Galangal

Generic name: Alpinia Galanga, Alpinia Officinarum Hance, Kaempferia Galanga L.
Brand names: Ankaferd BloodStopper, Blue Ginger, Chewing John, China Root, Chinese Ginger, East Indian Root, Galanga, Galangal Root, Greater Galangal (A. Galanga), Kulanjan, Laos, Lesser Galangal (A. Officinarum), Little John Chew, Rhizoma Galangae

Usage of Galangal

Clinical trials are lacking, with the majority of support for galangal therapeutic use based on in vitro or animal data, or anecdotal and traditional claims.

Antimicrobial activity

Animal and in vitro data

Activity against a number of pathogenic bacteria has been shown in vitro for whole plant and crude rhizome extracts, as well as for galangin and kaempferide.(Kaur 2010, Latha 2009, Niyomkam 2010, Rao 2010, Rao 2011, Sawamura 2010, Srividya 2010, Vuddhakul 2007) Synergistic effects with antibiotics against resistant bacteria have also been demonstrated in vitro.(Eumkeb 2010, Eumkeb 2012, Lee 2008) The rhizome extract of K. galanga was also found to have some inhibitory activity against Helicobacter pylori in vitro, with a minimal inhibitory concentration (MIC) of 25 mcg/mL.(Bhamarapravati 2003) In vitro experimentation in H. pylori–infected gastric epithelial cells was conducted with 24 medicinal plants indigenous to Pakistan to evaluate their effects on secretion of interleukin 8 (IL-8) and generation of Reactive oxygen species in order to assess anti-inflammatory and cytoprotective effects. Although no direct cytotoxic effects on gastric cells or bactericidal effects on H. pylori were found, a rhizome extract of A. galanga was observed to have moderate and strong inhibitory activity on IL-8 at 50 mcg/mL and 100 mcg/mL, respectively.(Zaidi 2012) Another in vitro study found no activity against Aspergillus niger or Candida albicans.(Srividya 2010)

In mice, a methanol extract of A. galanga rhizomes showed inhibitory activity against the malaria parasite Plasmodium berghei.(Al-Adhroey 2010) Activity against the influenza virus was demonstrated in mice following oral administration of an A. officinarum extract.(Sawamura 2010)

Antioxidant activity

Antioxidant activity has been described for galanga crude extracts and for specific flavonols and phenols.(Guo 2010, Hanish Singh 2011, Puangsombat 2011, Srividya 2010)

Antiulcer effects

Animal data

In a study of rats, A. officinarum extract reduced Indomethacin-induced gastric injury in a dose-Dependent manner, occurring through both cyclooxygenase and noncyclooxygenase pathways.(Gong 2018)

Cancer

Animal and in vitro data

In vitro studies have shown activity of galangal extracts against a variety of cancer cell lines. Active chemical constituents identified include galangin, 4-hydroxycinnamaldehyde, curcuminoids, and diarylheptanoids. Direct cytotoxicity, induction of apoptosis, antimigration, anti-invasion, and inhibition of tumor growth have been demonstrated.(An 2008, Banjerdpongchai 2011, Jaiswal 2012, Lu 2007, Matsuda 2009, Panich 2010, Tabata 2009, Zou 2020) Cytotoxic diterpenes have been found in the seeds of A. galanga.(Leung 2003, Morita 1988)

A. galanga shows antitumor activity in mice.(Jaiswal 2012, Matsuda 2009)

CNS

Animal and in vitro data

An ethanol extract of A. galanga decreased neurotoxin-induced amnesia in mice. A decrease in acetylcholinesterase and monoamine oxidase enzyme activity was observed in the amnesia mouse model and in an in vitro study.(Guo 2010, Hanish Singh 2011) An analgesic effect of A. galanga extract was demonstrated in mice using the hot plate and writhing tests.(Acharya 2011)

Clinical data

In a randomized, double-blind, double-dummy, placebo-controlled clinical trial of 59 patients with moderate caffeine intake, the effects of A. galanga (300 mg per capsule) alone, caffeine alone, a combination of A. galanga and caffeine, or placebo on mental alertness were assessed. A. galanga increased mental alertness scores at 1, 3, and 5 hours after dosing compared with placebo. Additionally when coadministered with caffeine, A. galanga impeded a caffeine "crash" at 3 hours after dosing.(Srivastava 2017)

Diabetic nephropathy

Animal data

A murine study found that an alcoholic extract of A. galanga reduced Glucose levels, improved glycosylated hemoglobin A1c levels, improved lipid parameters, and ameliorated histological changes in the kidneys of rats with streptozotocin-induced diabetes.(Kaushik 2013)

Hypoalgesia effects

Clinical data

A systematic review and meta-analysis of 8 randomized, double-blind, placebo-controlled clinical trials (N=734) published before December 2014 found an overall moderate to large effect of Zingiberaceae extracts (including turmeric, Ginger, and galangal) on chronic pain compared with placebo; however, substantial heterogeneity was found. Significantly lower subjective pain was reported with the Zingiberaceae extracts versus placebo (P=0.004). A strong dose-response relationship was also demonstrated. Three studies included patients with osteoarthritis of the knee or hip, and 1 study each included patients with gonarthritis, irritable bowel syndrome, muscle soreness following exercise, postoperative pain, and primary dysmenorrhea. One of the osteoarthritis trials (n=247) used 510 mg/day of mixed galangal and ginger rhizome extracts for 6 weeks, with a moderate reduction in pain when walking demonstrated in the treatment group versus placebo.(Lakhan 2015)

Metabolic syndrome

Limited studies in rats have shown improved lipid profiles and insulin resistance with galangal supplementation.(Sivakumar 2010, Xia 2010)

Galangal side effects

Research reveals little or no information regarding adverse reactions with use of galangal.

Before taking Galangal

Information regarding safety and efficacy in pregnancy and lactation is lacking.

How to use Galangal

Clinical studies of galangal monotherapy are lacking to provide a basis for doSage recommendations.

Warnings

In a murine study assessing acute toxicity, A. galanga ethanolic extract caused defecation, writhing, sedation, and calmness, while A. galanga dichloromethane extract caused increased respiration, piloerection, Straub tail, tremors, increased muscle tone, and sedation.(Alajmi 2018) In this SAMe study, the treatment period was extended to 12 weeks to assess chronic toxicity. Compared with control, mice receiving either extract of A. galangadid not differ in terms of body weight, food consumption, or water consumption. However, treatment with either extract was associated with increases in weight of the heart, liver, spleen, and kidneys. A. galangawas also noted to increase liver function tests and blood glucose in these models.(Alajmi 2018) One murine study indicated that an alcoholic extract of A. galangaat a dose up to 2,000 mg/kg was safe.(Kaushik 2013)

Another study in A. galanga–treated animals showed a rise in red blood cell levels, weight gain of sexual organs, and increased sperm motility and sperm counts. No spermatotoxic effects were noted.(Qureshi 1992)

What other drugs will affect Galangal

None well documented.

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