Helminthic therapy and aging

Hosting helminths could be key to living longer with greater freedom from chronic disease.

The scientific evidence[edit | edit source]

• 2021 Feb 2 Gross ways to live long: Parasitic worms as an anti-inflammaging therapy? -- Full text | PDF (Also reported by Press Release. [1])

Theoretically, helminths could counter inflammaging in several ways. For example, they could inhibit sources of inflammaging by preventing gut barrier permeabilization and obesity, neutralize existing inflammaging by increasing the proportion of anti-inflammatory to pro-inflammatory cytokines, or repair inflammaging-afflicted tissue damage, for example through promotion of IL-22 secretion

• 2023 Nov 23 Protection against lung pathology during obesity-accelerated ageing in mice by the parasitic worm product ES-62
• 2021 Jan 13 Parasite Presence Induces Gene Expression Changes in an Ant Host Related to Immunity and Longevity
• 2020 Mar 12 The parasitic worm product ES-62 promotes health- and life-span in a high calorie diet-accelerated mouse model of ageing -- Full text

This study was the first of its kind to report that weekly administration of the helminth-derived product, ES-62, improved late-life health and increased lifespan (+12%, median lifespan) in a mouse model of high-calorie diet-accelerated aging. This suggests that the anti-inflammatory effects of helminthic therapy can exert protective effects even in later life.

• 2018 Dec Early life infection and host senescence
• 2015 Apr Impairment of host resistance to helminthes with age in murine small intestine

See also

• 2025 Aug Nonuniversality of inflammaging across human populations
• 2025 Jun 26 Recent Advances in Aging-Related Diseases: Accelerated Aging, Molecular Mechanisms, Interventions, and Therapies -- Full text
• 2025 May 15 An evolutionary medicine and life history perspective on aging and disease: Trade-offs, hyperfunction, and mismatch
• 2024 Sep 11 IL-10 deficiency aggravates cell senescence and accelerates BLM-induced pulmonary fibrosis in aged mice via PTEN/AKT/ERK pathway
• 2020 Aug Eosinophils and White Fat: Protection from Worms and Inflammaging

Lipopolysaccharide (LPS)[edit | edit source]

Lipopolysaccharide (LPS), now more commonly known as endotoxin, is a collective term for components of the outermost membrane of the cell envelope of gram-negative bacteria, such as E. coli and Salmonella with a common structural architecture.

Excessive LPS in the blood, endotoxemia, may cause a highly lethal form of sepsis known as endotoxic septic shock. Recent research indicates that even small LPS exposure is associated with autoimmune diseases and allergies. High levels of LPS in the blood can lead to metabolic syndrome, increasing the risk of conditions like diabetes, heart disease and liver problems.

LPS binds Toll like receptor 4 (TLR-4) which is present in various organs and activates an inflammation process.

Helminths can act in 4 different ways:

• reduce the gram-negative bacteria in the microbiota
• fix leaky gut
• maybe send peptides that prevent interaction with the toll-like receptor (TLR) 4/MD2/CD14 complex [2]. (This is yet to be confirmed with therapeutic helminths.)
• the immunomodulatory effect

See

• Mechanisms underlying helminth colonization. Search with keywords and see sections: Toll-like receptor (TLR) and Myd88 pathways, Lipopolysaccharide (LPS) and Antagonist of TLR3 and TLR4 signaling pathway
• Helminthic therapy and sepsis

Other mechanisms[edit | edit source]

• 2025 Aug 26 Aging impairs type 2 immune responses to nematodes associated with reduced gut microbiota responsiveness
• 2022 Jun Age-dependent rise in IFN-γ competence undermines effective type 2 responses to nematode infection
• 2020 Apr 6 Activation of group 2 innate lymphoid cells alleviates aging-associated cognitive decline -- Full text | PDF
• 2015 Dec 3 Adiponectin/adiponectin receptor in disease and aging -- Full text | PDF
• 2011 Apr 15 Impaired basophil induction leads to an age-dependent innate defect in type 2 immunity during helminth infection in mice
• 2011 Apr Th2 immune responses and alternatively activated macrophages (AAMacs) in helminth infection in aged mice

see also Mechanisms underlying helminth colonization - Adiponectin

See also (Not directly related)

• 2026 Feb Minimal Evidence of Inflammaging in Naturalistic Chimpanzee Populations
• 2021 Exploring the potential contribution of inflammation to altered pain behavior in the aging mice (Master, McGill)
• 2019 Sep 20 Implication of the receptor for advanced glycation end-products (RAGE) during inflammation and ageing -- PDF

see Mechanisms underlying helminth colonization - RAGE signaling pathway

The anecdotal evidence[edit | edit source]

I’m a year into NA treatment. And I truly appear to be physically aging backwards. I barely recognize myself in pictures from a year ago… my skin, hair, and nails have changed. I’m more well nourished & my outside reflects that.” [3] [4]

At sixteen years since (my hookworm story) began, I continue to maintain my hookworm colony and I’m still enjoying the benefits reported (in this article). However, now that I’m close to entering my ninth decade of life, age is beginning to take its toll. I’m no longer as sprightly as I once was, and the acuity of some of my senses is diminishing somewhat. Nevertheless, I can still eat everything I want to, and my Crohn’s disease, allergies, sinusitis, chemical sensitivity and Restless Legs Syndrome are all still in remission. [5]

Age-related diseases[edit | edit source]

Age-related macular degeneration (AMD)[edit | edit source]

See Helminthic therapy and vision: Age-related macular degeneration (AMD)

Benign prostatic hyperplasia[edit | edit source]

See Helminthic therapy and urologic disease: Benign prostatic hyperplasia

Neurodegenerative diseases[edit | edit source]

See Helminthic therapy and neurodegenerative diseases

Osteoarthritis[edit | edit source]

See Helminthic therapy and osteoarthritis

Osteoporosis[edit | edit source]

See Helminthic therapy and osteoporosis

See also[edit | edit source]

• Helminthic therapy and sepsis