Histological Spectrum of Pure Neuritic Leprosy:

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Department of Histopathology Postgraduate Institute of Medical Education & Research Chandigarh,India Histological Spectrum of Pure Neuritic Leprosy: Experience at Tertiary Care Centre Dr Uma Nahar

INTRODUCTION Leprosy is still an important public health problem in India with Nerve involvement being a rare complication. Despite stringent control measures established by WHO and a consequent decrease worldwide, rate of newly detected leprosy cases remains epidemiologically high in endemic countries (WHO 2010).

INTRODUCTION Leprosy patients may present with peripheral neuropathy (simple or multiple mononeuropathies and/or polyneuropathy) in absence of any verifiable cutaneous lesions The clinical features of leprotic nerve involvement include nerve enlargement, tenderness, pain and sensory motor impairment. These are not specific and not always present. The most commonly affected nerves :posterior tibial, peroneal, ulnar and median nerves

DEFINITION Pure neuritic leprosy (PNL): Neural involvement by leprosy in absence of skin involvement. Accounts for 5-17.7% of all leprosy cases. Responsible for the disabilities and deformities. Confirmation of a PNL diagnosis requires the demonstrated presence of Mycobacterium leprae in a biopsy of any affected sensory nerve.

Diagnosis Most of the cases are diagnosed based on clinical findings. Nerve biopsy is required only in doubtful or challenging cases. Nerve biopsy examination is an important auxiliary procedure for diagnosing pure neural leprosy (PNL) Elevated levels of serum antiphenolic glycolipid antibodies (ELISA) would make a leprosy diagnosis certain, probable or possible Jardim et al.2005

The gold standard : Histopathological examination of a peripheral nerve biopsy. It is important for a histopathologist to recognise the histological spectrum of PNL. Value of nerve biopsy examination increases when the results are interpreted in the context of pertinent clinical, epidemiological, electroneuromyographical and laboratory data [i.e., M. leprae DNA determined with polymerase chain reaction(pcr) Mem Inst Oswaldo Cruz, Rio de Janeiro, Vol. 107(2): 246-253, March 2012

AIM To assess the histological spectrum of Pure Neuritic Leprosy

Material and Methods Retrospective study( January 2000 to June 2016) All histologically diagnosed cases of PNL were analysed. Biopsies were retrieved from the archives from department of Histopathology. All biopsies were reviewed by 3 histopathologists.

Material and Methods.. Detailed demographic profiles and clinical findings were noted from the histopathology requisition proforma: -Duration of symptoms -Nerve thickness -Loss of sensation -Associated features

Material and Methods.. The nerve samples was fixed in 4% paraformaldehyde Routinely processed and embedded in paraffin for routine histopathological examination Haematoxylin-eosin stain to evaluate inflammatory infiltrate and cellularity Masson s trichrome to assess fibrosis and nerve structure Ziehl Nelsen stain to detect AFB Luxol fast blue stain for Myelin IHC for Neurofilament protein

Material and Methods-Histopathology Detailed histopathological examination was done including special stains Modified Ziehl-Neelsen Luxol Fast Blue for myelin IHC for neurofilament protein(nfp) Various histological parameters were graded from scale 0 to 3 0-absent 1-mild 2-moderate 3-marked

RESULTS Total PNL cases during 2000-2016(16 year)period was 20 Clinical demography Average age : 40.8 yrs (Range 22-82 yrs) Male preponderance (5.7:1) The suspected clinical diagnosis : -Hansen in 15 cases (75% ) -Mononeuritis multiplex in 3 cases (15% ) -Demyelination in 1 case (5%) -Vasculitis in 1 case (5%)

RESULTS. Most common nerve biopsied : - Sural nerve (14 cases,70%) - Ulnar nerve (3cases,15%) - Radial - Lateral cutaneous and - Dorsal cutaneous (1 each, 5%)

RESULTS. Nerve biopsies in each case showed Both Longitudinal and transverse section in 11 cases (55%); Transverse Section only in 6 cases (30%) and Longitudinal Section only in 3 cases (15%) Average fascicles : 5, ranging from 3-9 Skin biopsy in 6 patients- no e/o leprosy

Histopathological Findings(n-20) 70 60 50 40 30 20 10 0 Perineural thickening Endoneural thickening Perineural inflammation Endoneural inflammation 0 1 2 3 Perineural thickening- 19 (95%) Endoneural thickening- 9 (45%) Endoneural LM inflammation- 19 (95%) Perineural LM inflammation- 18 (90%)

Histopathological Findings (n-20) 90 80 70 60 50 40 30 20 10 0 Endoneural granuloma Perineural granuloma Endoneural foam cells Perineural foam cells 0 1 2 3 Granuloma (n-14) : Endoneural : 14 (70%) Perineural : 3 (15%) Foam cells (n-13) : Endoneural : 13 (65%) Perineural : 4 (20%) Granuloma only : 4 (20%) Foam cells only : 3 (15%) Both granuloma and foam cells : 10 (50%) None of them : 3 (15%)

Histopathological Findings (n-20) 100 90 80 70 60 50 40 30 20 10 0 Perivascular inflammation Vasculitis Necrosis Absent Present

Lepra stain for acid fast bacilli was positive in 11 cases(55%) and negative in 9 cases(45%). One case showed normal histology with lepra bacilli positivity There was no significant histological difference between lepra bacilli positive and negative cases. Myelin and Axonal loss: Absent in only 1 case (5%) Moderate in 4 cases (20% ) Severe in 15 cases (75%)

LFB: Myelin stain

IHC: NFP

LFB LFB/PAS NFP

Atypical Histopathological Findings Vasculitis (2/20, 10%) Necrosis (1/20, 5%) Plasma cell rich inflammatory infiltrate (1/20, 5%) Normal morphology with Lepra positivity (1/20, 5%)

Histological Parameters AFB positive cases (11) AFB negative cases (9) Perineural thickening 10(90.9%) 9(100%) Endoneural thickening 4(36.3%) 4(44.4%) Perineural inflammation 10(90.9%) 9(100%) Endoneural inflammation 10(90.9%) 9(100%) Perineural granuloma 2(18.1%) 1(11.1%) Endoneural granuloma 9(81.8%) 7(77.7%) Perineural foam cells 2(18.1%) 2(22.2%) Endoneural Foam cells 8(72.7%) 6(66.6%) Perivascular inflammation 10(90.9%) 9(100%) Vasculitis 1(9%) 1(11.1%) Necrosis 0 1(11.1%) Myelin loss 10(90.9%) 9(100%) Axonal loss 10(90.9%) 9(100%)

CONCLUSION Endoneural inflammation, granuloma and foam cell infiltrate are common features of PNL. Inflammation and granulomas can be seen in perineural space as well. There may be variable epineural and perineural thickening, depending on the duration of the disease. Myelin and axonal loss are almost universal Myelin stain and IHC for NFP should be performed in all cases.

CONCLUSION Necrosis and vasculitis can be rarely found in PNL Even if morphologically biopsy is normal, lepra stain should be performed in all suspected cases of PNL Anti-PGL1 antibodies in patient s sera can be helpful in early diagnosis PCR may be done in cases with negative Lepra stain

Summary: Flowchart for the investigation of pure neuritic leprosy Einar WILDER- SMITH Neurol J Southeast Asia December 2002