Langerhans' Cell Histiocytosis

Last updated by Peer reviewed by Dr Krishna Vakharia
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Langerhans' cell histiocytosis (LCH) is one of the 'histiocytosis disorders', as defined by the Histiocyte Society. Langerhans' cell histiocytosis is caused by clonal expansion of myeloid precursors that differentiate into CD1a+/CD207+ cells in lesions that leads to a spectrum of organ involvement and dysfunction. The pathogenic cells are defined by constitutive activation of the MAPK signalling pathway.[2]

Although once considered a disorder of immune regulation, it is now described as a dendritic cell neoplasm with a strong inflammatory component.[3]

It was formerly considered as a disease of childhood but is now recognised as often presenting in adulthood.

The clinical manifestations of LCH are very variable, ranging from self-resolving single-organ disease to a disseminated, aggressive disease with a 10-20% mortality.[4] LCH may affect one or many organs. If only one organ or system is involved, this is referred to as single-system LCH (SS-LCH) and has the best prognosis. If two or more organs or systems are involved, this is referred to as multisystem LCH (MS-LCH). MS-LCH is then stratified into low risk, high risk and very high risk, depending on whether any 'risk organs' are affected at diagnosis (haematopoietic system, liver and/or spleen) and by initial response to standard treatment regimes.

  • LCH is a rare disease that is more commonly seen in children but is increasingly recognised in adults.
  • It affects 4-8 children per million each year:
    • Two thirds of children will have SS-LCH.
    • Children <2 years of age with MS-LCH, commonly have involvement of 'risk organs' and the highest mortality.
  • It affects 1-2 adults per million each year:
    • In adults the mean age at diagnosis is 35 years, with 10% >55 years of age.
    • 69% have MS-LCH, 62% affecting the lung and 51% the skin.
    • 31% have SS-LCH, 51% involving the lung (most of whom are smokers), 38% bone and 14% skin.
  • Progress in the development of treatments for LCH has been hampered by its rarity but also by the question of whether it is a reactive or a neoplastic disorder.
  • Current understanding suggests that LCH arises from a genetic mutation (BRAF V600E) occurring in a myeloid progenitor cell. It is thought that the developmental stage at which the mutation occurs determines the clinical manifestation of the LCH, although this concept is not proven.
  • The mortality and permanent organ damage sometimes seen in LCH are most probably due to the harmful effects of an uncontrolled inflammatory response rather than unchecked proliferation of clonal Langerhans' cells.[1]

The presentation is variable and depends on the organ or system affected; it ranges from a self-healing disease to chronic recurrences.[5]
The spectrum of symptomatic disease varies from a single bony lesion to multiple bony, skin and visceral lesions.

Clinical features of LCH (listed by organ system)[4]

Bony lesions - osseous LCH

  • Bone is commonly affected (75% of cases).
  • Well-localised bone pain is a common presenting symptom, with pain during both activity and rest.
  • Lesions are lytic.
  • Bone pain usually correlates with a radiologically evident lesion but lesions can be painless.
  • There may be tender swelling of the soft tissue overlying the bone.
  • Common sites for bone LCH are skull, proximal femur and ribs.
  • Multifocal bony LCH is predominantly diagnosed in pre-school children.
  • Rarely, bone lesions may cause pathological fractures.

Skin and mucous membranes

  • Skin involvement occurs in 34% of patients.
  • Rashes may be macular, papular, nodular or petechial.
  • Skin rashes in neonates may regress spontaneously.
  • Scalp lesions may be scaly.
  • Any mucosal tissue can be affected; ulceration and bleeding can occur.
  • Oral LCH may give rise to recurrent gingival ulceration and 'floating teeth'.
  • When the skin of the inner ear is affected, this may cause copious otorrhoea.
  • Purpuric lesions of the nailbed occur with nail involvement.

CNS

  • CNS lesions are most frequently found in the hypothalamic-pituitary region where they lead to endocrine disorders involving the hypothalamic-pituitary axis:
    • Diabetes insipidus (DI) is reported in 10-50% of patients.
    • 53% of patients with DI develop growth hormone deficiency over 10 years.
  • LCH lesions at other sites in the brain may cause neurological symptoms as a result of mass effect.
  • Orbit, mastoid and temporal bone lesions may lead to localised problems, including proptosis and sinusitis.
  • Progressive neurodegenerative symptoms may arise decades after the initial presentation.

Lungs - pulmonary LCH[5]

  • Rare; occurs predominantly in young smokers.[6]
  • Nonproductive cough, dyspnoea pleuritic pain or spontaneous pneumothorax.
  • Abnormal CXR showing a reticular-micronodular pattern.
  • Nodular/cystic pattern on a high-resolution CT scan.
  • Isolated pulmonary LCH occurs frequently in adults, predominantly smokers (>90%), with a peak at 20-40 years of age. Women are slightly more likely to be affected than men.
  • Pulmonary LCH is not considered high-risk but may proceed to multisystem involvement.

Lymphadenopathy

  • This is fairly common.
  • There are usually no symptoms unless the enlarged nodes damage or obstruct nearby organs and LCH cells are not typically identified in draining lymph nodes of affected tissue.

'Risk' organs - liver, spleen, bone marrow

  • Diffuse infiltration or focal lesions of the spleen, liver or bone marrow are the most severe presentation and are defined as 'high-risk'.
  • Most commonly seen in infants less than 2 years of age.
  • Present with cytopenia or liver dysfunction.

Gastrointestinal (GI)

  • GI lesions are rare.
  • Sometimes associated with chronic diarrhoea, hypoalbuminaemia, weight loss or faltering growth.
  • May lead to ulceration and GI bleeding.

Other presentations
LCH can involve other organs - for example, scrotal mass was a rare presentation in one study.

The diagnosis of LCH is based on histological and immunological examination of a lesional biopsy, which at the same time may provide a healing stimulus:[1]

  • Morphological identification of characteristic Langerhans' cells.
  • Positive staining for CD1a, CD207 (Langerin) and S100 cell markers is diagnostic.
  • Birbeck's granules on electron microscopy.

Investigations will otherwise depend on the clinical presentation but usually include:[7]

  • A thorough physical examination, including skin and oral mucosa, height and weight.
  • Blood tests: FBC, clotting studies, U&E, LFT, urine osmolality.
  • Plain X-ray - for bone pain or suspected bone lesions.
  • Skeletal survey.
  • CT/MRI scans of head and spine.
  • Bone marrow biopsy may be required for staging.
  • Endoscopy if GI involvement is suspected.
  • For suspected pulmonary involvement, investigations are:
    • Plain CXR - may show upper lobe infiltrates.
    • Lung function tests - may show impaired diffusing capacity.
    • CT scan - may show typical changes of pulmonary LCH.
    • Bronchoalveolar lavage.
    • Bronchoscopy or surgical lung biopsy.
  • Otolaryngological examination with audiogram may also be indicated.

Treatment of LCH is risk-adapted. People with single lesions may respond well to local treatment, whereas those with multisystem disease require systemic therapy.[2]

General points

  • Because LCH is rare, there are relatively few clinical trials and less experience available to inform treatment.
  • Treatment may involve surgical excision, radiotherapy, chemotherapy, or combinations of these.
  • The prognosis and treatment protocol depend on the number of organs involved, which organ systems are involved and the degree of organ dysfunction.
  • Recommendations and protocols are available from the Histiocytosis Association.[8]

The following is an overview of current possible treatments, according to organs involved.

Limited cutaneous disease

  • No treatment (it may remit).
  • Topical steroids.
  • Topical nitrogen mustard.
  • Psoralen combined with ultraviolet A (PUVA) therapy.

Localised bone lesions

  • Surgical curettage is the usual treatment (for accessible sites).
  • Other treatments for bone lesions include:
    • Radiotherapy.
    • Intralesional steroids.
    • Bisphosphonates.
    • Early chemotherapy (vinblastine and prednisolone) for bony lesions at crucial anatomical sites.

CNS lesions

  • Radiotherapy may be used for isolated cerebral tumours.
  • Chemotherapy with cladribine or cytarabine is the most suitable treatment for pituitary/hypothalamic lesions, multifocal brain lesions or any brain lesion in multi-system disease.

Lymphadenopathy

  • Surgical excision of single nodes with LCH.
  • Regional node involvement may respond to a course of systemic steroids.
  • Chemotherapy for nodes resistant to treatment.

Pulmonary LCH[9]

  • Smoking cessation is essential. This may be the only treatment required.
  • If smoking cessations fails and treatment is required, corticosteroids are the main treatment.
  • Chemotherapy may be used for progressive disease not responding to steroids; however, this is a last resort because its efficacy is uncertain. Drugs which have been used in this context are vinblastine, methotrexate, cyclophosphamide, etoposide and, most recently, cladribine.
  • Pleurodesis should be considered for recurrent pneumothorax.
  • Lung transplantation can be considered for advanced disease.

Multi-system LCH

  • The standard initial treatment in children is a combination of prednisolone and vinblastine with 6-mercaptopurine added after the first six weeks.[10]
  • Compared with children, adults experience increased neurotoxicity, worse myelosuppression and more steroid toxicity with the above regime. Cladribine or cytarabine are recommended initial therapy for adults requiring systemic therapy.[3]
  • Duration of treatment of twelve months compared with six months reduces the rate of reactivation.[11]
  • Around 50% of patients with LCH do not respond to initial therapy or develop reactivation within five years.[3] Optimal treatment for these patients is, as yet, unknown:
    • A combined regimen of cladribine and cytarabine has shown some promise but is associated with high toxicity.[12]
    • Vemurafenib, an inhibitor of the BRAF V600E mutation, has shown efficacy in preliminary studies.[3, 13]
    • Stem cell transplantation may be used in patients with a poor prognosis whose LCH has not responded to conventional treatment.
  • Patients receiving systemic therapy for LCH are at risk of Pneumocystis jiroveci infection and require prophylaxis.

Endocrinopathies

  • DI should be treated with desmopressin.
  • Hormonal deficiencies should be adequately replaced as soon as diagnosed.

Lifelong follow-up is required because of the possibility of late recurrence or late complications. Complications of LCH may occur at any time from presentation or many years later. Complications can arise even in patients without multi-organ involvement. It is estimated that about 50% of LCH patients have late complications of the disease or its treatment.[14] Complications include:

  • Progressive neurodegeneration develops in 5% of people with LCH. Often severe and debilitating, the diagnosis is made by typical signal changes in the brain stem, basal ganglia, and cerebellum on neuroimaging, together with some neurological symptoms, such as ataxia, dysarthria, dysmetria, cognitive problems and behavioural abnormalities.[15]
  • DI (relatively common) - treated with desmopressin.
  • Late relapse or progression to systemic involvement.
  • Hypothalamic-pituitary dysfunction.
  • Hearing loss.
  • Sclerosing cholangitis
  • There may be an increased risk of other neoplasms.[9]
  • Prognosis depends on the extent and nature of organ involvement. The clinical course of LCH is extremely variable, ranging from a self-healing solitary bone lesion to widely disseminated life-threatening disease.[16]
  • Although survival rates for people without organ dysfunction are excellent, mortality rates for patients with organ dysfunction may reach 20%. Despite progress made in the treatment of LCH, disease reactivation rates remain above 30%, and standard second-line treatment is yet to be established. Treatment failure is associated with increased risks for death and long-term morbidity, including LCH-associated neurodegeneration.[2]
  • Survival of children with high risk LCH has improved dramatically, to nearly 90%.[15]
  • Neonates with LCH limited to the skin and mucous membranes have a good prognosis.[17]

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Further reading and references

  1. Hutter C, Minkov M; Insights into the pathogenesis of Langerhans cell histiocytosis: the development of targeted therapies. Immunotargets Ther. 2016 Oct 125:81-91. eCollection 2016.

  2. Rodriguez-Galindo C, Allen CE; Langerhans cell histiocytosis. Blood. 2020 Apr 16135(16):1319-1331. doi: 10.1182/blood.2019000934.

  3. Abla O, Weitzman S; Treatment of Langerhans cell histiocytosis: role of BRAF/MAPK inhibition. Hematology Am Soc Hematol Educ Program. 20152015:565-70. doi: 10.1182/asheducation-2015.1.565.

  4. Zinn DJ, Chakraborty R, Allen CE; Langerhans Cell Histiocytosis: Emerging Insights and Clinical Implications. Oncology (Williston Park). 2016 Feb30(2):122-32, 139.

  5. Girschikofsky M, Arico M, Castillo D, et al; Management of adult patients with Langerhans cell histiocytosis: recommendations from an expert panel on behalf of Euro-Histio-Net. Orphanet J Rare Dis. 2013 May 148:72. doi: 10.1186/1750-1172-8-72.

  6. Radzikowska E; Pulmonary Langerhans' cell histiocytosis in adults. Adv Respir Med. 201785(5):277-289. doi: 10.5603/ARM.a2017.0046. Epub 2017 Oct 30.

  7. Satter EK, High WA; Langerhans cell histiocytosis: a review of the current recommendations of the Histiocyte Society. Pediatr Dermatol. 2008 May-Jun25(3):291-5.

  8. The Histiocytosis Association

  9. Vassallo R, Ryu JH; Pulmonary Langerhans' cell histiocytosis. Clin Chest Med. 2004 Sep25(3):561-71, vii.

  10. Matsuki E, Tsukada Y, Nakaya A, et al; Successful treatment of adult onset Langerhans cell histiocytosis with multi-drug combination therapy. Intern Med. 201150(8):909-14. Epub 2011 Apr 15.

  11. Gadner H, Minkov M, Grois N, et al; Therapy prolongation improves outcome in multisystem Langerhans cell histiocytosis. Blood. 2013 Jun 20121(25):5006-14. doi: 10.1182/blood-2012-09-455774. Epub 2013 Apr 15.

  12. Donadieu J, Bernard F, van Noesel M, et al; Cladribine and cytarabine in refractory multisystem Langerhans cell histiocytosis: results of an international phase 2 study. Blood. 2015 Sep 17126(12):1415-23. doi: 10.1182/blood-2015-03-635151. Epub 2015 Jul 20.

  13. Haroche J, Cohen-Aubart F, Emile JF, et al; Dramatic efficacy of vemurafenib in both multisystemic and refractory Erdheim-Chester disease and Langerhans cell histiocytosis harboring the BRAF V600E mutation. Blood. 2013 Feb 28121(9):1495-500. doi: 10.1182/blood-2012-07-446286. Epub 2012 Dec 20.

  14. McClain KL, Natkunam Y, Swerdlow SH; Atypical cellular disorders. Hematology Am Soc Hematol Educ Program. 2004:283-96.

  15. Abla O, Rollins B, Ladisch S; Langerhans cell histiocytosis: progress and controversies. Br J Haematol. 2019 Dec187(5):559-562. doi: 10.1111/bjh.16099. Epub 2019 Jul 15.

  16. Abla O, Egeler RM, Weitzman S; Langerhans cell histiocytosis: Current concepts and treatments. Cancer Treat Rev. 2010 Jun36(4):354-9. doi: 10.1016/j.ctrv.2010.02.012. Epub 2010 Feb 25.

  17. Battistella M, Fraitag S, Teillac DH, et al; Neonatal and early infantile cutaneous langerhans cell histiocytosis: comparison of self-regressive and non-self-regressive forms. Arch Dermatol. 2010 Feb146(2):149-56. doi: 10.1001/archdermatol.2009.360.

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