The benefits of natural supplementation in medicine has stimulated the development of functional and integrative dermatology.1 Inositol (Ins) is a family of naturally occurring cyclohexanehexol (myo-, scyllo-, muco-, neo-, and D-chiro-Inositol) and its derivatives (L-chiro-, allo-, epi-, cis-Inositol) that has received much interest.2 Myo-inositol (MI) and D-chiro-Inositol (DCI) have been shown to improve insulin resistance and decrease total testosterone, granting their utility in patients with polycystic ovarian syndrome (PCOS) and hyperandrogenism.3–5
Over the past years, MI was used for the treatment of metabolic syndrome, reproductive diseases, and pregnancy development. Given the intricate link of skin health to hormones and metabolism,6 this systematic review will explore the potential roles of Ins in skin diseases, including acne vulgaris, hirsutism, psoriasis, seborrheic dermatitis (SD), hidradenitis suppurativa (HS), trichotillomania, and melanoma.
This study was performed in accordance to the Preferred Reporting Items for Systematic Reviews and Meta-Analyses (PRISMA).7 A primary literature search was conducted with MEDLINE, EMBASE, and Cochrane Library databases on December 20, 2021, with no limitation on date. The search terms included: (“Acne Vulgaris” OR “Acne” OR “Dermatitis” OR “Skin Diseases” OR “Skin” OR “Skin Physiological Phenomena” OR “Skin Abnormalities” OR “Dermatology” OR “Cutaneous”) AND (“Myo-inositol” OR Inositol). The full list of the search terms is available in online supplementary materials (
Two reviewers (T.L and Y.C) independently screened all articles to include clinical trials and case series written in English or Chinese on Ins and skin disorders. Any discrepancies were resolved with a third reviewer (F.C). Animal studies, reviews, and those not discussing skin diseases were excluded. Additional studies meeting the criteria were identified from references and included if the above-mentioned criteria were met.
Quality of evidence was determined per the Oxford Centre for Evidence-Based Medicine 2011 Levels of Evidence.8 The Cochrane Risk of Bias tool was used for randomized controlled trials (RCTs),9 the Risk of Bias in Non-randomized Studies of Interventions was used for non-RCTs,10 and the National Institute of Health quality assessment tool was used for case reports and case series.11
The initial search identified 1,181 records non-duplicate articles from the database. A total of 282 studies met the inclusion criteria. After full-text review, 13 studies including 6 randomized controlled trials (RCTs),12–17 five non-RCTs,18–22 one case series,23 and one case report24 were included in this systematic review (Figure 1).
Oral Ins as a treatment for acne has been described in four clinical trials (total n = 204) and one study using topical MI (n = 40). In a study by Fruzzetti et al, 38% of PCOS females who consumed 4 g MI plus 400 mcg folic acid daily reported improvement in acne symptoms.12 Although these PCOS women had a higher average testosterone level, Ins did not consistently affect patients’ androgen levels. Advani et al assessed the effect of twice daily oral combined 600 mg Ins (MI+DCI) on 51 PCOS women with normal (≤23) or high (>23) body mass index (BMI).18 They revealed a larger decrease in acne scores in overweight or obese subjects compared to lean individuals (-10.05 vs -4.38), although both groups achieved significant acne clearance within a 12-week treatment course. Another study assessing 2 g Ins twice daily in 50 PCOS women found decreased numbers of papulopustular lesions.13 Ramanan et al conducted a trial on 32 females with mild-to-moderate acne and hirsutism but no comorbid endocrine and metabolic diseases.20 Their result revealed a significant reduction of the modified Cook’s acne scale from 4.34±0.33 to 1.3±0.17 after 24 weeks of twice daily 2 g MI. Lastly, Fabbrocini et al tested topical Ins on 40 women with adult female acne.22 Participants were instructed to apply 4% MI peel-off mask every other night for 2 months. The study reported a 45-69% reduction in mean acne counts.22
We identified three clinical trials on hirsute women with or without PCOS using oral Ins (n = 129). Minozzi et al prescribed 2 g MI twice daily for 6 months to 46 women with mild to moderate hirsutism and found a significant decrease in hirsutism scores (-2.3±0.9,
The use of Ins in psoriasis has been reported in two randomized controlled trials (n = 69). Allan et al published a study on 23 patients with concomitant plaque psoriasis and bipolar disorder using the oral preparation of 6 g Ins daily for 2.5 months.16 Improvement of psoriasis, as measured by Psoriasis Area and Severity Index score (PASI), was seen in the subgroup of patients taking lithium but not in the other non-lithium treated subgroup. There was no difference in treatment of bipolar disorder appreciated in patients with use of Ins. Another study by Owczarczyk-Saczonek et al investigated topical 0.25% and 1% DCI for the treatment of chronic plaque psoriasis on 46 patients and showed subjective and clinical improvement of psoriasis as measured with PASI.14 In addition, the high-dose group showed improvement objective measurement of transepidermal water loss while patients in the low-dose group achieved better clinical outcomes seen in PASI improvement.
A topical gel containing glycerol-phospho-Inositol (GPI) was tested on 25 patients with mild-to-moderate facial SD in an uncontrolled clinical trial.19 They demonstrated a significant reduction in the investigator’s global assessment scale and an excellent response with more than 80% improvement reported in nearly 50% of the cases. However, it was unclear whether the effect was due to GPI or other ingredients in the product. More studies are required to further look at topical inositol as a potential treatment for seborrheic dermatitis.
Donnarumma et al evaluated the effectiveness of additional oral MI (2 g daily) in 20 hidradenitis suppurativa (HS) patients taking concurrent antimicrobials.15 The study reported a significant reduction of the Sartorious Score in the dual therapy group from 38.3±7.75 to 27.3±8.02 (
Two studies using Ins in patients with psychodermatoses (n = 22) were identified. Seedat et al, reported successful treatment of refractory trichotillomania and compulsive skin picking with Ins in 3 cases using daily dose of 18 g/d administered in white powder form.23 The other study was a randomized controlled trial assessing 19 patients with trichotillomania.17 In this study, 42.1% of the 19 patients reported “much or very much improved” with oral Ins 6 to 18 g/day, while 35.3% of the 19 patients on placebo reporting clinical improvement. These studies did not show statistically significant effects of Ins therapy (
Khurana et al reported a stage IV melanoma patient who had preferred treatment with inositol hexaphosphate (IP6) plus MI (800 mg/220 mg) over standard of care treatment.24 The patient received a total dose of 8 g IP6 and 2.2 g Ins daily for 2 years and when complete, clinical and radiological remission was achieved and no relevant side effects reported. However, this is the only case report reported in the literature.
Inositol is a polyol widely distributed in animal and plant cells as phosphorylated derivates and in cell membranes and serves as a fundamental component for cellular membranes and intracellular messengers.16 Inositol’s function in cellular signaling transduction is postulated to be insulin-like in quality,22 and comprising a major role in cellular growth and survival, metabolic regulation, nerve functionality, and reproductive activity.5 Due to its ubiquitous nature, the average human consumes one gram per day of Ins. It also is available without prescription as an oral nutritional supplement but can also be used in topical forms.3,16
Through this systematic review, we have provided quantitative estimates of the efficacy of Ins as adjunctive treatment for various dermatologic pathologies with inflammatory, psychiatric, and neoplastic etiologies. The wide breadth of pathologies highlighted in this review suggest the diverse roles that inositol possibly plays as a cell signal transducer.
Inositol is known to have positive systemic effects consistently found on reproductive disturbance and insulin resistance in populations with PCOS.5 This androgen-lowering property of Ins was investigated as a possible adjunct to acne and hirsutism topical therapy, as acne arises from the interplay between sebaceous glands, skin flora, and androgenic hormones.25 Like most current regimens, effect of Ins on acne may involve multiple mechanisms other than hormonal regulation, including anti-inflammatory effects.26,27 Hirsutism is characterized by excessive male-pattern hair growth in women. Like acne, hirsutism can also be hormonal or idiopathic.25 Ins may improve PCOS-related hirsutism in the same fashion as PCOS-related acne. Two out of three studies investigated hirsutism in non-PCOS women. Thus, synergistic hormonal balance and inflammatory cytokine down-regulation could have contributed to the improvement in either type of hirsutism. Overall, topical Ins may be considered as an adjunctive treatment in acne and hirsute women with PCOS or non-PCOS-related due to its promising reported efficacy and safety profile.
Psoriasis is characterized partly by an overproduction of TNF-α, a key inflammatory cytokine underlying the formation of skin and joint lesions.28 Studies have reported some anti-inflammatory and antioxidant properties of MI and DCI.27 In particular, TNF-α was found significantly suppressed by pinitol, a methylated form of DCI.26 Despite these plausible mechanisms, the role of Ins in psoriasis requires further elucidation. Different responses between the two groups in the study reported by Allan et al’s16 the authors suggested that endogenous Ins, which is inhibited by lithium, may be a sufficient but not necessary molecule for psoriasis pathogenesis.29 Therefore, the efficacy of Ins may depend on patient characteristics and route of administration, more research is warranted to identify possible underlying mechanism.
SD is a common multifactorial inflammatory skin condition associated with aberrant hormone levels, skin flora composition, fatty acid metabolism, and neurogenic factors.30 Recently,
HS is a relapsing-remitting inflammatory dermatosis characterized by painful nodules, abscesses, and sinus tract formation.32 Interactions between innate immunity and skin microbiota, and genetic factors have all been linked to the development of HS.33 The inflammatory cytokines at play are very similar to psoriasis, including TNF-α, IL-17, and IL-23.34 Therefore, a detailed understanding of its pharmacodynamics may shed light on the possible roles of Ins in treating both conditions.
MI regenerates hydrolyzed phosphoinositides (PI), the first messenger in multiple neurotransmitter pathways, making it an emerging therapeutic treatment for psychiatric disorders.35 Trichotillomania, characterized by repetitive hair pulling leading to hair loss, is not uncommonly seen in this population. Although selective serotonin reuptake inhibitors were proposed to treat comorbid skin diseases, concerns about worsening psychological stability have limited their use. More studies are required to improve the understanding on the relationship between psychodermatology disorders with inositol.
MI and its derivative IP6 have been demonstrated to be involved in a wide range of physiological and pathological settings, including cell cycle progression, apoptosis, and differentiation.36 Ins inhibits RB protein phosphorylation, preventing cell cycle progression through the RB/E2F pathway. It was also proposed that MI significantly reduces PI3K/Akt pathway activity.37 Downstream inhibition of molecular pathways supporting epithelial-mesenchymal transition prohibits possible transformation of cells into aggressive carcinomas.38 Ins has been shown to inhibit the proliferation of other types of cancer in vitro, including breast cancer, colon cancer, and lung cancer. However, its efficacy for melanoma requires further investigation.
There are wide variety of isoforms, dosing, and treatment duration employed among the included studies. Out of a total of 371 patients included in this study, mild gastrointestinal distress was reported in 11 patients, and headaches were reported in 3 patients. None of the adverse events were severe and they usually wore off with continual use. However, Seedat et al,23 reported that psychiatric patients are more prone to neurological side effects.
Integrative treatment for dermatology is on the rise. Our study highlighted the existing utilities of Ins in acne and hirsutism. Limited studies were available to demonstrate utility in dermatoses such as SD, HS, psoriasis, trichotillomania, and melanoma, which highlights the need for future well-designed clinical studies on alternative and adjunctive treatments are required to provide additional evidence to the field.
Significantly reduced mean count of comedones (-3.9), papule (-6.1), pustule (-2.0), and nodular (-0.5) lesion (P<0.001) Global acne grading score reduced from 16.8±5.3 to 9.8±4.6 (P<0.001) Sabotage score decreased from 3.4±0.6 to 1.8±0.2 (P<0.001) Patient-self assessment, 20% felt a slight improvement in hirsutism, the remaining reported no change 38% felt a slight improvement in acne, 12% reported worsening, the remaining reported no change In the obese and lean group, Acne score scores -10.05 (P<0.001) and -4.38 (P<0.01), respectively Hirsutism score scores -0.45 (P<0.01) and -0.25 (P<0.05), respectively GA scores reduced from 4.34±0.33 to 1.3±0.14 by Weeks 24 Modified Ferriman-Gallwey hirsutism score reduced to 8.6, 7.4, and 5.8 by Weeks 4, 12, and 24, respectively Patients on lithium: PASI scores -1.7 in the inositol group compared to +1.9 in the placebo group (P>0.05) Patients not on lithium: PASI scores +0.7 in the inositol group compared to -0.75 in the placebo group (P=0.015) Excellent response (IGA = 4) in 47.9% of patients and no case of worsening (IGA = 0) Significant reduction in desquamation, erythema, and pruritus (P<0.001) Visual analogue scale reduced by 22% and 33% in the B and C group; and 23% in the placebo group (P<0.05) Plaque severity index reduced by 30% and 45% in the B and C group; and 28% in the placebo group (P<0.05) Abbreviations: AE: adverse event; FU: follow-up; PCOS: polycystic ovarian syndrome; MI: myo-Inositol; DCI: d-chiro-Inositol; QD: once daily; BID: twice daily; TH: trehalose; TIW: thrice weekly; PASI: psoriasis area and severity index; TID: thrice daily; GID: gastrointestinal disturbance; CGI-I: clinical global impressions-improvement scale; IGA: investigator global assessment; SD: seborrheic dermatitis; GPI: glycero-phospho-Inositol; IP6: inositol-6 phosphate; HS: hidradenitis suppurativa; LOE: level of evidence; SRI: serotonin reuptake inhibitor; Hexopal : inositol nicotinate. *Obese/overweight: BMI >23; non-obese/lean: BMI ≤23.
Hyperandrogenism – acne, hirsutism
Pezza et al,13 2015
RCT, 1b
50 PCOS women with acne
Inositol, 2 g, BID
Oral
Decreased number of papulopustular lesions
None
6
Fabbrocini et al,22 2017
Uncontrolled clinical trial, 2b
40 women with adult female acne
4% MI and 1% trehalose-loaded liposomes, overnight every other day
Peel-off facial mask
None
2
Fruzzetti et al,12 2017
RCT, 1b
25 PCOS women
MI, 4 g, QD plus folic acid, 400 mcg, QD
Oral
None
6
Minozzi et al,21 2008
Uncontrolled clinical trial, 2b
46 women with mild to moderate hirsutism
MI, 2 g, BID
Oral
Hirsutism score decreased by -2.3±0.9 (P<0.001)
None
6
Advani et al,18 2020
Controlled clinical trial, 2b
Obese (35) or lean (16) PCOS women*
Trazer F Forte, BID: Inositol (MI:DCI) 600 mg, NAC 300 mg, Biotin 5 mg, 10%
Oral tablet
None
3
Ramanan et al,20 2020
Uncontrolled clinical trial, 2b
32 females with mild-to-moderate acne and hirsutism
Tracnil, BID: MI, 2 g; folic acid 1 mg, vit D3 1000 IU
Oral powder sachets
Mild GID in some patients
6
Inflammatory dermatosis – seborrheic dermatitis, hidradenitis suppurativa, psoriasis
Allan et al,16 2004
Crossover RCT, 1b
Patients on lithium who developed chronic plaque psoriasis (15) or patients not on lithium with psoriasis (8)
Inositol, 6 g, QD
Oral
None
2.5
Dall’ Oglio et al,19 2017
Uncontrolled clinical trial, 2b
25 patients with mild-to-moderate SD
GPI, piroctone olamine, lactoferrin, and Aloe vera, BID
Topical gel
None
1.5
Donnarumma et al,15 2020
RCT, 1b
10 patients with HS
Antibiotics with MI 2 g, liposomal magnesium and folic acid, BID
Oral
Reduction of Sartorius scores from 38.3±7.5 to 27.3±13.53 (P<0.04)
None
6
Owczarczyk-Saczonek et al,14 2021
RCT, 1b
46 patients with mild plaque psoriasis (PASI<10, BSA<10%)
1% (B) or 0.25% (C) DCI, 1 fingertip unit, BID, or placebo applied to three different psoriatic plaques
Topical cream
Not reported
1.5
Psychodermatoses – skin picking, trichotillomania
Seedat et al,23 2001
Case series, 4
3 patients with trichotillomania and compulsive skin picking
Inositol, 6 g, TID (primary treatment in two and adjunct to SRI in one)
Oral powder dissolved in water or juice
Two patients reported a CGI-I score of 2 (much improved), and 1 (adjunct to SRI) reported CGI-I of 1 (very much improved)
Mild GID (2) and headache (1)
2-3
Leppink et al,17 2017
RCT, 1b
19 patients with trichotillomania
Incrementing inositol from 6 to 12 to 18 g, QD, every 2 weeks for a total duration of 10 weeks
Oral powder
Patients were “much or very much improved”
Mild GID (9) and headache (2); one hospitalization due to ectopic pregnancy
2.5
Neoplasm
Khurana et al,24 2019
Case report
A patient with stage IVB melanoma
IP6+inositol (800 mg/220 mg), 5 tablets, BID
Oral tablets
Restaging scans showed significant improvement after 6 months, complete clinical and radiological remission after 2 years
None
24
Q1: Question/Objective Stated; Q2: Population Specified and Defined; Q3: Consecutive Cases; Q4: Subject Comparability; Q5: Intervention Clearly Described; Q6: Outcome Measures Defined, Valid, Reliable, and Consistently Implemented; Q7: Sufficient Length of Follow-up; Q8: Statistical Methods Well Described; Q9: Results Well Described; Q10: Quality Rating (Good/Fair/Poor)
Allan et al,16 2004
Low
Low
Low
Low
Low
Low
Pezza et al,13 2015
Low
Low
Low
Moderate
Low
Low
Fruzzetti et al,12 2017
Low
Low
Low
Low
Low
Low
Leppink et al,17 2017
Low
Low
Low
Low
Low
Low
Donnarumma et al,15 2020
Low
Low
High
High
Low
Low
Owczarczyk-Saczonek et al,14 2021
Low
Low
Low
Low
Low
Low
Minozzi et al,21 2008
Moderate
Low
Low
Low
Low
Low
Low
Low
Dall’ Oglio et al,19 2017
Moderate
Low
Low
Low
Low
Moderate
Low
Moderate
Fabbrocini et al,22 2017
Moderate
Low
Low
Low
Low
Low
Low
Low
Advani et al,18 2020
Moderate
Low
Low
Low
Low
Moderate
Low
Moderate
Ramanan et al,20 2020
Moderate
Low
Low
Low
Low
Low
Low
Low
Seedat et al,23 2001
Yes
Yes
Unclear
Unclear
Yes
No
Yes
Unclear
Yes
Fair
Khurana et al,24 2019
Yes
Yes
Unclear
Unclear
Yes
Yes
Yes
Unclear
Yes
Fair
The authors have no conflict of interest to declare.
This article has no funding source.
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