division combined with decreased cell death. This imbalance allows cancer cells to multiply rapidly and resist the body’s natural mechanisms for eliminating abnormal cells[4].
Less commonly, the second genetic change involves the BCL6 gene instead of BCL2. BCL6 also plays a role in controlling cell death and survival. When all three genes—MYC, BCL2, and BCL6—are involved, the cancer is called triple-hit lymphoma[4].
The MYC gene is particularly important in understanding this disease. Beyond its role in cell proliferation, differentiation, and programmed cell death, MYC also regulates other cellular processes including the production of small molecules called microRNAs and the processing of genetic information. This makes MYC a powerful driver of cancer when it becomes dysregulated[12].
Risk Factors
The specific risk factors for developing double-hit lymphoma are not well established in the available medical literature. Unlike some other cancers where clear lifestyle or environmental factors have been identified, double-hit lymphoma appears to result primarily from spontaneous genetic changes that occur in B cells. The translocations that define this disease happen at the cellular level and are not currently linked to specific behaviors or exposures that could be modified to reduce risk.
Symptoms and Clinical Presentation
Because double-hit lymphoma shares many characteristics with diffuse large B-cell lymphoma, the symptoms are often similar. Many people experience what doctors call B symptoms, a group of symptoms common to many forms of lymphoma. These include fevers that occur without an obvious cause, drenching night sweats that may require changing bedclothes, and sudden, unexplained weight loss[4].
Other common signs and symptoms include swollen lymph nodes, which may appear as painless lumps in the neck, armpits, or groin. Many people experience persistent fatigue that doesn’t improve with rest. Trouble breathing can occur if the cancer affects lymph nodes in the chest. Loss of appetite is also frequently reported[4].
These high-grade lymphomas typically don’t reveal themselves during a routine physical examination. Instead, they tend to announce their presence suddenly with the symptoms described above. The disease often progresses rapidly, and people may present with advanced-stage disease, meaning the cancer has spread to multiple areas of the body. Involvement of areas outside the lymph nodes, called extranodal involvement, is also common[9][12].
Prevention
Based on current medical understanding, there are no known prevention strategies for double-hit lymphoma. Because the disease results from specific genetic changes that occur within cells, and these changes are not linked to identifiable lifestyle factors or environmental exposures, there are no recommended screenings, vaccinations, supplements, or lifestyle modifications that have been shown to prevent its development.
Pathophysiology: How the Disease Affects the Body
Double-hit lymphoma disrupts the body’s normal processes through multiple mechanisms that stem from the genetic rearrangements at its core. Understanding how these changes affect cell behavior helps explain why this form of lymphoma is so aggressive and difficult to treat.
In normal circumstances, B cells are carefully regulated to ensure they multiply when needed and die when they become old or damaged. The MYC gene acts like an accelerator for cell growth and division. When it functions normally, it helps B cells multiply appropriately in response to infections. The BCL2 and BCL6 genes, on the other hand, help control cell death pathways, ensuring that cells die at the right time through a process called apoptosis[4].
When translocations occur involving these genes, their normal regulatory mechanisms are disrupted. The MYC gene may become overactive, driving constant cell multiplication. Simultaneously, changes in BCL2 or BCL6 prevent cells from dying when they should. This combination creates a powerful driver of cancer growth—cells that divide rapidly and refuse to die[12].
The synergistic effect of having both MYC dysregulation and BCL2 or BCL6 dysregulation is what makes double-hit lymphoma particularly aggressive. This combination not only promotes rapid tumor growth but also increases resistance to chemotherapy and other treatments. Many standard chemotherapy drugs work by triggering cancer cells to die, but when the cell death pathways controlled by BCL2 or BCL6 are disrupted, these drugs become less effective[5].
The cancer cells in double-hit lymphoma typically show high rates of division, which can be measured by looking at a marker called Ki67. In double-hit lymphoma, Ki67 levels are often very high, sometimes exceeding 90 percent, indicating that the vast majority of cancer cells are actively dividing at any given time[9].
As these rapidly dividing cancer cells accumulate, they form tumors in lymph nodes and can spread throughout the lymphatic system. The disease frequently involves the bone marrow, where blood cells are produced, and can affect other organs as well. This widespread involvement contributes to many of the symptoms people experience, from swollen lymph nodes to fatigue caused by disrupted blood cell production[9].
Recent research has begun to uncover additional layers of complexity in how these genetic changes affect cells. MYC doesn’t just control whether cells divide or die—it also influences many other cellular processes. It regulates the production of microRNAs, small molecules that help control gene expression throughout the cell. It affects how messenger RNA is processed and prepared to make proteins. All of these functions mean that when MYC becomes dysregulated through translocations, the effects cascade through multiple cellular systems[12].
Scientists have also learned that double-hit lymphoma may involve more than just the primary translocations. Additional genetic changes, including alterations in the number of copies of certain genes (called copy number alterations) and mutations in other cellular pathways, may contribute to the disease’s behavior. This suggests that while the MYC and BCL2 or BCL6 translocations define the disease, they may be part of a more complex genetic landscape that influences how aggressive the cancer is and how it responds to treatment[5].
The rapid growth and widespread involvement characteristic of double-hit lymphoma mean that people often present with advanced disease. The cancer may be classified as stage IV, meaning it has spread to multiple sites throughout the body, including bone marrow or organs outside the lymphatic system. This advanced presentation at diagnosis contributes to the challenges in treating the disease effectively[9].