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Friday, January 28, 2022

Fw: Ref.: (LML) WHO Goodwill Ambassador's Leprosy Bulletin NO. 107, January 2022

 

 

 

 
Leprosy Mailing List – January 28,  2022

 

Ref.:  (LML) WHO Goodwill Ambassador's Leprosy Bulletin NO. 107, January 2022

From:  Takahiro Nanri, Tokyo, Japan

 

Dear Dr. Schreuder and Friends,  


Warm greetings from Sasakawa Health Foundation/Sasakawa Leprosy (Hansen's Disease) Initiative in Tokyo. We have issued WHO Goodwill Ambassador's Leprosy Bulletin NO. 107 January 2022 "Don't forget leprosy" on World Leprosy Day today. In this issue, we feature:


MESSAGE FROM THE AMBASSADOR

In August 2021, I launched an awareness campaign called "Don't forget leprosy." The slogan is meant to be a reminder that persons affected by leprosy and their families continue to experience stigma and discrimination, Read More


INTERVIEW - Professor Muhammad Yunus, 2006 Nobel Peace Prize Laureate and founder of Grameen Bank

Change the system rather than looking for solutions within the system

Based on the idea that "the poor themselves can create a poverty-free world" as long as we "free them from the chains that we have put around them," Professor Muhammad Yunus developed a system of "microcredit" that gives very small collateral-free business loans to society's poorest people.  Read more


SPOTLIGHT
Entrepreneurial success in Bangladesh

Maksuda Khatun's life story exemplifies what can happen when an individual is given just enough financial or material support to start a business. At the age of 18, Maksuda noticed a white patch on her hand. Read more


INITIATIVE NEWS
 "Don't forget leprosy" campaign update

World Leprosy Day has been observed annually on the last Sunday of January since 1954. The purpose of this day is to increase public awareness of leprosy (Hansen's disease). Read more


INITIATIVE NEWS
A month of activity for Global Appeal 2022

Initiated by the WHO Goodwill Ambassador for Leprosy Elimination in 2006, the annual Global Appeal to End Stigma and Discrimination against Persons Affected by Leprosy takes place annually in January in conjunction with World Leprosy Day. Read more


PEPORT- Five members of Morhan's Women's Policy Department (DPW-Morhan)

We need to hear what girls and women affected by Hansen's disease have to say

Women and girls have been part of the Movement for the Reintegration of Persons Affected by Hansen's Disease (Morhan) since its foundation in 1981 in Brazil. Read more


INITIATIVE NEWS
Three regional meetings held in preparation for first Global Youth Forum

The Nippon Foundation and Sasakawa Health Foundation, now working together as the Sasakawa Leprosy (Hansen's Disease) Initiative, have been supporting the empowerment of persons who have experienced leprosy for nearly 30 years.  Read more


WISH LIST - Maksuda Khatun, Treasurer, Sirajganj District Leprosy and Disability Federation, Sirajganj, Bangladesh and Dr. Michael Chen, Secretary General, HANDA Rehabilitation & Welfare Association, China.

With World Leprosy Day approaching, the Leprosy Bulletin asked two people involved in "Don't forget leprosy" activities for three wishes related to how they would like the world to change for persons affected by leprosy.  Read more


BACK ISSUES 

We hope that you would enjoy reading the latest Leprosy Bulletin.


Takahiro NANRI, Ph.D.


Executive Director, Sasakawa Health Foundation

*********************************************************
Sasakawa Leprosy (Hansen's Disease) Initiative
Sasakawa Health Foundation
Tel
81-3-6229-5377, Fax81-33-6229-5388
email: hansen@shf.or.jp
website: https://sasakawaleprosyinitiative.org/,  https://www.shf.or.jp
********************************************************* 

 

LML - S Deepak, B Naafs, S Noto and P Schreuder

LML blog link: http://leprosymailinglist.blogspot.it/

Contact: Dr Pieter Schreuder << editorlml@gmail.com

 

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Thursday, January 27, 2022

Fw: Ref.: (LML) Median nerve damage in leprosy

 

 

 
Leprosy Mailing List – January 27,  2022

 

Ref.:  (LML) Median nerve damage in leprosy

 

From:  Zhaudat Umerov, Moscow, Russia

 

Dear Pieter,

 

 

Thanks to Wim Theuvenet  for the important question in the LML mail of January 9th.2022. The possibility of widespread use of nerve decompression techniques in the carpal canal in the early stages (loss of sensitivity, without muscle atrophy) is a very tempting program to combat disability. This can be successful with the detailed development of both indications and contraindications.  

 

It may be useful to recall the mechanism of nerve damage. The results of the study using polyclonal and monoclonal antibodies established cross reactive (mimicking) antigenic determinants of M.leprae and the myelin sheath of peripheral nerves. Consequently, the pathogen causes a cellular and humoral immune response against the pathogen and peripheral nervous tissue (CMI and autoantibodies). The normal (non-immunodeficient) host immune system protects the body by removing autoreactive T cells in the thymus and peripheral lymphatic system using a subclass of CD4+CD25 FOXP3+ T-regulatory cells. The removal of these cells suppresses the host's cellular immune response against the pathogen and the myelin sheath of Schwann cells. This is typical for multibacillary leprosy. However, T-reg. cells do not affect B-lymphocytes and the production of cross-reacting IgM and IgG antibodies.     

 

The place of doubling (reproduction) of the pathogen is the phagolysosome compartment of the host macrophages, and the cell wall of macrophages and membranes of phagolysosomes are impervious to high-molecular IgG - 150 kDa, IgM - 970 kDa autoantibodies. Consequently, the reaction of autoantibodies with intracellular pathogen and Schwann cell myelin does not occur. However, antibodies react with pathogen antigens expressed on surrounding tissues including epineurium.  An inflammatory immune response causes fibrosis, which compresses nerve fibers.

 

In these cases, the functional activity of the nerves may persist for a long time, which is an indication for performing a nerve decompression operation in the carpal tunnel. 

Stimulation of the host with low doses of the M.leprae mimicking antigen can lead to tolerance by suppression of increasing Treg cells. In this case, a strong Th1-mediated cellular immune reaction develops against the pathogen and the myelin sheath of Schwann cells, causing a decrease in the bacillary load of host tissues and damage to peripheral nerves by irreversible demyelination. This is typical for paucibacillary leprosy. Performing a nerve decompression operation in the carpal tunnel in such patients will not fulfill the expectations.  

 

I hope the above will be useful when deciding on surgical intervention.

 

   Kind regards,

 

   Zhaudat UMEROV

   Moscow and Antalya.

 

 

LML - S Deepak, B Naafs, S Noto and P Schreuder

LML blog link: http://leprosymailinglist.blogspot.it/

Contact: Dr Pieter Schreuder << editorlml@gmail.com

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Monday, January 24, 2022

Fw: Ref.: (LML) Median nerve damage in leprosy




From: Leprosy Mailing List <leprosymailinglist@googlegroups.com>
Sent: 24 January 2022 16:14
To: Leprosy Mailing List <leprosymailinglist@googlegroups.com>
Subject: Ref.: (LML) Median nerve damage in leprosy
 

 

 
Leprosy Mailing List – January 24,  2022

 

Ref.:  (LML) Median nerve damage in leprosy

 

From:  Arry Pongtiku, Papua, Indonesia

 

Dear Pieter,

 

The photo from Dr Noto and discussion, I would also say atrophy of the palm muscles, scars from burns of the skin of the fingers, contracture of fingers means it is late and  nerve damaged already and usually poor prognosis. Self Care and prednisolone  treatment may  work effectively to survive the nerves  before 6 months  or during leprosy reaction. Filling POD (Prevention of Disability) form is important for  leprosy health workers to detect the weakness and deformity of nerves.

 

I would  add some photos about weak fingers, hand and self care exercise.

Thank you very much,

 

Best regards,

 

Arry Pongtiku,

Papua- Indonesia

 

LML - S Deepak, B Naafs, S Noto and P Schreuder

LML blog link: http://leprosymailinglist.blogspot.it/

Contact: Dr Pieter Schreuder << editorlml@gmail.com

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Tuesday, January 18, 2022

Fw: Ref.: (LML) Median nerve damage in leprosy

 


Leprosy Mailing List – January 18,  2022

 

Ref.:  (LML) Median nerve damage in leprosy

 

From:  Zhauda Umerov, Moscow, Russia

 

 

Dear Pieter,

 

What did I see on the figure from S. Noto. The doctor correctly diagnosed the patient with paucibacillary  leprosy and treated with the WHO suggested MDT and he was ready to be released from treatment, but the accompanying ( untreated ) neuropathy was missed and the deformity continued to develop. Atrophy of the palm muscles, scars from burns of the skin of the fingers indicate the duration of leprosy - at least 3 - 5 years. However, the diagnosis of leprosy was made 6 months ago and what we see is that irreversible nerve changes had happened.

 

The reason is the lack of lab. tests of the early stages of leprosy. It is appropriate to recall that 20 years ago, Stewart Cole's brilliant team deciphered the genome of the leprosy pathogen. Unfortunately, the huge work of researchers has not reached the practical medicine.

 

The patient has been treated with the WHO suggested MDT in which there is no drug for the protection of nerve damage in leprosy. It is probably believed that nerve damage is a complication, but not leprosy itself and there is no need to develop a treatment course. A very strange position of WHO experts.

 

In Russia, it is very popular in such cases to ask two questions: "Who is to blame? and What to do?" Perhaps we should answer these questions as well. Here's what I saw in the photo of S. Noto and I completely agree that clinical skills should be on the forefront for everyone, not only a field doctors and their nurses.

 

Kind regards,

 

Zhauda UMEROV

Moscow and Antalya


 

LML - S Deepak, B Naafs, S Noto and P Schreuder

LML blog link: http://leprosymailinglist.blogspot.it/

Contact: Dr Pieter Schreuder << editorlml@gmail.com

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Sunday, January 16, 2022

Fw: Ref.: (LML) Median nerve damage in leprosy

 


Leprosy Mailing List – January 16,  2022

 

Ref.:  (LML) Median nerve damage in leprosy

 

From:  Joel Almeida, London and Mumbai

 

 

Dear Pieter & colleagues,

 

Esteemed colleagues have made important points about protecting HD patients adequately. Those who monitor nerve function regularly set a good example (e.g. the Brazilian national program, Fondation Raoul Follereau personnel, others). Respect for patients prompts adequate medical care, and wider care.

 

It may be helpful to imagine a patient as a family member walking a tightrope from disease to healing. If they fall off that tightrope, they will suffer irreversible damage. We need to provide adequate safety nets. What are the safety nets we would provide to a family member?

 

1) Antimicrobial protection with uninterrupted MDT. If they have LL (lepromatous) HD and live in an endemic area, then they would benefit also from post-treatment prophylaxis to protect them against reinfection. This can be with MDT or with combinations of 3 bactericidal drugs. MIP vaccine often yields rapid clearance of bacilli in even LL patients, making it useful. 

 

2) Nerve function monitoring & prompt intervention when required

 

A pilot survey in two rural communities in India revealed that 15% to 33% of persons who previously received MDT had visible deformity (1). Fewer than 5% of patients in that Indian state had visible deformity at diagnosis. Evidently, most visible deformity in that state arose during or after MDT. A total-population survey among over 100,000 persons in a rural area 100 km from Mumbai (India) revealed a prevalence of visible deformity among previously treated patients of 2308 per million population (2). This suggests that several million people are living with visible deformities that developed during or after MDT treatment.

 

A randomized double-blind clinical trial among persons with mild and recent sensory impairment compared prednisolone, given for 4 months, with placebo.(3) The placebo group had a 158% higher risk of deterioration in sensory scores between the start and end of treatment. Prednisolone works.

 

In South Asia, 85% of nerve damage during MDT was found to be "silent", without signs or symptoms of reaction (4). Even the patients did not suspect anything until they suffered irreversible damage. MB patients showed a greatly multiplied risk of nerve damage compared to PB patients. Therefore, assessment of nerve function in MB patients (correctly classified) needs to be done at diagnosis and at least every quarter thereafter. This needs to continue for 2 years after the start of MDT. Otherwise, patients who newly develop sensory impairment are left without timely prednisolone treatment, allowing permanent nerve damage. That in turn leads to visible deformity, with all its adverse consequences.    

 

Specially trained and skilled health workers provided with transport and covering a wide geographical area have been used for monitoring nerve function in well-run programs (including in exemplary sub-districts of India). NGOs such as Fondation Raoul Follereau, who monitor nerve function regularly and intervene with prednisolone promptly, are showing respect for patients.

 

 

3) Surgical intervention if patients fall through the safety nets 1) and 2) above.

 

All the above are what one would do for one's mother or child (or indeed one might require for oneself if afflicted by HD). HD patients, like others, are entitled to adequate medical care according to the Universal Declaration of Human Rights, article 25. We can keep removing patients from registers and assuring them that they are healed. However, they might not believe us when they are left with visible deformity despite having started MDT without deformity.

 

In 2022 we can improve the quality of care for patients after diagnosis, especially by ensuring

A) Uninterrupted MDT for all, plus post-treatment prophylaxis for LL HD patients in endemic areas

 

B) Quarterly nerve function monitoring, especially for MB patients during the first 2 years after the start of MDT, with prompt prednisolone treatment at the first sign of sensory loss. 

 

C) Availability of surgical interventions for patients who fall through the safety nets above

 

For millennia people with HD have been neglected as if they do not matter, as if they are sub-human in some way or blameworthy. This neglect and ostracism often deprive them of normal relationships, schooling, housing, utilities, income, etc. Denial of adequate medical care need not be added to their deprivations. It seems more humane to monitor nerve function every quarter, as done in the Brazilian national program, and to intervene promptly with prednisolone when required.

 

Best,

 

Joel Almeida

 

References

 

1)      Aggarwal A, Pandey A. Inverse sampling to study disease burden of leprosy. Indian J Med Res 132, October 2010, pp 438-441.

2)      Ganapati R, Pai VV, Tripathi A. Can primary health centres offer care to the leprosy disabled after integration with general health services? - a study in rural India. Lepr Rev 2008, 79:340–341

3)      Van Brakel WH1, Anderson AM, Withington SG, Croft RP, Nicholls PG, Richardus JH, Smith WC. The prognostic importance of detecting mild sensory impairment in leprosy: a randomized controlled trial (TRIPOD 2). Lepr Rev. 2003 Dec;74(4):300-10.

4)      Croft RP, Nicholls PG, Richardus JH, Smith WC. Incidence rates of acute nerve function impairment in leprosy: a prospective cohort analysis after 24 months (The Bangladesh Acute Nerve Damage Study). Lepr Rev. 2000 Mar;71(1):18-33.


LML - S Deepak, B Naafs, S Noto and P Schreuder

LML blog link: http://leprosymailinglist.blogspot.it/


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Saturday, January 15, 2022

Fw: Ref.: (LML) Leprosy Research

 

 
Leprosy Mailing List – January 15,  2022

 

Ref.:  (LML) Leprosy Research

 

From:  Pieter Schreuder, Maastricht, the Netherlands

 

 

Dear colleagues,

 

Kindly note the correct Email address for Robert  Machang'u:

machangu@sua.ac.tz


 

Pieter AM Schreuder

Editor LMl



LML - S Deepak, B Naafs, S Noto and P Schreuder

LML blog link: http://leprosymailinglist.blogspot.it/

Contact: Dr Pieter Schreuder << editorlml@gmail.com

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Friday, January 14, 2022

Fw: Ref.: (LML) Leprosy Research



 
Leprosy Mailing List – January 14,  2022

 

Ref.:  (LML) Leprosy Research

 

From:  Robert Machang'u, Morogoro, Tanzania

 

Dear Pieter,

 

I would like to know if there are colleagues among us who would be interested to be interested to partner with a Tanzanian team interested in research & outreach in HD hotspots. 

 

Interested people could contact me directly, or through LML

 

Regards,

 

Robert Machang'u

 

Department of Veterinary Microbiology and Parasitology, Sokoine University of Agriculture, Morogoro, Tanzania

machnagu@sua.ac.tz


LML - S Deepak, B Naafs, S Noto and P Schreuder

LML blog link: http://leprosymailinglist.blogspot.it/

Contact: Dr Pieter Schreuder << editorlml@gmail.com

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Thursday, January 13, 2022

Fw: Ref.: (LML) Median nerve damage in leprosy

 

 
Leprosy Mailing List – January 13,  2022

 

Ref.:  (LML) Median nerve damage in leprosy

 

From:  Marcos Virmond, Bauru, Brazil

 

Dear Pieter

 

Discussions initiated by Dr. Noto on nerve damage/surgery (Dr. Theuvenet) are most welcome and comments by Dr. De Laguiche quite opportune.

 

Let me say that this issue has direct connection with a post by Dr. B. Naafs some weeks ago, which I dare to resume on the following - monitoring nerve function is an essential step in the follow-up of leprosy cases.

 

In the same line, I dare to say that - correctly indicated, opportune and quality nerve decompression surgery is an essential part of any leprosy control program. It must be available as a choice for cases with progressive nerve function loss non responsive to adequate steroids treatment.

 

With kind regards,

 

Marcos Virmond

School of Medicine-USP,  Bauru


LML - S Deepak, B Naafs, S Noto and P Schreuder

LML blog link: http://leprosymailinglist.blogspot.it/

Contact: Dr Pieter Schreuder << editorlml@gmail.com

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Wednesday, January 12, 2022

Fw: Ref.: (LML) Median nerve damage in leprosy

 

 
Leprosy Mailing List – January 12,  2022

 

Ref.:  (LML) Median nerve damage in leprosy

 

From:  Laila de Laquiche, Curitiba, Brazil

 

Dear Pieter,


I thank Dr. Grauwin for his contribution to our discussion on nerve damage (January 10 - LML) which masterfully explained details of upper limb neuritis: Ulnar and Median Nerve, in addition to indications for nerve decompression and treatment. Acting in African territory certainly brings the necessary difference for quality medical care in that region, which I particularly appreciate this effort.


The question I raised is what would be the correct therapeutic approach, since this case under discussion (Dr. Noto - Italia 07 January LML) was diagnosed and treated with a Paucibacillary regimen for 6 months. 

 

Paraesthesia was accidentally diagnosed at the end of treatment due to an accidental injury to the fingers. We do not have data on which initial lesions corroborated this clinical classification and if there was an initial analysis of the sensory and motor function of that limb or even if there was a suspicion of neural damage. But if there were, it would already be indicative of MB treatment according to the WHO guidelines.


The biggest question is: what is the desired therapeutic approach: to face neuritis as an immunological reaction or as a continuation of the neural injury directly caused by the bacillus lodged in the nerve sheaths?


I don't have that answer, but I would certainly like to fully treat patients who suffer from an infectious-immunological disease, at least as far as the infectious part is concerned. Both approaches are not mutually exclusive and we can continue to seek our gold standard in the management of these patients.


Sincerely,

 

Laila de LAGUICHE

Curitiba - Paraná

 

LML - S Deepak, B Naafs, S Noto and P Schreuder

LML blog link: http://leprosymailinglist.blogspot.it/

Contact: Dr Pieter Schreuder << editorlml@gmail.com

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Monday, January 10, 2022

Fw: Ref.: (LML) Median nerve damage in leprosy

 


Leprosy Mailing List – January 10,  2022

 

Ref.:  (LML) Median nerve damage in leprosy

 

From:  Michel-Yves Grauwin, Lille, France


Dear Pieter, dear colleagues,


Thanks to Doctor NOTO (LML January 7) for his observation of the tenderness in the median nerve territory.

If we look closely at the image, there does not seem to be any muscular involvement of the median nerve yet, the volume of the thenar eminence appears to be preserved.


And then, on the other side, the volume of the hypothenar eminence, ulnar side seems a little reduced and the 3 middle fingers are slightly clawed, even if there is not the classic hyperextension of the MCP joints, we could perhaps- be suspected of a beginner medio-ulnar involvement. The involvement is undoubtedly recent and in this case the MDT, whether PB or MB, does not change much in the nerve involvement of this hand (LML doctor de LAQUICHE - January 8).


If this is confirmed that it is recent, an accurate baseline neurological workup should be done and traced and treated with prednisolone.


Nerve decompression is only indicated in the event of failure of this well-conducted and protocolized cortisone treatment (LML doctor THEUVENET 9 January).

This is what we are doing in Francophone West Africa in support of ministries of health and national leprosy control programs with the FOLLEREAU Foundation.


This disability prevention program has been in place in many countries for a long time with interesting and encouraging results when diagnoses of nerve damage are made early enough, taken care of and followed up. We also have results with systematic management of all WHO grade I, early impairment of the sensitivity and trophicity of the skin before muscle involvement as I was able to observe recently during supervisions with the national program doctors in Senegal in October and in Guinea in December.

 

Cordial greetings


Dr Michel-Yves GRAUWIN

Neuro-orthopedic surgeon


LML - S Deepak, B Naafs, S Noto and P Schreuder

LML blog link: http://leprosymailinglist.blogspot.it/

Contact: Dr Pieter Schreuder << editorlml@gmail.com

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Sunday, January 9, 2022

Fw: Ref.: (LML) median nerve damage in leprosy

 

Leprosy Mailing List – January 9,  2022

 

Ref.:  (LML) median nerve damage in leprosy

 

From:  Wim Theuvenet, Apeldoorn, the Netherlands

------------------------------------------------------------------------------------------------

 

Dear Pieter,

 

Thanks to Salvatore Noto for sharing this patient in the LML mail of January 7th.

 

When there is recent loss of sensation and no loss of extrinsic muscle strength, would Salvatore or any leprosy control programme consider a nerve decompression of the median nerve at the carpal tunnel?

 

With best regards,

 

Wim Theuvenet


--------------------------------------------------------------------------------------------------------------

LML - S Deepak, B Naafs, S Noto and P Schreuder

LML blog link: http://leprosymailinglist.blogspot.it/

Contact: Dr Pieter Schreuder << editorlml@gmail.com

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Saturday, January 8, 2022

Fw: Ref.: (LML) Median Nerve damage in leprosy

 

 
Leprosy Mailing List – January 8,  2022

 

Ref.:  (LML) Median Nerve damage in leprosy

 

From: Laila de Laquiche, Curitiba, Brazil

 

 

 

 

Dear Pieter,


In response to Dr. Noto (LML, January 2022), unfortunately, we can say that this is a very frequent reality in Brazil as well.


The diagnosis of paucibacillary instead of multibacillary confirms the lack of common tools capable of correctly classifying the patient, in addition to demonstrating that the treatment proposed by the WHO may be insufficient in many cases.

 


Sincerely,

 

Laila

Curitiba, Paraná

 

LML - S Deepak, B Naafs, S Noto and P Schreuder

LML blog link: http://leprosymailinglist.blogspot.it/

Contact: Dr Pieter Schreuder << editorlml@gmail.com

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Fw: Ref.: (LML) Infolep monthly overview of new publications on leprosy - Jan '22


 

Leprosy Mailing List – January 8,  2022

 

Ref.:  (LML) Infolep monthly overview of new publications on leprosy - Jan '22

 

From:  Anniek Akerboom, Amsterdam, the Netherlands

 

 




Dear colleagues,
 

Infolep wishes you a Happy and Knowledgeable New Year!


Many thanks for your continued support! We are excited to keep you up-to-date with the latest information on leprosy this new year.

This month we celebrate World Leprosy Day on Sunday 30 January. The theme of World Leprosy Day 2022 is "United for Dignity." We want everyone to know that people who experience leprosy have the right to a dignified life free from disease-related stigma and discrimination. Watch this video in which people who experience leprosy express what dignity means to them.

The ILEP Federation announced the new ILEP strategy for 2021-2025 'Towards a world free from leprosy'. The new strategy comprises five key strategic goals that are seen as potential global 'game-changers'. Click here to learn more.

The Leprosy Mission has launched a new quarterly newsletter for the leprosy/NTD sector. The aim is to equip people within the sector with new and interesting insights, best practice tips from TLM's experience, and other information. Sign-up here and multiply your impact!

Enjoy reading the latest publications on leprosy and have a look at the coming events below, this time including funding opportunities. Feel free to contact me to receive full-text versions if these cannot be found through the Infolep portal. Also, I would be happy to assist you with literature searches on Infolep.

Warm regards,

Anniek Akerboom

Infolep Coordinator
www.leprosy-information.org
a.akerboom@infolep.org
 

 



 



Leprosy Review highlights

 



Click here to go to all publications of the latest Leprosy Review issue focusing on self-care
 

The 21st International Leprosy Congress (ILC) – 2022 8th to 11th November, 2022, Hyderabad, India Theme: Better Knowledge – Early Diagnosis – Improved Care
Leprosy Review. Lepra. 2021; 92 (4) : 437-438. 
 

Organizing and managing a programme for self-care in leprosy
Celiktemur B, Choudhury SM, Lilford R. Leprosy Review. Lepra. 2021; 92 (4) : 338-343.
 

Application of behavioural psychology principles to self-care programmes for people living with leprosy
Choudhury SM, Kudrna L, Celiktemur B, et al. Leprosy Review. Lepra. 2021; 92 (4) : 344-355.
 

Inflamed skin lesions along the course of a nerve as patient self-help proxy indicator of nerve abnormalities in leprosy
Balagon MF, Maghanoy AM, Roferos FO, et al. Leprosy Review. Lepra. 2021; 92 (4) : 385-397.
 

First cases of Mycobacterium leprae (Hansen's disease) detection in Côte d'Ivoire using molecular diagnosis (PCR)
N'Golo David C, Christiane AA, Henry K, et al. Leprosy Review. Lepra. 2021; 92 (4) : 406-411.
 

 



 



Leprosy & COVID-19

 



Updates on management of leprosy in the context of COVID-19 pandemic: Recommendations by IADVL SIG Leprosy
Narang T, Bhardwaj A, Gupta S, et al. Indian Dermatology Online Journal. Medknow. 2021; 12 (7) : 24.
 

Erythema nodosum leprosum and active leprosy after ChAdOx1-S/nCoV-19 recombinant vaccine. A report of two cases
Rebello PFB, Pennini S. Leprosy Review. Lepra. 2021; 92 (4) : 421-426.
 

Multibacillary leprosy unmasked by COVID-19 vaccination.
Aponso S, Hoou L, Wei Y, et al. JAAD case reports. 2021.
 

 



 



New resources

 



Development of immunodiagnostic tests for leprosy: from biomarker discovery to application in endemic areas
van Hooij A. Faculty of Medicine, Leiden University Medical Center. Leiden University. 2021.
 

Mimicking B and T cell epitopes between Mycobacterium leprae and host as predictive biomarkers in type 1 reaction in leprosy.
Pathak V, Singh I, Singh S, et al. Scientific reports. 2021; 11 (1) : 24431.
 

Deep resequencing identifies candidate functional genes in leprosy GWAS loci.
Fava V, Dallmann-Sauer M, Orlova M, et al. PLoS neglected tropical diseases. 2021; 15 (12) : e0010029.
 

Clinical progression of leprosy in Eurasian red squirrels (Sciurus vulgaris) in a naturally infected wild populations
Schilling A, van Hooij A, Lurz PW, et al. Journal of Zoo and Wildlife Medicine. American Association of Zoo Veterinarians. 2021.
 

Lepra Bubalorum, a Potential Reservoir of Mycobacterium leprae
Faber WR, Menke H, Rutten V, et al. Frontiers in Microbiology. Frontiers Media SA. 2021.
 

Laboratory diagnosis of leprosy: Two staining methods from bacilloscopy and rapid ml flow test
Paro Pedro HS, Ule Belotti N, Tonelli Nardi S, et al. International Journal of Mycobacteriology. Medknow. 2021; 10 (4) : 393.
 

Presentation on Capacity Development
Eggens H. info Hansen. 2021.
 

Quali-quantitative synthesis of the global scenario of patent families about leprosy.
Meneghin R. Ciencia & saude coletiva. 2021; 26 (11) : 5411-5426. 
 

Chronic recalcitrant erythema nodosum leprosum: therapeutic dilemma and role of mycobacterium indicus pranii vaccine.
Gupta S, Kumari S. Anais brasileiros de dermatologia. 2021.
 

Human macrophage polarization in the response to Mycobacterium leprae genomic DNA.
Marin A, Van Huss K, Corbett J, et al. Current research in microbial sciences. 2021.
 

Estudo de caso sobre os sintomas e a relação dos efeitos colaterais na desistência de pacientes durante o tratamento da hanseníase realizado em Palmas-TO
Sobrinho JDC, Melo ACCD, Pinto RR. Research, Society and Development. Research, Society and Development. 2021; 10 (14) : e483101422166. 
 

Epidemiological characteristics and trends of leprosy in children and adolescents under 15 years old in a low-endemic State in Southern Brazil.
de Moraes P, Eidt L, Koehler A, et al. Revista do Instituto de Medicina Tropical de Sao Paulo. 2021.
 

Modeling and Transmission Dynamics of Leprosy Disease: Via Numerical Methods
Raza A, Rafiq M. Iranian Journal of Science and Technology, Transactions A: Science. Springer Science and Business Media LLC. 2021.
 

The Profile of Type 1 Leprosy Reaction at Leprosy Division of Dermatology and Venerology Outpatient Clinic of Dr. Soetomo General Academic Hospital, Surabaya, Indonesia
Rosdiana BI, Astari L, Astindari A, et al. Berkala Ilmu Kesehatan Kulit dan Kelamin. Universitas Airlangga. 2021; 33 (3) : 168. 
 

Fatores associados ao tempo de ocorrência das reações hansênicas numa coorte de 2008 a 2016 em Rondônia, Região Amazônica, Brasil
Coriolano CRF, Freitas Neto WAD, Penna GO, et al. Cadernos de Saúde Pública. FapUNIFESP (SciELO). 2021.
 

Social school contacts of multibacillary leprosy cases in children living in the hyperendemic region of the Midwest of Brazil.
Sato C, Rodrigues T, Silva P, et al. Jornal de pediatria. 2021.
 

Assessment of Risks of Cardiovascular Diseases among Leprosy Patients Settlement at Ossiomo-Ogan Rehabilitation Center, Edo State, Nigeria
Umahi-Ottah G, Adejumo BIG, Oyakhilome LI, et al. Health. Scientific Research Publishing, Inc.. 2021; 13 (12) : 1475-1487.

 


A comparison of three types of targeted, community-based methods aimed at promoting early detection of new leprosy cases in rural parts of three endemic states in India.
Govindasamy K, John A, LAL V, et al. PloS one. 2021; 16 (12) : e0261219.
 

Leprosy and cutaneous leishmaniasis affecting the same individuals: A retrospective cohort analysis in a hyperendemic area in Brazil.
de Carvalho A, Tiwari A, Luz J, et al. PLoS neglected tropical diseases. Plos NTDs. 2021; 15 (12) : e0010035.
 

Lepromatous leprosy as a presenting feature of HIV.
Belgaumkar V, Chavan R, Deshmukh N, et al. Indian journal of sexually transmitted diseases and AIDS. 2021; 42 (2) : 162-165.
 

How do Positive Deviants Overcome Health-Related Stigma? An Exploration of Development of Positive Deviance Among People With Stigmatized Health Conditions in Indonesia.
Rai S, Syurina E, Peters R, et al. Qualitative health research. 2021.
 

The Demography, Clinical Characteristics, and White Blood Analysis of Leprosy Reactions in Multibacillary Leprosy: A Retrospective Study
Tanojo N, Damayanti D, Utomo B, et al. Berkala Ilmu Kesehatan Kulit dan Kelamin. Universitas Airlangga. 2021; 33 (3) : 187.
 

Diálogos sobre a descentralização do programa de controle da hanseníase em município endêmico: uma avaliação participativa
Corrêa CM, Lanza FM, Carvalho APM, et al. Escola Anna Nery. FapUNIFESP (SciELO). 2022.
 

Promotion of self-care for people with leprosy: educational intervention in the light of Orem's theory
Cavalcante JL, Silva KND, Barbosa RDS, et al. Revista Gaúcha de Enfermagem. FapUNIFESP (SciELO). 2021.
 

Ulnar Artery Perforator Adiposal Flap for Paraffinoma Treatment in a Patient With Leprosy: A Case Report
Morimoto Y, Sogabe Y, Kawabata A, et al. Journal of Hand Surgery Global Online. Elsevier BV. 2021.
 

Efficacy of autologous smashed follicular dermal graft and epidermal cell suspension in the treatment of chronic nonhealing trophic ulcers in Hansen's patients
Dheemant M, Yadalla H, Raju B. Indian Dermatology Online Journal. Medknow. 2021; 12 (6) : 868. 
 

A clinicoepidemiological study of psychiatric co-morbidity in Hansen's Disease
Verma G, Rani R, Tegta G, et al. Indian Dermatology Online Journal. Medknow. 2021; 12 (6) : 847.
 

Dramatic secukinumab-mediated improvements in refractory leprosy-related neuritis via the modulation of T helper 1 (Th1) and T helper 17 (Th17) immune pathways
Kurizky PS, Motta JDOCD, Bezerra NVF, et al. Revista da Sociedade Brasileira de Medicina Tropical. FapUNIFESP (SciELO). 2021.
 

Patterns of leprosy at Chris Hani Baragwanath Academic Hospital, Johannesburg, South Africa, and review of current clinical practice.
Nkehli L, Menezes C, Tsitsi J. South African medical journal. 2021; 111 (9) : 879-885. 
 

Perfil sociodemográfico e avaliação neurofuncional de mulheres no pós-alta de hanseníase
Lima ABDA, Tavares CM, Santos TSD, et al. Research, Society and Development. Research, Society and Development. 2021; 10 (16) : e110101623020.
 

O desenvolvimento de um dispositivo de tecnologia assistiva/ortoprótese para a reabilitação de pacientes com hanseníase e presença de mão em garra e/ou reabsorção óssea
Rodrigues Júnior JL, Santos Júnior HCFD, Silva ECD, et al. Research, Society and Development. Research, Society and Development. 2021; 10 (16) : e449101623742. 
 

A Comprehensive Rehabilitation of a known Case of Leprosy Operated for Midshaft Femur Fracture
Vaidya L, Bawiskar D, Upadhyay P, et al. Journal of Pharmaceutical Research International. Sciencedomain International. 2021.

 



 



 



Events

 



World Leprosy Day
30 Jan 2022

World Neglected Tropical Diseases Day
30 Jan 2022

Global disability summit
16-17 Feb 2022 | Virtual
 

Call for proposals
Leprosy Research Initiative
Deadline 28 January 2022
Click here for more info
 

 


ILEP Conference
14-16 Mar 2022 | Virtual
More info will follow soon

21st International Leprosy Congress
9-11 Nov 2022
Hyderabad & Virtual


 

Call for proposals
Sasakawa Health Foundation
Deadline 24 April 2022
Click here for more info

 



 



Links

 



Info Hansen - A innovative hub for knowledge sharing about Hansen's Disease
 

ALLF - Official website of the Association des Léprologues de Langue Française
 

LML - Leprosy Mailing List - a free moderated email list that allows all persons interested in leprosy to share ideas, information, experiences and questions
 

InfoNTD - Information on cross-cutting issues in Neglected Tropical Diseases (NTDs)

 


ILEP newsletter archive

GPZL newsletter archive

WHO Goodwill Ambassador's Leprosy Bulletin

Leprosy Review

Leprosy Review Repository (1928-2001)

Fontilles Revista de Leprología

Indian Journal of Leprosy

Hansenologia Internationalis

 




GDPR & the Infolep newsletter

 
New EU data protection regulations came into force on 25 May 2018. We have been reviewing our practices with regards to the GDPR, including our privacy statement and mailing list.

Infolep sends out monthly e-mails with an overview of recent publications on leprosy and related issues. The purpose of this activity is to keep subscribers up to date.

Infolep will only process the data we have (names, email addresses) for the purpose of sending you the newsletter. We take your security seriously and will never share your contact details with anyone else.

You can update your preferences or unsubscribe from this list at any time.

 


 



LML - S Deepak, B Naafs, S Noto and P Schreuder

LML blog link: http://leprosymailinglist.blogspot.it/

Contact: Dr Pieter Schreuder << editorlml@gmail.com

 

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Friday, January 7, 2022

Fw: Ref.: (LML) median nerve damage in leprosy


 
Leprosy Mailing List – January 7,  2022

 

Ref.:  (LML) median nerve damage in leprosy

 

From:  Salvatore Noto, Bergamo, Italy


Dear Pieter,

 

I would like to present a case of a leprosy patient treated with a six-month course of multi-drug therapy for paucibacillary leprosy. 


While I was visiting a clinic in a rural area, in West Africa, we saw a patient that had just completed his treatment course and was due for "release of treatment".  The local nurse noticed blood on the 2nd fingertip of his hand.  One picture is in attachment.  The picture also shows sequela of trauma to the 1st  finger and dry palm. 

The sequelae of "unnoticed" trauma on 1st and 2nd fingers are sign of advanced sensory damage of the median nerve. 


The patient had been rightly diagnosed of leprosy and treated with the WHO suggested multi-drug therapy and he was ready to be released from treatment but, diagnosis of neuritis of his median nerve and of loss of sensation of the median region of the hand had been missed.  Deformity was going on. 


I believe that in leprosy, like other diseases, clinical skills should be on the forefront.


Best regards,


Salvatore

S. Noto
Bergamo, Italy


LML - S Deepak, B Naafs, S Noto and P Schreuder

LML blog link: http://leprosymailinglist.blogspot.it/

Contact: Dr Pieter Schreuder << editorlml@gmail.com

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Tuesday, January 4, 2022

Fw: Ref.: (LML) Doing what works

 


Leprosy Mailing List – January 4,  2022

 

Ref.:  (LML) Doing what works

 

From:  Joel Almeida, London and Mumbai

 

Dear Pieter & colleagues,

 

It is helpful to understand how the world was mobilised against other diseases, and how stagnation was transformed into widespread effective action. 

 

In TB, the 1980s saw the declaration of victory. It was a mistaken declaration. The real battle was yet to begin. Bactericidal regimens had been defined through clinical trials and some projects used them to achieve consistent "sputum conversion" (from bacillated to non-bacillated). These successful projects were the exceptions. The rest of the world continued to drag its feet. Most endemic countries used ineffective interventions. One or two of those countries even declared that TB was no longer a problem. It emerged later that many of their citizens were being killed by TB year after year.

 

When we (WHO team) tried to introduce a more effective intervention into Bangladesh, it was derided as a "Sheraton program". That is, fancy but unworkable methods fit only for discussion in five-star hotels by well-fed people who did not understand the realities of life. Only when pilot projects demonstrated consistent sputum conversion, instead of the usual 50% conversion or worse, were the sceptics somewhat shaken. Some local organisations adopted the more effective interventions and even tweaked them. Illiterate village women were allocated the central task of ensuring regular ingestion of drugs. These illiterate women produced the world's best outcomes in TB (matched only in China and Vietnam). 

 

We compared the outcomes from various countries across the globe, and identified the key ingredient for consistent success. This was the action taken when a dose was missed. Wherever swift follow-up was done after a missed dose, with resulting ingestion of the missed dose, sputum conversion approached 100% (well over 90%). In nearly every other circumstance, sputum conversion fell away to the sub-50% to 80% level. This critical ingredient (or the absence of it) continues to influence outcomes today.

 

I visited these village women in Bangladesh and asked them what happened when a patient under their supervision missed a dose. One of them told me, "He comes regularly at about 8am. If he doesn't come by 8:30 am, I find him and scold him severely." That's how near-100% sputum conversion was being achieved. Nowhere else was follow-up so prompt, within only half an hour. Decades of research had gone into identifying the potent molecules, but the magic at the front line was indispensable. The same woman explained, "I tell my villagers that if they start coughing and go to the doctors in the town, they will die. If they come to me, they will live." This was, roughly, true. Without prompt follow-up for missed doses, even people who started treatment were dying of TB.

 

That strategy, labelled the DOTS strategy, was introduced in one country after another with the help of highly successful pilot projects. The sceptics found it increasingly difficult to resist. (Incidentally, the DOTS strategy included more than just supervision and follow-up for missed doses. It includes generation of political commitment, uninterrupted drug supplies, quality-controlled microscopy and a reliable recording & reporting system). 

 

TB was once a neglected disease, because victory had been declared prematurely and mistakenly. As the DOTS strategy started producing good outcomes, TB control moved higher up in the world's agenda. TB research too got a boost. Now TB work is an important global priority, with all sections of society being roped in to fight TB. Successful projects are the key to mobilising the world for effective action. Successful pilot projects create oases of success. These oases open our eyes to a vision of a transformed world, where gardens replace deserts.

 

Did the world know everything there was to know about the TB bacillus and its epidemiology? No. We continue to learn. Did that stop the DOTS strategy from saving lives? No. There will always be room for further knowledge. However, that is not a good reason for dragging one's feet. Austin Bradford-Hill wrote, wisely: "All scientific work is incomplete - whether it be observational or experimental. All scientific work is liable to be upset or modified by advancing knowledge. That does not confer upon us a freedom to ignore the knowledge we already have or postpone the action that it appears to demand at a given time." We drive cars without knowing what is under the bonnet. The car works if we know only how to find the starter key, steering, brakes, gear stick and accelerator. We plug holes in dams without fully understanding the routes by which towns were flooded. We do that because it works. More knowledge is always desirable, of course. It can enable breakthroughs. But effective action does not depend on having perfect knowledge.

 

 

HD

 

In HD (leprosy), we know that victory is in the future and not in the past. There are millions living with the sequelae of HD, and those with polar LL (lepromatous) HD in endemic areas are at risk of reinfection. Reinfection converts previously treated but genomically anergic LL HD patients into factories for astronomical numbers of viable bacilli. Recurrent LL HD often goes undiagnosed for years, because the signs are masked by sequelae of previous infection, and annual skin smears are rarely done. This allows HD bacilli to keep spreading to children and others even in well-run programs where active case-finding has been practised for years. Bacilli do not care how they find a new home. They will spread through the nose, through the skin, through the soil, through all channels available to them. 

 

The main thing is that we can stop transmission at source. We can achieve this by prompt diagnosis and prolonged anti-microbial protection of LL HD patients in endemic areas. Then LL HD patients no longer can keep replenishing the environment with bacilli. LL HD patients are uniquely important because careful studies revealed that the nasal discharges of even BL (borderline lepromatous) HD patients did not contain such astronomical numbers of bacilli, whether before or after anti-microbial protection. When LL HD patients were granted prolonged anti-microbial protection, a demonstrable16% to 20% annual decline in the incidence rate of MB HD was achieved even in places that had low incomes at that time (e.g., Uele/DRC, Karigiri/India, Weifang/Shandong/China). Careful surveys demonstrated that these were real declines in incidence rate, not just artefacts of case-finding methods.

 

Transmission continues in even well-run programmes because we are late in diagnosing LL HD patients and hasty in withdrawing anti-microbial protection.

 

Further, if MDT is withdrawn at 12 months from LL HD patients instead of being continued, these patients suffer a 600% increase in the risk of ENL neuritis during months 13 to 24 (as discussed here previously). ENL neuritis is an excruciatingly painful condition that drives many LL HD patients to the verge of suicide. It is not in the patients' best interests for us to allow a 600% increase in the risk of ENL neuritis.

 

Instead of championing anti-microbial neglect of LL HD patients in endemic areas, we could champion prolonged anti-microbial protection for them. That would be not only humane and ethical but also transform our epidemiological impact.

 

 

What works in HD? 

 

What is the equivalent of the DOTS strategy in TB? The DOTS strategy had 5 points. The corresponding strategy in HD would appear to have 4 points. It is even more effective than the DOTS strategy in TB, because the HD strategy produced rapid and measurable epidemiological impact..

1) Expert skin camps to ensure that LL HD patients with only subtle signs are diagnosed promptly. Wherever local expertise is scarce, telemedicine allows experts to participate. They can instruct frontline staff how to pinch skin, examine ears & eyebrows etc. Otherwise, we keep diagnosing all types of HD except LL HD, the most highly bacillated and infectious type. Smear microscopy reveals the astronomical numbers of bacilli in nasal discharges (or skin fluid) of unprotected LL HD patients. 

 

In places where finance and technicians are available, further tests can be used. They reveal that up to 50% of randomly selected school children in endemic areas have IgM antibodies to phenolic glycolipid-1, an antigen specific to HD bacilli. Such further tests are not a substitute for smear microscopy, however. Microscopy uniquely allows direct visualization of the astronomical numbers of bacilli present in nasal discharges (or skin fluid) of unprotected LL HD patients. The key distinction to be made is between LL HD and non-LL HD. Then appropriate case management of LL HD becomes possible.

 

 

2) Prolonged anti-microbial protection for anergic LL (lepromatous) HD patients. MDT followed by post-MDT chemoprophylaxis in LL HD patients is used in centres of excellence in endemic countries including India and Brazil. Destitute LL HD patients who cannot afford combinations of bactericidal drugs would have to rely on prolonged free-of-charge MDT. We know that about 17% of previously treated homeless and destitute patients in two south Indian towns had bacilli in skin smears. There is no reason to keep offering genomically anergic LL HD patients as fodder for the bacilli in endemic areas.

 

There are options for post-MDT chemoprophylaxis with combinations of bactericidal drugs. Monthly ROM (rifampicin + ofloxacin + minocycline) was demonstrated to be roughly as effective as MDT. Monthly rifampicin + moxifloxacin + minocycline (RiMoMi) is likely to be even more effective than monthly ROM because moxifloxacin is more bactericidal than ofloxacin. Where finances permit, daily regimens can replace monthly regimens to maximise the area under the curve (AUC) of drug concentration over time. This AUC generally is correlated with the bactericidal effect of drugs, and increasing it helps to eliminate endogenous mycobacteria (as observed in TB). Even when highly bactericidal daily and high-dose regimens are used, however, prolonged anti-microbial protection for anergic LL HD patients remains important. That is because sources of infection in endemic areas can keep reinfecting genomically anergic LL HD patients. 

 

Those LL HD patients who do not have genomically related anergy and "de novo" LL HD but instead "downgraded" from inadequately treated BL HD tend to respond well to MIP vaccine (Mycobacterium w vaccine) Typically, about 70% of LL HD patients in India respond well to MIP vaccine, as demonstrable by accelerated clearance of bacilli from skin and conversion of lepromin status. The remaining 30% of LL HD patients may be taken to have genomically related anergy. Even where MIP vaccine is used, this 30% of LL HD patients is capable of shedding astronomical numbers of bacilli and suffering excruciating ENL episodes if anti-microbial protection is withdrawn.

 

Where smear microscopy is unavailable, patients in need of monthly post-MDT chemoprophylaxis (and/or MIP vaccine) can be identified by widely distributed, bilaterally symmetrical signs. This is not as specific as measuring the BI (bacillary index) under the microscope. However, it is good enough to protect nearly all genomically anergic patients against reinfection. Otherwise, transmission continues even in well-run programmes because of undiagnosed or belatedly diagnosed recurrent LL HD.

 

 

These 2 points above (expert skin camps and prolonged anti-microbial protection for anergic LL (lepromatous) HD patients) can yield a 16 to 20% annual decline in new MB (multibacillary) HD cases as observed in Karigiri (India) and Weifang/Shandong (China). Such declines probably occurred elsewhere too, wherever LL HD patients were protected against reinfection by allowing them prolonged anti-microbial protection. 16% to 20% annual decline is better than the sub-10% decline achieved in Norway or the sub-7% decline being achieved in Yunnan (China) with 24 months of MDT (despite vast increases in income since the 1990s) or the sub-3% decline being achieved globally. It is much better than the near-zero decline of new HD cases observed in the Indonesian LPEP projects that for several years supplemented 12 months of MDT with single dose rifampicin among contacts of newly diagnosed HD patients.

 

 

3) In high endemic hot spots in addition to points 1) and 2), add the following

 

Mass multi-drug administration (e.g., ROM) at intervals of less than a year. Repeat until no child case is found for a few years. This was used alongside points 1) and 2) above in FS Micronesia with remarkable success. It achieved a decline of about 40%/year in new HD cases. Unfortunately, the intervention was discontinued after only two annual rounds of mass multi-drug administration, and prolonged MDT was replaced by only 12 months of MDT. 


Which high endemic hot spots could be first in the queue for exemplary projects? Former HD "colonies" are prime candidates for mass multi-drug administration alongside expert skin camps and prolonged anti-microbial protection for LL HD patients. For example, Vila Santo Antonio do Prata in Para, Brazil, showed enrichment of genetic risk factors among the residents. Former HD colonies can rapidly become transmission-free zones. They can be the oases of success that demonstrate how the desert of stagnation can be transformed. Persons affected by HD, in partnership with expert clinicians, and supported by philanthropic organizations, can lead the way out of epidemiological stagnation. 

 

 

4) Political commitment, generated on the basis of rapid decline in new MB cases resulting from points 1), 2) and 3) above. Successful projects are the best answer to scepticism. No politician can resist success. 

 

(If I may be pardoned a personal story relating to TB, President Clinton visited only one health project in the course of an official visit to India. This was to a Public-Private Mix project in Hyderabad that I had designed and supervised. It was implemented by local professionals who I had trained during a field visit to the illiterate village women in Bangladesh. The outcomes in the project had been transformed from 56% sputum conversion to consistent 100% sputum conversion, with the participation of private practitioners, then an unprecedented step. The President's visit helped change the world's perception of TB and of Public-Private mixes. Successful projects are magnets for political commitment. Real political commitment yields adequate financing).

 

The fifth point in HD is not part of the strategy. It consists of delaying drug resistance. Avoiding the use of single drugs (e.g., avoiding single dose rifampicin) is very important to delay drug resistance and keep MDT effective. Mass multi-drug administration of ROM enabled a 40%/year decline in new HD cases without rapid selection of rifampicin-resistant mutant bacilli. Regressing to the use of single drugs seems unduly reckless because multiple drugs delay drug resistance while single drugs select drug resistant mutants.

 

2022 is a turning point. We can progress rapidly with booster rockets attached, in the shape of the four points above (the "HD strategy" that works). There is no reason to remain trapped in epidemiological stagnation, selection of rifampicin-resistant bacilli in undiagnosed LL HD contacts, and increased risk of ENL neuritis. Those adverse outcomes accompany SDR-PEP for contacts and fixed duration MDT for LL HD patients. That does not work. Success seems preferable to stagnation.

 

We are a community of integrity, justice, compassion and science. In 2022 we can be a community of highly effective action, steadily creating oases (successful projects) that keep transforming the desert of stagnation into a garden of epidemiological impact. Step by step, other areas & countries will join in. Eventually, the whole world will cheer us on & assist this noble effort. 

 

1) Expert skin camps for prompt diagnosis 

especially of LL HD patients (highly bacillated) with new or recurrent HD


2) Uninterrupted MDT for all patients plus prolonged anti-microbial protection for LL HD patients in endemic areas 


3) In high endemic hot spots (e.g., former "HD colonies) mass multi-drug administration (e.g., ROM) at intervals of less than a year

 

4) Generate political commitment & adequate financing based in part on genuine decline in new MB cases

 

Alongside this, we can monitor nerve function especially in MB HD patients & intervene promptly with prednisolone when needed, boost respect for the inalienable dignity of every human being, replace public misinformation & fear with facts & understanding, help persons affected to advance socio-economically & cope with distress, promote inclusion & respect.

 

This is the future we care about. This is the world we want to create. It is great work, worth doing..

 

Happy New Year to all.

 

Best,

 

Joel Almeida

 

 

LML - S Deepak, B Naafs, S Noto and P Schreuder

LML blog link: http://leprosymailinglist.blogspot.it/

Contact: Dr Pieter Schreuder << editorlml@gmail.com

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