Abstract
The health catastrophe originated by COVID-19 pandemic construed profound impact on a global scale. However, a plethora of research studies corroborated convincing evidence conferring severity of infection of SARS-CoV-2 with the aberrant gut microbiome that strongly speculated its importance for development of novel therapeutic modalities. The intense exploration of probiotics has been envisaged to promote the healthy growth of the host, and restore intestinal microecological balance through various metabolic and physiological processes. The demystifying effect of probiotics cannot be defied, but there exists a strong skepticism related to their safety and efficacy. Therefore, molecular signature of probiotics termed as “postbiotics” are of paramount importance and there is continuous surge of utilizing postbiotics for enhancing health benefits, but little is explicit about their antiviral effects. Therefore, it is worth considering their prospective role in post-COVID regime that pave the way for exploring the pastoral vistas of postbiotics. Based on previous research investigations, the present article advocates prospective role of postbiotics in alleviating the health burden of viral infections, especially SARS-CoV-2. The article also posits current challenges and proposes a futuristic model describing the concept of “precision postbiotics” for effective therapeutic and preventive interventions that can be used for management of this deadly disease.
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Introduction
The world is facing the apocalypse of egregious pandemic COVID-19 due to SARS-CoV-2 that confers cataclysmic impact on social, economic, and public health at global level. The various respiratory manifestations including sore throat, fever, fatigue, cough, shortness of breath, headache, sputum production, and acute respiratory distress syndrome (ARDS) are an outcome of infection of SARS-CoV-2 [1]. The severity of infection leads to various complications including renal, gastrointestinal, cardiac, neurological symptoms, as well as serving a palette for other chronic secondary fungal and bacterial infections culminating hospitalization and eventually in death [2]. However, these respiratory manifestations accentuated scientific community for bolstering their research in lungs for finding pharmacological and non-pharmacological ailments and most importantly vaccines [3] for combating this problem but the severity of infection has been well correlated with our most dynamic organ of the body, i.e., gastrointestinal tract [4]. The pioneering efforts of various microbiologists present in nineteenth century conceptualize the idea of the presence of microorganisms inside the human body that interplays a constant struggle against each other; however, the advent of next-generation sequencing transformed our understanding towards these microorganisms. Presently, we are living in the era of “rendezvous with our microbes” emboldened the fact that the human body is colonized by trillions of microorganisms and contains approximately 150 million genes that exists in negotiated “state of détente” in symbiotic manner, severely impacting the health and diseased status of humans. This dynamic consortium is referred as “gut microbiome” and the year 2020 portrayed quantum leap on various insights on correlation of gut microbiome with COVID-19 [5, 6]. Research findings evidenced the presence of viral replication in infected human intestinal epithelial cells, high expression of ACE-2 receptors in intestinal epithelium, presence of viral RNA in feces, depletion of gut commensals, and enhancement of opportunistic pathogens that highlighted the pivotal role played by gut microbiome in COVID-19 [7,8,9,10,11]. Plenty of research articles have emphasized the intervention of diet, prebiotics, probiotics, and synbiotics that can be used as prophylactic measures for modulation of the gut microbiome [12,13,14,15,16]. Also, scientists are trying to underpin the role of probiotics that can be envisaged in the form of several clinical trials that are still under investigation. Table 1 summarizes the various clinical trials utilizing probiotics for combating COVID-19. Despite the marvelous credentials possessed by probiotics, certain studies indicated their adverse technological and clinical effects including the presence of virulence factors in some probiotic strains, strain-specific mechanisms, diverse patterns of colonization, production of biogenic amines, short lived, ability to cause opportunistic infections, bacteremia and sepsis in immunocompromised individuals, niche-specific action of probiotics (allochthonous or autochthonous), lacking long-term clinical trials, and clear recommendations across the globe [17]. Therefore, the postbiotics, functional bioactive molecules released by probiotics have been thrust area of research nowadays, and there is a growing continuum of studies highlighting the various health benefits that have been reported in the past decade [18, 19]. However, there is dearth of studies pertaining to the use of postbiotics for antiviral effect especially combating SARS-CoV-2 infections but the past research efforts highlighted the role of postbiotics in ameliorating various viral infections. Thus, based on previous investigations, the article culminates the prospective therapeutic opportunities of postbiotics for coping up the imperil of COVID-19 as well as posits current challenges, and proposes a futuristic roadmap of utilizing the postbiotics in precise manner for overcoming such pandemic situations.
Conception of Postbiotics and Mechanism of Action
The advancements in elucidating the structural and functional dimensions of gut microbiome lead the world into new era of biotic research. The word “biotics” is derived from the Greek term “biotikós” meaning “pertaining to life” that signify the presence of living organisms in biological ecosystem connected with their physical environment. More comprehensively, the term biotics is more connected towards the adoption of various nutritional strategies that favors the modulation of gut microbiota attaining towards the healthy status of the host [20]. The research has already been directed towards various biotic components like prebiotics, probiotics, and synbiotics and their magnificent ramifications in the host physiology. However, in the quest for interpreting their effects at molecular level in the host, the research has progressed towards understanding the probiotic effector molecules eliciting beneficial response known as postbiotics, the relatively new member of “biotics” family. Postbiotics are considered functional bioactive molecules generated during microbial fermentation of food in gastrointestinal tract. The difference in their effects and composition lies with the extent of microbial metabolization of diverse food matrix; therefore, the term postbiotics is referred as umbrella term for all microbial fermented products and their synonyms [21, 22]. However, several researchers recommended different terminologies to describe probiotic effector molecules like metabiotics, ghost probiotics, inactivated probiotics, non-viable probiotics, paraprobiotics, and pseudoprobiotics [23,24,25]. Though exact definition has not been described yet, but hitherto postbiotics are defined as non-viable bacterial products or metabolic products from microorganisms that have biological activity in the host [26]. From conception to various applications of postbiotics along with its timeline development is depicted in Fig. 1. The preliminary research highlighted two major classes of postbiotics known as paraprobiotics and fermented infant formulae (FIFs). According to Food and Agriculture Organization/World Health Organization (FAO/WHO), paraprobiotics is defined as “non-viable microbial cells (either intact or broken) which when administered (either orally or topically) in adequate amounts, confer a benefit on the human or animal consumer” [27], and FIFs are infant or follow-on formula mostly obtained with the fermentation of food by lactic acid–producing microbes and devoid of any viable bacterial cells [28]. Therefore, diversified metabolic products such as short-chain fatty acids (SCFAs), microbial cell fractions, functional proteins, extracellular polysaccharides (EPS), cell lysates, teichoic acid, peptidoglycan-derived muropeptides, and pili-type structures have been categorized as postbiotics. The application of postbiotics alleviates various technical and functional challenges like colonization efficiency, stability and viability in GIT and industrial processing, shelf life, transfer of virulent, and antibiotic resistance genes that are associated with utilization of living cells as probiotics. The credentials of postbiotics such as safe profile, known chemical structures, resistance to hydrolysis, nontoxic, stable to digestive system conditions, and better shelf life confer lucrative options for biotherapeutic utility. Therefore, currently humongous efforts have been made to visualize the application of postbiotics as biotherapeutic agents for the elimination of various diseases. Table 2 summarizes the various applications of postbiotics for maintaining the health status of an individual [29,30,31,32,33,34,35,36,37,38,39,40,41,42,43,44,45,46,47,48,49,50,51,52,53,54,55,56,57,58,59,60,61,62,63,64,65,66,67,68,69,70,71,72,73,74,75,76,77,78]. The current catastrophe imparted due to COVID-19 motivates us to think the prospective role of postbiotics for combating COVID-19 [79, 80]. However, it is an intriguing fact that there exists an intricate complexity between invasive virus, gastrointestinal microbiome, and host physiology, but scientists are rigorously trying to unravel these complexities. The antiviral effect of probiotics has been reported in previous studies and based on these research efforts, the antiviral mechanism of postbiotics against COVID-19 can be correlated as (a) production of antiviral inhibitory metabolites, (b) improvement of intestinal epithelial lining barrier function, (c) modulation of innate and adaptive immune system, (d) effect on gut-brain axis, and (e) role in alleviation of secondary fungal infections. The proposed idea of postbiotics triggering various effects that can be a milestone for development of therapeutics for ameliorating COVID-19 needs well-designed clinical trials in humans for further validation and approval for commercial use in the future.
Conception, timeline development, and applications of postbiotics
Delineating the Anti-COVID Mechanisms of Postbiotics
Prospective Role of Postbiotics in Modulating Intestinal Epithelial Barrier Integrity
The intestinal epithelial cells act as a frontier in maintaining the synergistic balance between host molecules and microbiota. The intrusion of pathogens posits high risk of pathogenesis leading to various anomalies such as disruption of intestinal barrier, dysbiosis, and subsequently leaky gut. These factors induce panoply of highly coordinated defense mechanisms that restore barrier function, innate and adaptive immune response for restricting the entry of various pathogens. The intestinal barrier integrity gets disrupted with entry of SARS-CoV-2 that leads to various changes in the intestine that significantly impact the integrity of IEC. The different secretory metabolites of probiotics such as indole, bacteriocins, organic acids, secretory proteins, hydrogen peroxide, and nitric oxide (NO) have shown potential in reserving the intestinal barrier function by enhancing the expression of tight junctions, mucus secretion by goblet cells, and boosting the production of antimicrobial peptides [81,82,83,84]. The secretory proteins p40 and p75 have been reported to maintain the homeostasis of intestinal epithelial cells by two known mechanisms [85, 86]. Firstly, these proteins lead to the transactivation of epidermal growth factor receptor (EGFR) followed by upregulation of proliferation-inducing ligand (APRIL) expression in intestinal epithelial cells. The expression of APRIL induces the production of IgA as well as impaired the cytokine-induced apoptosis that helps in the clearance of the virus [87]. Secondly, these proteins also actuate the production of heat shock proteins Hsp72 and Hsp25 that has the ability to protect tight junction proteins as well as stimulate the phosphatidylinositol 3-kinase (PIK3)–dependent Akt pathway for the proliferation of gut epithelial cells. In addition to that, a soluble protein HM0539 from novel LGG enhances mucus secretion through mucin expression and protects intestinal integrity by the expression of tight junction proteins. Similarly, extracellular vesicles also known as outer membrane vesicles a lipid bilayer structure secreted by probiotics and other intestinal microbiota also impact the integrity of IECs. The extracellular vesicles released by Akkermansia muciniphila reduce the permeability of the intestine by upregulating the expression of claudin-3 protein through activation of AMP-activated protein kinase (AMPK) pathway [88]. The OMVs released by E. coli Nissle and E. coli ECOR63 have the ability to upregulate two tight junction proteins, i.e., ZO-1 and claudin-14 as well as expression of IL-22 that may prevent the entry of the virus into systemic circulation [89]. Furthermore, short-chain fatty acids (SCFAs) constituting acetate, propionate, and butyrate secreted by various probiotics by the fermentation of undigested dietary fibers (prebiotics) confer considerable role in intestinal integrity. Among SCFAs, butyrate is the most preferentially utilized energy source by IECs; thus, voluminous information has been available elucidating its effect on intestinal epithelial barrier. There are various mechanisms of SCFA by which it plays a crucial role that helps in maintaining the homeostasis of IECs. The binding of G-protein-coupled receptors, such as GPR109A, GPR43, and GPR41in IECs, strengthens the integrity of epithelial cells particularly the binding with GPR109A induces IL-18 that promotes intestinal homeostasis [90]. In addition to that, butyrate also induces the binding of AP-1 with MUC2 promoter followed by enhancement of expression of MUC2 mRNA level leading to enhanced production of mucin. As butyrate is also considered good histone, deacetylase inhibitor thus promotes acetylation of H3 and H4 histone proteins and methylation of H3 protein on the MUC2 promoter that boost the safety of mucosal barrier. The stability of hypoxia-inducible factor (HIF) by enhancing the expression of HIF target genes strengthening epithelial barriers is also linked with the action of butyrate [91]. The production of LL-37 (cathelicidin) confers antimicrobial property in IEC that maintains the functionality of IECs in the presence of pathogens [59]. The maintenance of TEER by binding of butyrate with various receptors mentioned above may confer protective role in IEC homeostasis. Apart from that, another secretory metabolite indole produced by E. coli Nissle maintains the TEER by downregulation of TNF-α-mediated NF-κB signaling pathway facilitating the epithelial function [92]. The binding of indole 3-propionic acid (IPA) with one of the gut epithelial receptors, i.e., pregnane X receptor (PXR), facilitates the upregulation of tight junction proteins coding mRNAs followed by augmentation of production of claudins and occludins that is crucial for epithelial barrier integrity after viral infection. In addition to that, indole secreted by Bifid. infantis induces the activation of aryl hydrogen receptors (AhRs) that facilitates the upregulation of the protein expression of CYP1A1 followed by enhanced transcription of IL-22 [93]. This induction activates the secretion of antimicrobial peptides that may help in clearance of the virus. In addition to that, bacteriocins an important antimicrobial peptide is secreted by probiotics and other gut microbes. They are divided on the basis of mechanism of action, size, and inhibitory spectrum. The antiviral effect of various bacteriocins has been reported for the treatment for viral disorders by modulating the immune system. Research studies speculated that the replication of viruses at early and late stages has been inhibited by the application of enterocin AAR-74, enterocin AAR-71, erwiniocin NA4 secreted from Enterococcus faecium CRL35 and other species, and bacteriocin B1 from Lact. delbrueckii subsp bulgaricus. Apart from that, labyrinthopeptin A1 and A2 (LabyA1), carbacyclic lantibiotics, have also been shown to inhibit the virus entry into the host [94]. In addition to that, various other bacteriocins such as Nisin A and mutacin B-Ny266, microbisporicin, lacticin, thuricin CD, and reuterin produced by various probiotic strains also reported to have antimicrobial activity that can be further warranted for reducing SARS-CoV-2 infection. Moreover, other surface components such as lipoteichoic acid, surface layer proteins (SLPs), capsular polysaccharide (CPS), pili, flagella, and lipopolysaccharides have been designated as microbial-associated molecular patterns (MAMPs) and credited with various bioactive properties. The infection of SARS-CoV-2 can be reduced by implementation of these molecules as they possess the binding affinity with various pattern recognition receptors (PRRs) such as toll-like receptors (TLRs) and NOD-like receptors (NLRs) that further regulate various signaling cascades including mitogen-activated protein kinases (MAPK), nuclear factor kappa B (NF-κB), peroxisome proliferator–activated receptor gamma, and other protease-depending signaling pathways in IECs. The alteration in TEER and integrity caused by viral entry into gut epithelium was maintained by surface layer proteins produced by Lactiplantibacillus plantarum and Lact. acidophilus. Micro integral membrane proteins (MIMPs), a small domain of SLPs from Lactiplantibacillus plantarum, have been shown to restore the integrity of IECs by enhancing the mRNA expression of various tight junction proteins claudin-1, occludin, and JAM-1 and F-actin [95, 96]. Furthermore, research studies depicted convincing evidence that the attachment of flagellin produced by E. coli Nissle 1917 (EcN) with TLR5 receptor present in basolateral membrane of IEC activates phosphatidylinositol-3-kinase (PI3K)/AKT signaling pathway that reduce the expression of proinflammatory genes that further reduce inflammation [97]. It has also been reported that β-defensin, an antimicrobial peptide secreted by intestinal epithelial cells through NF-κB and activating protein-1 (AP-1) signaling pathways, has also been induced by EcN flagellin [98, 99]. Furthermore, pili, a filamentous accessory organ present in the surface of bacteria, have capability of maintaining the integrity of intestinal epithelial cells. Tight adhesion (Tad) pili of Bifid. breve UCC2003 have been reported to enhance the proliferation of IECs and mucus secretion [100]. Apart from that, SpaC pilin present in Lacticaseibacillus rhamnosus GG (LGG) activated the ERK phosphorylation pathway for the protection of intestinal epithelial barrier [101]. Moreover, F1C pili of EcN possess ability to bind with mannosylated glycoproteins in the intestine through TLR4-mediated pathway for strengthening the production of tight junction proteins. Furthermore, the reinforcement of intestinal microenvironment is done by capsular polysaccharides secreted by probiotics. CPS5 secreted by Bact. thetaiotaomicron reduced the antibiotic stress in IECs and improves the colonization of beneficial bacteria preventing the adhesion of pathogens [102, 103]. In addition to that, the K5 capsular polysaccharide induces the expression of chemokines by activation of MAPK pathway by binding with TLR5 in IECs that reduce the inflammation in the gut [104]. The comprehensive mechanistic view of postbiotic action is represented in Fig. 2. Thus, by stating above facts, the postbiotics impart disparate effect on strengthening and maintaining the integrity of epithelial cells. The IECs have primary line of contact of SARs-CoV-2 entry and trigger severe immunological and biochemical changes in the gut; thus, by highlighting the effects of postbiotics, it is tangible to use these molecules for reducing the viral load and its clearance for combating COVID-19 in cutting-edge manner.
Modulation of intestinal barrier integrity by various postbiotics (schematic illustration depicting the action of various postbiotic molecules affecting intestinal barrier functions) (red arrow representing the upregulation of various signaling pathways by various postbiotic molecules while blue arrow representing the downregulation of signaling pathways). AMPs, antimicrobial peptides; AP-1, activating protein; CSP, capsular polysaccharide; IECs, intestinal epithelial cells; HIF, hypoxia-inducible factor; GPCRs, G-protein-coupled receptors; AhRs, aryl hydrogen receptors; P75 and P40, cell wall–associated hydrolase; EGFR, epidermal growth factor receptor; PI3K, phosphatidylinositol-3-kinase; PXR, pregnane X receptor; APRIL, a proliferation-inducing ligand; Hsp72 and Hsp25, heat shock proteins; ZO-1, zona occludin,1; IPA, indole 3-propionic acid; TEER, transepithelial electrical resistance; TJPs, tight junction proteins; TLR, toll-like receptors
Prospective Role of Postbiotics in Innate and Adaptive Immunity
The invasion of SARS-CoV-2 into the host cell is immediately recognized by antigen-presenting cells (APCs) that leads to the stimulation of innate immune system. The various viral structural components such as glycoproteins, dsRNA, or other intermediate metabolic products of the virus collectively termed pathogen-associated molecular patterns (PAMPs) recognized by pattern recognition receptors (PRRs) conferred as primary viral sensors for mediating antiviral effector program by producing type I interferon (Type I IFN) response. However, 10% of patients of COVID-19 have been found to produce autoantibodies against type 1 IFN-γ due to the mutations found in IFN genes that is associated with lymphopenia. Thus, various innate immunomodulatory molecules secreted by probiotics in the gut lumen may confer protecting role against deadly virus. Various postbiotic molecules stimulate the production of mucin from goblet cells, antimicrobial peptide as defensins, trefoil factor by paneth cells and secretory IgA, heat shock proteins, and various p-glycoproteins that are responsible for maintaining innate immunity after the entry of the virus in the intestinal system. It is well proven that ACE-2 is a viral receptor, and a type I cell surface glycoprotein is also found in enterocytes apart from type I and type II alveolar epithelial cells, the arterial smooth muscle tissues, arterial and venous endothelial cells, and renal and cardiovascular tissues. The basic function of ACE-2 is to perform amino acid homeostasis in the intestine that helps in the alleviation of intestinal inflammation, the expression of antimicrobial peptides, and maintenance of healthy gut microbiota. After the ACE2 receptor engagement, the processing of SARS-CoV2 has been done by a type II transmembrane serine protease, TMPRSS2, present in intestinal epithelial cells and other serine proteases such as TMPRSS4 [105, 106] and ST14/matriptase are also expressed in mature enterocytes. The severity of infection is accelerated by the action of TMPRSS4. However, the expression of B0AT1 the sodium-dependent neutral amino acid transporter and amino acid (proline) SIT1 transporters on the luminal side of intestine epithelial cells is also associated with ACE2 expression. SARS-CoV-2 leads to the downregulation of ACE2 that further leads to the impairment in one of essential amino acid tryptophan, an essential modulator of kynurenine pathway for the formation of serotonin and other bioactive molecules by utilizing the indoleamine 2,3-dioxygenase (IDO) enzyme. The various indole metabolites such as indole acetic acid, indole propionic acid, and tryptamine are generated during kynurenine pathway by metabolism of tryptophan that is secreted by probiotics that confers potential role in the differentiation of Treg cells and suppression of T effector cells [107]. Apart from these, indole metabolites also activate the production of IL-22 from natural killer T (NKT) cells, innate lymphoid cells (ILCs), and CD4+ lymphocytes cells by inducing the expression of IL-22 receptor on IECs by triggering Stat3 pathway, mucin production, and release of AMPs by paneth cells [108, 109]. The tryptophan impairment also leads to the aberrant expression of serum IL-6 and mammalian target of rapamycin (mTOR) protein kinase, p70S6kinase, that further impacts the production of various antimicrobial peptides such as lysozyme, cysteine-rich cationic peptides, RegIIIg, and α-defensin HD5 and HD6 and alerted microbial diversity that enhances the susceptibility of intestine towards inflammation. Thus, the severe diarrhea in COVID-19 is the outcome of such alterations; therefore, supplementation of tryptophan in diet can be considered a preventive strategy for reducing the viral invasion in GIT. Furthermore, the secretion of antimicrobial peptides is also triggered by an effector molecule known as bacterial muramyl dipeptide (MDP) that is secreted by various Lactobacillus probiotics. The molecule is recognized by nucleotide-binding oligomerization domain2 (NOD-2) receptor that led to the activation of MAPK and NF-kB signaling pathway for secretion of various above-mentioned antimicrobial peptides [110, 111]. Among all AMPs, the human defensin-5 (HD5) has highest affinity of 76.2 nM with ACE2 receptor; thus, it can be acting as competitor with SARS-CoV-2 for binding. Moreover, the intestinal immune system also embraced the IgA, a non-inflammatory immunoglobulin acting as receptor for various pathogens. The secretion of IgA is mediated by intestinal B cells that can bind with polymeric Ig receptor (pIgR) which function as an antibody transporter expressed on the surface of intestinal epithelium facilitates the translocation of IgA dimmers in gut lumen and converted to secretory IgA. It was reported that lipoteichoic acids and peptidoglycan secreted by various probiotic species have the ability to induce the secretion of IgA with the help of TLR activation that has the ability to kill the virus particle. Research studies also speculated some aspects of antiviral defense through secretion of trefoil factors from mucin-producing cells have been upregulated by postbiotics. Furthermore, butyrate, an important type of SCFA, has been found to be low after viral infection that facilitates the upregulation of NRP-1 contributing towards the infectivity of SARS-CoV-2 through furin-mediated cleavage of viral spike proteins [112]. To abrogate the infectivity rate of the virus, butyrate as postbiotics can bind to the both GPR41 and GPR43 receptors. The binding of butyrate with GPGR41 activates protein kinase A (PKA) pathway while binding with GPR43 activates phospholipase C for the production of diacyglycerol (DAG) that activates protein kinase C (PKC) and inositol triphosphate which trigger the release of intracellular Ca2+ ions that plays significant role in reduction of binding of viral spike protein with ACE2 receptor on IECs. The secretion of Vit D through probiotics or supplemented with diet triggers the attachment of vitamin D receptor (VDR) and p65 subunit of NF-kB pathway followed by its downregulation leads to the enhanced synthesis of tight junction proteins such as claudin and occludin that maintains the integrity of intestinal epithelium. Apart from that, the binding of VDR also downregulates the JAK/STAT pathway that leads to the enhanced synthesis of various antimicrobial peptides like LL-37 and β-defensin.
The signaling cascades described above foster phagocytosis of viral antigens by host macrophages that orchestrated the development of adaptive immune response [113]. In fact, the exaggerated immune response is manifested with enormous release of cytokines better termed as “cytokine storm” and secreted through various immune cells like innate macrophages, dendritic cells, natural killer cells, and the adaptive T and B lymphocytes. The colossal release of TNF-α, IL-6, IL-1β, IL-2, IFNα, IFNβ, and MCP-1 along with proinflammatory cytokines such as IL-1, IL-2, IL-7, G-CSF, IP-10, and MIP-1A is likely to contribute multi-organ failure and high mortality rate of people having COVID-19 at global scale [114]. However, research studies confirmed the application of heat-killed Lacticaseibacillus casei IBS041 (LC) and Lact. acidophilus AD031 (LA) that has been reported to decrease the expression of IL-6 and TNF-α and diminish the inflammation in IECs but the link with secreted components has not beet conclusively established yet. Similarly, the upregulation of IL-10 by inducing the expression of Treg cells has been reported for the reinforcement of intestinal homeostasis mediated through the secretory components of Bifid. breve. Furthermore, the internalization of probiotics either through M cells or paracellular transport through epithelial cells into payer’s patch (PP) and subsequent release of their components may promote the secretion of IgA antibodies that is crucial for clearance of viral components [115]. The detailed mechanistic view of postbiotics is summarized in Fig. 3. Thus, these studies strongly support that various postbiotics play pivotal role in modulating the innate and adaptive immunity to reduce the burden of SARS-CoV-2 infection and proliferation in the gut. Thus, postbiotics could be a prospective armamentarium for abrogating the enigma of COVID-19 [116, 117].
Modulation of innate and adaptive immunity by various postbiotics (schematic illustration depicting the action of various postbiotic molecules affecting innate and adaptive immunity) (red arrow representing the upregulation of various signaling pathways by various postbiotic molecules while blue arrow representing the downregulation of signaling pathways; green arrow representing the reduction of postbiotic molecules after binding of SARS-CoV-2 with ACE-2 receptor) ACE2, angiotensin-converting enzyme; B0AT1, amino acid transporter; NOD, nucleotide-binding oligomerization domain2 (NOD-2); IDO, indoleamine 2,3-dioxygenase; NKT, natural killer T; NRP-neuropilin; mTOR, mammalian target of rapamycin; PKA, protein kinase A; HD-5, human defensin-5; GPRs, G-protein receptors; IL, interleukin; IFN, interferon; JAK/STAT, Janus kinase/signal transducers and activators of transcription; MCP-1, monocyte chemoattractant protein,1; G-CSF, granulocyte colony-stimulating factor; IP-10, interferon gamma-induced protein 10; MIP-1A, macrophage inflammatory protein,1; VDR, vitamin D receptor
Prospective Role of Postbiotics in Mental Health
The pandemic COVID-19 decimated more than three million deaths within a year despite the modern advancements in medical field. Apart from the death toll, more than 150 million recovered people have suffered from physical, emotional, and economic problems that leads to vicarious traumatization causing various mental health problems including depression, anxiety, and posttraumatic stress disorder (PTSD). Research studies defined the criteria for posttraumatic stress disorder (PTSD) varying from individuals who themselves suffered from COVID-19 and also witnessed the death of their family members, close relatives, and friends. The stress also encompasses the individuals greatly exposed to aversive information due to COVID-19. Recently, the people who have suffered from COVID-19 also faced the problem of aberrant cognition, memory loss, severe depression, and anxiety and thus considered emerging health concern at post-COVID scenario is better known as “Brain Fog”[117]. Though the current modality for diagnosing the maladies of the brain with MRI does not signify any damage or injury yet due to COVID-19 but as the gut plays pivotal role in COVID-19, there might be a chance that certain factors like gut dysbiosis [118] lead to alteration in neurotransmitters, adrenal gland secretion, and inflammation in nerve cells that aggravate the mental problems. The bifacial communication between the brain and gut forms the basis of “gut-brain axis” that affects the functionality of each other via immune, neural, and endocrine pathways. The normal regimens like taking nutritious diet, maintaining healthy lifestyle and good sleep, eliminating psychological distress, and exercise may alleviate this problem at certain extent but not at full pace. The routine pharmacological interventions are associated with numerous side effects such as nausea, headaches, agitation, and sedation. Thus, recently the research studies suggested the ingestion of live microbes known as psychobiotics in sufficient amount that has the ability to alleviate the suffering from anxiety, depression, stress, and poor cognition. The strain-specific effects and their vulnerability for natural selection in the host have proven their dilemmatic role in mental medicaments. Therefore, various bioactive molecules released by psychobiotics (as postbiotics) may provide more viable option for treating and managing COVID-19 in futuristic scenario. Research studies have proven that there exist three routes by which postbiotics may influence the PTSD in COVID-19. There is convincing evidence that various neurotransmitters such as acetylcholine, dopamine, gamma-aminobutyric acid (GABA), catecholamines, and serotonin have been secreted by probiotics that affect the normal functioning of the brain. We also know that the brain and gastrointestinal (GI) tract share a bifacial communication axis called “gut-brain axis” [119] that has the ability to affect other functions through neural, immune, endocrine, or humoral links [120]. Furthermore, homeostasis of hypothalamic–pituitary–adrenal axis (HPA) during stress conditions is also maintained by probiotic effector molecules and thirdly, the anti-inflammatory molecules released by probiotics have neuromodulatory effects. As COVID-19 is manifested by vicious cycle of altered gut microbiota profile, increased intestinal permeability and chronic inflammation lead to changes in mental framework through imbalances in neurotransmitter and hyperactive HPA axis which triggers stress, anxiety, depression, and impaired cognition gradually. The wide range of postbiotics secreted by probiotics may act via distinct pathways for overcoming the PTSD due to COVID-19 [121]. As it is evident, SARS-CoV-2 entry triggers the production of inflammatory cytokines ILs, tumor necrosis factor TNF-α, and IFN-γ that affects the permeability of intestinal cells leading to the movement of these cytokines by humoral pathways (through blood brain barrier), neural pathway (through vagus and spinal nerves), and cellular pathway (through monocytes or macrophages). These cytokines trigger the production of proinflammatory signals in the brain by binding with microglial receptors, disrupts the HPA homeostasis and impairment in regulation of neurotransmitters. This is a major mechanism that can be proposed for PTSD and brain fogging symptoms. The growing evidence of anti-depressive effect of GABA secreted by Lacticaseibacillus rhamnosus and Lacticaseibacillus casei enters through the neural route that modulates the GABAergic system and HPA axis in the brain. The alteration of mRNA expression of GABAA and GABAB receptors leads to reduction in depressive behavior. GABA secreted by Levilactobacillus brevis induces sound sleep and results in the aversion of depressive effects [122]. Furthermore, the cognitive impairments like loss of concentration and memory can be enhanced by secretion of serotonin and norepinephrine (NE) by Lact. hevleticus through the modulation of central 5-HT system, NE system, and HPA axis. In addition to that, histamines secreted by Limosilactobacillus reuteri in intestinal epithelial cells reduce the expression of proinflammatory cytokines that prevent the reduction of hippocampal brain-derived neurotrophic factor (BDNF), a biomarker for mental health [123]. Moreover, SCFAs such as butyrate play pivotal role in maintaining the gut barrier integrity that further impacts the expression of BDNF and modulation of 5-HT system in the central nervous system. The regulation of SCFAs in the brain leads to reduction in inflammation thus prevents anxiety and stress in the body. Furthermore, miscellaneous postbiotic molecules released by specific strains of probiotics also impart significant role in neuromodulation activities. The serpins secreted by Bifid. longum reach the brain through neural route that alter the inflammation by reduction of proinflammatory signals. In addition to that, gassericins secreted by Lact. gasseri promote the sleep and strengthen the composition of gut microbiome. Lactocepins secreted by Lacticaseibacillus paracasei facilitate the reduction of migration of inflammatory cytokines released during viral attack by maintaining the integrity of intestinal epithelium [124]. EPS secreted by Lact. kefiranofaciens confer immunomodulatory property that has potential to prevent the hyperactivity of HPA axis, and similar kind of polysaccharides produced through Bifid. infantis induces the production of NE neurotransmitter in CNS [125]. Furthermore, the conversion of albiflorin into BZA by Bifid. breve affects glutaminergic pathway via the humoral route. Furthermore, H2O2 released by Limosilactobacillus reuteri may prevent activation of IDO and circulation of KYN by proinflammatory cytokines that has the ability to reduce stress and depression in the host body [126]. The functionality of postbiotics on mental health is depicted in Fig. 4. Thus, based on the above discussion, it is conceivable to envision that postbiotics may have prospective role in abrogating various mental ailments during and post-COVID scenario. However, complete unravelling of pathophysiology must be required for completing the endeavor of postbiotic use in this aspect.
Postbiotics in balancing hypothalamic–pituitary–adrenal axis and mental health during post-COVID regime (schematic illustration depicting the action of various postbiotic molecules affecting mental health) (red arrow representing the upregulation of various signaling pathways by various postbiotic molecules while blue arrow representing the downregulation of signaling pathways) BDNF, brain-derived neurotrophic factor; DA, dopamine; 5-HT, 5-hydroxytryptamine or serotonin; BZA, benzoic acids; dgk, diacylglycerol kinase; EPS, exopolysaccharide; GABA, gamma-Aminobutyric acid; GLP-1, glucagon-like peptide,1; Glu, glutamate or glutaminergic; H2O2, hydrogen peroxide; HPA, hypothalamic–pituitary–adrenal axis; IECs, intestinal epithelial cells; IDO, indoleamine 2,3-dioxygenase; IL-6, interleukin-6; KYN, kynurenine; NE, norepinephrine; ROS, reactive oxygen species; SCFA, short-chain fatty acid; Tph1, tryptophan hydroxylase 1; TRP, tryptophan
Prospective Role of Postbiotics in the Management of Secondary Invasive Fungal Infections
COVID-19 has been sweeping around the world and accentuated exhaustive research on finding various treatment modalities to overcome the high mortality rate has been visualized in the second wave. The associated co-morbidities such as immunocompromised conditions, diabetes, chronic obstructive pulmonary disease (COPD), and hematological malignancies as well as overwhelming utilization of corticosteroids and antibiotics, prolonged ventilation, and intensive care unit stay provide the lucrative opportunity for various secondary invasive opportunistic infections [127]. These infections have been characterized as oropharyngeal candidiasis (OPC), COVID-associated pulmonary aspergillosis (CAPA), bloodstream candida infections, mucor mycosis (black fungus and white fungus), and Mucor septicus (yellow fungus) [128,129,130,131]. The strategic diagnostic embodiments are critically needed for identifying the invasiveness of fungus that traverses the major parts of the body and require critical care management. The significant decrease in lymphocyte count and increment in neutrophil count together with aggressive inflammatory response lead to severe immunosuppression that is the major cause of developing these chronic infections. In fact, recent research emphasized the dysbiosis of mycobiota in COVID-19. The reduction in the population of Aspergillus and Penicillium and enhancement in the population of Candida glabrata were observed in COVID-19 patients. Furthermore, the gut mycobiota profile of COVID-19 patients highlighted the positive correlation of Mucoromycota with Fusicatenibacter and Aspergillus niger with diarrhea, while presence of Penicillium citrinum depicted negative correlation with C-reactive protein (CRP) [132]. Till date, the first line of treatment is done by intravenous application of amphotericin B but several new generation triazoles like posaconazole, isavuconazole, and voriconazole have been used as salvage therapy for chronic patients who are refractory to amphotericin B. The empiric utilization of these medications leads to severe side effects including major impact on the kidney. Therefore, exploring the postbiotics can be an important way to resolve the complicacy of fungal infections. Various antimicrobial secreted by probiotics especially Lactobacillus species such as lactic acid, acetic acid, hydrogen peroxide, bacteriocins such as small heat-stable lantibiotics (SHSL), larger heat-labile proteins (LHLP), non-lanthionine-containing membrane-active peptides (MAP), and complex bacteriocins can be sustainable alternative for eradicating various fungal infections by blocking the growth and development of biofilm. The inhibition of various Candida species such as C. albicans, C. glabrata, C. tropicalis, C. krusei, C. kefyr, C. dubliniensis, and C. parapsilosis as well as A. flavus and A. parasiticus has been done by the supplementation of various probiotics majorly including Lactobacillus strains [133]. Recently, cell-free supernatant (CFS) as postbiotic, derived from Lacticaseibacillus paracasei 28.4, has depicted potential inhibitory activity against C. auris [134]. In addition to that, capric acid as postbiotic component secreted by Saccromyces boulardii has potential to reduce the expression of various virulence genes such as ino1, csh1, and hwp1 in C. albicans [135]. Furthermore, it has been reported that the infection of various Mucor species, like mucor mycosis and mucor sepsis, leads to alteration in the integrity of intestinal epithelial cells and modulates the healthy gut microbiome. These findings suggest that different postbiotic molecules that have potential to modify the integrity of IECs (described in the “Prospective Role of Postbiotics in Modulating Intestinal Epithelial Barrier Integrity” section) can be utilized for abrogating the deadly fungal infections. Though prodigious research is required to reach a convincing conclusion but rising data of resistant fungal strains and surge in immunocompromised patients due to prolonged antifungal treatments, the use of postbiotics is considered to be worthy ally for managing post-COVID-19 complications.
Current Challenges and Future Perspectives
The severe convulsion and wide-spread mortality have been seen across the globe due to the dreadful spread of COVID-19. The virus carries forward the legacy of mutation precisely by generating more infectious strains within a year. Currently, the exhaustive research has been pursued for the development of various diagnostic platforms, vaccines, and other pharmacological interventions for the effective control of this pandemic. Parallelly, mounting evidence of correlation of gut microbiome with severity of COVID-19 has also been highlighted. There is a growing enthusiasm for utilizing probiotics albeit their detailed mechanism of action is still under investigation due to inherent complexity and cross talk between host microbiome and invasive virus. Furthermore, their discordant proof of efficacy in some individuals leads to skepticism about their role as friends or foe. Thus, postbiotics may confer significant advantage over probiotics in reducing the severity of infection from deadly SARS-CoV-2. However, certain key questions need to be answered that is posing challenges for their massive utilization and acceptance both from therapeutic and regulatory perspective, such as: Which probiotic species are well suited for the retrieval of postbiotics? Which analytical method is best suited for their extraction? What is their effective delivery method inside the host, their stability, and shelf life? What are the relevant methodologies that could be used for assessing their biological and clinical effects? What are the bioprocessing strategies for the commercialization of postbiotics?
Till date, extensive studies have been pursued in animal models and in vitro platforms therefore translating in human body are quite challenging due to varied physiological conditions as well as the complex cross talk of host with their microbiome. The guidelines for recommending the use of postbiotics should also be rigorously formed for their safety and acceptance [136]. The pressing demand for comprehensive studies should be required for assessing the direct correlation between immunomodulatory activities of postbiotics and their suppressing effects by onset of predisposing disease features. Thus, well-designed multicentric clinical trials in humans using suitable postbiotic should be conducted for adopting these remarkable molecules at massive scale. However, diet, age, microbiome, and the surrounding environment confer significant impact on the outcome of postbiotics. Thus, there is a pressing need to shift from the conventional top-down approach of identifying efficient postbiotic molecules in healthy individuals and elucidating their mechanism of action for development of “precision postbiotics.” The advent of affordable next-generation DNA and high-throughput sequencing and “multiomics” technologies (metagenomics, metatranscriptomics, metaproteomics) enhances our knowledge of structural and functional dynamism of gut microbiome that leads to the analysis of voluminous data that require advanced computational tools. The growing continuum of the development of computational intelligence methods like machine learning metamorphosizes the microbiological research and paves the way forward to digitalized microbiology [137]. The prolific application of machine learning has been visualized in last 5 years in microbiome studies that has focus on clarifying microbial taxonomy and their mutual interactions as well as also evaluating microbiome biomarkers of diagnosis of multiple diseases [138]. More recently, the efficacy of probiotic therapeutics has been evaluated by utilizing the ABIOME (A Bioreactor Imitation of the Microbiota Environment) utilizing machine learning algorithms at metabolome level [139]. The same approach can be well applied for microbiome-based diagnostic for COVID-19. The whole metagenomic fecal data, i.e., microbiome, mycobiome, and virome, gives longitudinal molecular and metabolite profiles of host and microbes interaction. Furthermore, 16sRNA sequencing data and other taxonomic markers can be used to study specific microbial diversity of an individual. The unique microbiome profile can be further modelled through various machine learning methods and utilizing the ABIOME, an artificial model of the human gastrointestinal tract that will give an idea of efficient probiotics and its effector molecules. This approach is better coined as bottom-up approach that can be assessed at both cellular (phenotypic perspective) and molecular level (genotypic perspective). An overview of proposed model for utilizing precision postbiotics is depicted in Fig. 5. The phenotypic perspective covers the screening of postbiotic effects by utilizing in vitro and ex vivo cell cultures as well as animal models comprising immune, neuronal, metabolic, or microbial read-outs. The genotypic perspective is based on selection of postbiotics through in silico prediction of their effects governing microbial or host pathways that impacts the severity of COVID-19. Based on microbiome profile, precision postbiotics will be given for the efficient management of this disease. However, the proposed scheme will foresee major challenge in collection of person-specific data with respect to their genetics, immune profiling, microbiome data, and anthropometrics as well as implementation of correct machine learning tools for optimum outcome. The road for the execution of the proposed framework seems to be overoptimistic and arduous in the current scenario but it is likely to be seen that in the next few years every human has its own microbiome card that facilitates the use of postbiotics as personalized therapeutics depending on the prevalence of pathogen variants. Furthermore, recent studies reported the presence of bacterial genus Veillonella in the gut that metabolizes lactic acid to propionate and enables the enhancement of physical performance [140]. This concept leads in the emergence of biological doping where postbiotics can be used for modifying the physical fitness and performance. This signifies their role in enhancing or modulating the immunity of an individual that can also be explored in reducing the susceptibility or severity towards other viral infections.
Proposed model for the development of precision postbiotics to be used in the management of COVID-19 pandemic
Conclusion
The past decade has seen stupendous stride in underpinning the molecular mechanism and bioactive metabolites of probiotics. The continuous refurbishing of probiotic effector molecules as postbiotics and their health benefits has radically transformed the basic research to translational aspects. However, the scarcity of data on antiviral effect of postbiotics warrants comprehensive investigations, but the existing research evidences prove that these molecules possess magnificent properties from clinical, technological, and economic perspectives for controlling the virus. As today, the entire world is scourged by COVID-19 pandemic, and working hard to overcome and control the current situation. Yet, its long-term effects need to be precisely investigated. The overwhelming utilization of repurposed drugs and antibiotics will be detrimental to our gut microbiome and it may lurk another menace behind COVID-19. Thus, it reminded us a very old adage of our ancestors that “It’s all about gut feelings.” By keeping this view in mind, the exploration of postbiotics as therapeutics is “carte blanche” provided us by our “buddy bugs.” Looking forward for exploring the human internal bioreactor may be a ray of hope in dark clouds; thus, a vision of “precision postbiotics” will be certainly on horizon.
Data Availability
Not applicable.
Code Availability
Not applicable.
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The authors greatly acknowledge the support of Gautam Buddha University and Maharishi Dayanand University for writing this manuscript.
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Barkha Singhal conceptualized the idea and wrote the manuscript and Krishna Kant Sharma has critically revised the manuscript by giving his meticulous suggestions. Muskan Pandey has formulated four figures and helps in technical assistance related to referencing of manuscript and Archana Bhati and Kumari Priya drawn the specialized diagrams depicting the mechanistic details of postbiotics in gastrointestinal region and made comprehensive tables of this manuscript. The authors also acknowledged the support of Biorender software for making Figs. 2, 3, and 4 in this manuscript.
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Pandey, M., Bhati, A., Priya, K. et al. Precision Postbiotics and Mental Health: the Management of Post-COVID-19 Complications. Probiotics & Antimicro. Prot. 14, 426–448 (2022). https://doi.org/10.1007/s12602-021-09875-4
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DOI: https://doi.org/10.1007/s12602-021-09875-4