Doctors try to avoid GvHD by genetically “matching” donors to recipients, often by recruiting a sibling or other family member with a similar genetic makeup. If GvHD symptoms develop, doctors can prescribe steroidal and nonsteroidal immune-suppressants that can temper and eventually control the autoimmune-like assault.
Types of Graft-Versus-Host Disease
Bone marrow or stem cell transplants are sometimes used in people with leukemia and lymphoma as well as certain solid tumor cancers and blood-related disorders. GvHD is a complication associated with allogeneic transplants (in which cells are donated) rather than autologous transplants (in which the donor and recipient are the same).
There are two main types of GvHD, differentiated by the timing of their occurrence and distinctive clinical features:
Acute GvHD, also known as classic acute GvHD, occurs within 100 days of a transplant and mainly affects the skin, gastrointestinal tract, and liver in 70%, 74%, and 44% of cases, respectively. Chronic GvHD, also known as classic chronic GvHD, occurs 100 days or more after a transplant and tends to affect the skin, liver, mouth, gastrointestinal tract, lungs, eyes, nervous system, or genitourinary tract.
GvHD doesn’t always present in a consistent manner. It can sometimes manifest with features of acute and chronic GvHD, which doctors refer to as “overlap syndrome.” If acute symptoms develop after 100 days, the condition is often referred to as persistent, recurrent, late-onset acute GVHD.
Graft-Versus-Host Disease Symptoms
The symptoms of GvHD can differ from person to person but tend to involve specific organ systems and disease patterns. Acute GvHD typically manifests with the rapid onset of cutaneous (skin) symptoms, followed by those affecting and gastrointestinal (GI) tract and liver.
With chronic GvHD, the affected organ systems tend to be more diverse. Even so, the symptoms tend to originate in the skin before moving on to the gut, liver, lungs, eyes, and other organs. Chronic GvHD is also characterized by the tightening and hardening of the skin and connective tissues, similar in appearance to systemic sclerosis (scleroderma).
For instance, people who develop eye problems with chronic GvHD will almost invariable have a poorer prognosis than those who don’t. Similarly, people who develop oral lichen planus, an inflammatory condition frequently seen in people with chronic GvHD, are at an increased risk of aggressive oral cancers and early death.
Causes
The causes of graft-versus-host disease are complex but, at its heart, GvHD is characterized by a mismatch between certain genes in the transplant donor and transplant recipient.
These genes, referred to as major histocompatibility complex (MHC), are responsible for encoding surface proteins on cells known as human leukocyte antigen (HLA). HLA, in turn, helps the body differentiate between cells that are “normal” and those that are “foreign.”
Any cell considered foreign will trigger an immune response, releasing an army of white blood cells, called T-cells, that target and neutralize the perceived invader.
With allogeneic transplants, donor cells will sometimes fail to recognize the recipient’s tissues as normal due to minute variations in the HLA structure. If this occurs, the donor cells can turn the body’s defenses on itself, leading to the onset of GvHD.
If no matches are available, the doctors match unrelated donors to recipients based on HLA blood test results. But even with a genetic match, the risk of GvHD remains high.
Research suggests that between 40% and 50% of people receiving a transplant from an HLA-matched sibling will develop acute GvHD, while 30% to 70% will develop chronic GvHD. The rate is even higher when an unrelated HLA-matched donor is involved.
Beyond HLA typing, there are other factors that can increase the risk of acute or chronic GvHD.
The type of transplant may also play a role in often surprising and contradictory ways.
According to a 2012 study in the New England Journal of Medicine, undergoing a bone marrow transplant reduces the risk of chronic GvHD compared to a peripheral-blood stem cell transplant (PBSCT). On the flip side, PBSCT is less likely to result in graft failure (in which a transplant fails to implant) compared to a bone marrow transplant.
Diagnosis
It may seem reasonable to diagnose GvHD based on symptoms alone in an allogeneic transplant recipient. But there are actually strict criteria by which a diagnosis is made, in part to ensure that the symptoms are, in fact, GvHD and not some other condition.
According to guidelines issued by the National Institutes of Health (NIH), the diagnosis typically requires at least one clinical sign of GvHD paired with a biopsy or other test to confirm the characteristic features of the disease.
Examples of confirmatory tests include:
Organ-specific tests, such as pulmonary function tests (used to detect respiratory problems), bilirubin tests (used to detect liver dysfunction), and Schirmer tests (used to determine if a tear duct is producing tears) Imaging tests, such as computed tomography (CT) scan with barium contrast to detect abnormalities in the gastrointestinal tract Tissue biopsy, in which samples of skin, liver, gastrointestinal tract, mouth, lung, or genitals are taken to detect structural changes to tissues (such as sclerosis) under the microscope
The doctor would also take into account the timing of the symptoms and perform a differential diagnosis to exclude all other possible causes for the symptoms.
The NIH also allows for leeway in the diagnosis of chronic GvHD based on whether the symptoms are “diagnostic” or “distinctive.” Diagnostic symptoms are those regarded as defining features and do not require any form of confirmatory testing. Distinctive symptoms are those that are only suggestive of chronic GvHD and, therefore, must be supported by confirmatory testing.
Acute GvHD
There are several classifications systems used to grade acute GvHD, but among the most popular is the International Bone Marrow Transplant Registry (IBMTR) grading system.
The IBMTR system grades the severity of acute GvHD based on the degree of involvement of the skin, liver, and gastrointestinal tract. The system is graded from A through D, with A being the mildest form and D being the most severe.
The grading system of chronic GvHD is slightly different. The system used by the NIH assigns a score ranging from 0 (for no symptoms) to 3 (for severe symptoms) for each of nine different organ systems: the skin, mouth, liver, upper GI tract, lower GI tract, esophagus, lungs, eyes, and joints.
These scores are then used individually, rather than cumulatively, to grade chronic GvHD as either mild, moderate, or severe. Mild GvHD is often referred to as low-grade disease, while moderate to severe GvHD are considered moderate- and high-grade disease, respectively.
Clostridioides difficile colitis Drug skin eruptions Erythema multiforme Ischemic colitis Mixed connective-tissue disease Scleroderma Sjogren syndrome Varicella-zoster virus (shingles) Viral gastroenteritis Viral hepatitis
Treatment
GvHD is characterized by an inappropriate response of the immune system. As such, both acute GvHD and chronic GvHD are managed by reining in the immune system with immunosuppressant drugs. There are several types used in the treatment of GvHD.
Corticosteroids
Corticosteroid drugs (a.k.a. steroids) are the cornerstone of treatment for both acute and chronic GvHD. Corticosteroids temper the immune system by mimicking a hormone called cortisol that helps regulate the immune response (including the activation of T-cells).
Mild cutaneous GvHD may only require a topical steroid to control skin symptoms. Options range from low-potency 1% hydrocortisone cream to high-potency 0.05% clobetasol propionate ointment. PUVA phototherapy and Protopic (topical tacrolimus) may be added to the treatment plan for moderate to severe cases.
Severe symptoms in people with GvHD are typically treated with intravenous corticosteroids like prednisone and methylprednisone.
To avoid this, the steroid dose is gradually tapered over the course of months once the condition has been brought under control. Some people may require no further treatment. Others may require long-term topical, oral, or IV steroids to manage their condition, either alone or in combination with other therapies.
Other Immunosuppressants
In addition to steroids, there is an increasing number of nonsteroidal immune suppressants used to control GvHD, especially when the long-term harms of corticosteroid use outweigh the benefits. These include:
Jakafi (ruxolitinib): FDA approved in 2019, Jakafi can be beneficial in patients who have not responded as well to steroids. CellCept (mycophenolate mofetil): An immunosuppressant used to prevent heart, liver, or kidney transplant rejection Enbrel (etanercept): A drug commonly used to treat autoimmune diseases Methotrexate: A commonly prescribed immunosuppressant drug used to treat certain cancers and autoimmune diseases Nipent (pentostatin): An anticancer drug that can be used to treat severe, treatment-resistance GvHD Ontak (denileukin diftitox): Another anticancer drug that is sometimes used when corticosteroid drug resistance develops Prograf (tacrolimus): An oral immunosuppressant related to Protopic Rapamune (sirolimus): An immunosuppressant commonly used to prevent kidney transplant rejection Remicade (infliximab): A popular immunosuppressant used to treat autoimmune disorders Thalomid (thalidomide): An anticancer drug that has immunomodulating effects Thymoglobulin (anti-thymocyte globulin): A T-cell reducing agent Zenapax (daclizumab): An immunosuppressive monoclonal antibody
Maintaining the balance between GVT and GvHD can be tricky but, with consistent care from a skilled oncologist, the right therapy can be found and fine-tuned to achieve control.
Prognosis
Between 40% and 60% of people with acute GvHD will respond to corticosteroid therapy within four weeks. Failure to respond by an improvement of at least one grade is associated with a poor prognosis, translating to a six-month mortality rate of 45% to 65%. Those who fail to respond with grade 4 GvHD have closer to a 95% likelihood of death within six months.
Although people who respond to corticosteroids have far better outlooks, the overall five-year survival rate hovers around 50% (meaning that half of all people with GvHD will live for at least five years). Of those who do respond to corticosteroid therapy, anywhere from 20% to 25% will relapse.
Having acute GvHD is the predominant risk factor for the development of chronic GvHD and almost invariably leads to worse outcomes when it does.
Coping
There is no way to predict who will get GvHD, how well they will respond to treatment if they do, or whether or not they will relapse. The uncertainty can cause a great deal of stress, adding to the challenges that a transplant recipient already faces.
To better cope, you need to address symptoms of fatigue and weight loss that can complicate recovery as well as dealing with common skin and respiratory problems. Among the self-help tips:
Exercise
Gentle exercise can improve joint flexibility and range of motion, increase lean muscle mass, and help overcome persistent fatigue. Incorporating gentle aerobics in your exercise plans, such a brisk walk, can improve respiratory function while stimulating the release of the “feel-good” hormones called endorphins.
Skin Care
Regular moisturizing is key to improving the tightness and dryness of the skin. Use an emollient-rich moisturizer without perfumes or fragrance, applied immediately after showering and throughout the day as needed.
Wear loose breathable fabrics like cotton to avoid heat build-up, which can trigger skin inflammation, and always wear sunscreen with a minimum SPF 15 when outdoors.
Diet
GvHD occurring in the gastrointestinal tract can cause significant diarrhea and weight loss. It often helps to embark on a BRAT diet (an acronym for bananas, rice, apple, and toast) to deal with acute diarrhea.
Follow with a low-fiber, high-energy diet (defined as 1.2 to 1.5 grams of protein per kilogram of body weight per day) to prevent symptom recurrence and reverse weight loss. It often helps to work with a dietitian to ensure you get the calories and nutrition needed to maintain optimal health.
Sex
GvHD can sometimes affect the genitals and libido of both women and men. Estrogen cream (used two to three times weekly) may be prescribed to help soften vaginal tissues, while vaginal dilators can be used on a regular basis to avoid or reduce vaginal stenosis.
Testosterone replacement therapy can often help improve libido in men. Medical treatment under the care of a urologist or reconstructive surgeon may be needed to treat severe urethral stricture or vaginal stenosis.
Stress Management
Stress can impact any illness, but, with chronic GvHD, it can compound breathing problems by increasing the respiratory rate in lungs that may already be compromised.
To compensate, a physical therapist can teach you breathing exercises (like diaphragmic breathing and pursed-lip breathing) that not only increase the respiratory volume but help reduce stress by slowing the respiratory and heart rate.
Other stress management techniques include meditation, progressive muscle relaxation (PMR), and guided imagery.
A Word From Verywell
As distressing as it may be to diagnosed with graft-versus-host disease, it is important to remember that GvHD is more common than people think and can even occur when a donor is the “perfect match.” If symptoms develop, they can often be effectively controlled medications. While some people require lifelong treatment, a great many don’t.
To better cope with treatment, remain linked to medical care and maintain a healthy lifestyle, including a proper diet, routine exercise, and the avoidance of infections. These may not only reduce the severity of GvHD symptoms but improve your overall quality of life.
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